key: cord-0690745-7rfc73qb authors: Karabasz, Alicja; Bzowska, Monika; Szczepanowicz, Krzysztof title: Biomedical Applications of Multifunctional Polymeric Nanocarriers: A Review of Current Literature date: 2020-11-06 journal: Int J Nanomedicine DOI: 10.2147/ijn.s231477 sha: b1eee39803258eef06d8a3675ffbc70a8b91d948 doc_id: 690745 cord_uid: 7rfc73qb Polymeric nanomaterials have become a prominent area of research in the field of drug delivery. Their application in nanomedicine can improve bioavailability, pharmacokinetics, and, therefore, the effectiveness of various therapeutics or contrast agents. There are many studies for developing new polymeric nanocarriers; however, their clinical application is somewhat limited. In this review, we present new complex and multifunctional polymeric nanocarriers as promising and innovative diagnostic or therapeutic systems. Their multifunctionality, resulting from the unique chemical and biological properties of the polymers used, ensures better delivery, and a controlled, sequential release of many different therapeutics to the diseased tissue. We present a brief introduction of the classical formulation techniques and describe examples of multifunctional nanocarriers, whose biological assessment has been carried out at least in vitro. Most of them, however, also underwent evaluation in vivo on animal models. Selected polymeric nanocarriers were grouped depending on their medical application: anti-cancer drug nanocarriers, nanomaterials delivering compounds for cancer immunotherapy or regenerative medicine, components of vaccines nanomaterials used for topical application, and lifestyle diseases, ie, diabetes. Medical application of nanomaterials is becoming increasingly crucial in diagnostics (delivery of contrast agents for imaging) as well as in prophylaxis (vaccines) and therapy of various diseases (drug delivery systems). Nanocarriers employed in medicine improve the bioavailability, pharmacokinetics, and effectiveness of various therapeutics or contrast agents, ensuring: increased hydrophilicity, reduced interaction with plasma and cellular proteins, and better accumulation in target tissues. The most promising purpose of exploiting nanoparticles in medicine is their potential to localize (or be targeted) in a specific manner to the site of disease and reduce or eliminate the possible side effects. 1 Targeting can be broadly classified into three regimes; passive, active, andphysical. 2 Passive is based on accumulating nanoparticulate systems containing drugs through leaky vasculature of a diseased area. It was found in tumors, infarcts, and inflammation regions. In such regions with increased vascular permeability, nanoparticulate systems can selectively accumulate and release a drug that exerts a therapeuticeffect. 3 This phenomenon allows the delivery of drugs to the tumors, for which "enhanced permeability and retention" (EPR) effect is observed. 2, 4, 5 The EPR effect is predominantly described for solid tumors where fenestrations between epithelial cells, disorders in the pericyte coverage, and the lack of a smooth muscle layer of new blood vessels are sufficient for nanomedicines accumulation. Additionally, impaired lymphatic drainage in this tissue is responsible for nanocarriers retention. 6 Another approach, active targeting, is based on the specific recognition of targeted diseased region/cells' ligands. Finally, physical targeting includes pH-sensitive, temperature-sensitive, redox potential sensitive, ultrasound sensitive, and magnetic sensitive systems. As a result of nanomaterials' research, over 50 nanoformulations for oral, intravenous, subcutaneous, intrabronchial, topical, or intramuscular administration have already been approved by the American Food and Drug Administration (FDA) or the European Medicines Agency (EMA) for human use. 7, 8 The most clinically approved nanomedicines belong to liposomes and polymeric nanoparticles; however, the number of nanomaterials accepted by the FDA for medical applications is still low. An example of a polymeric nanomedicine is Apealea/Paclical containing micellar paclitaxel (paclitaxel formulated with the surfactant XR17) used to treat epithelial ovarian cancer, primary peritoneal cancer, and Fallopian tube cancer. 9 The new polymer nanomaterials' safety and therapeutic efficacy recently verified several clinical studies that mostly concerned nanocarriers of anti-cancer drugs. Phase three of clinical trials have already been completed for yet another paclitaxel formulation -NK105, a "core-shell-type" polymeric micellar nanoparticle formulation used in patients with metastatic or recurrent breast cancer. 10 Still, other studies concerned nanomedicines such as cyclodextrin-based polymer-camptothecin CRLX101 or conjugated docetaxel CRLX-301. Soon, the first phase of clinical trials will begin on polymeric nanoparticles loaded with monoclonal antibody Cetuximab and decorated with somatostatin analog for the targeting of colon cancer (data from clinicaltrials.gov). In connection with the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) pandemic, at least several different nano-based-tools have been developed that could be useful in the treatment of patients with the coronavirus disease-19 . 11, 12 Clinical trials have recently started for a full-length recombinant SARS-CoV-2 glycoprotein nanoparticle vaccine adjuvanted with the saponin-based Matrix M (NVX-CoV2373, developed by Novavax, NCT04368988) or inhaled nanoparticle formulation of Remdesivir (developed by NeuroActiva, NCT04480333, data from clinicaltrials.gov). 13 Nanocarriers were initially developed to improve the pharmacokinetics of drugs, but they unexpectedly received much attention from researchers and have become the center of this promising trend of multifunctional nanomedicine. 14 Unlike molecular drugs or imaging agents, nanoparticles can easily integrate more than one kind of contrast or therapeutic agent, making them potential multifunctional nanoplatforms. The concept of multifunctional nanocarriers also refers to the precise delivery of more than one drug simultaneously, which increases the effectiveness of therapy or overcome resistance to a given compound. Delivery of more than one agent also allows the use of various therapeutic methods (for example, chemotherapy and immunotherapy, chemotherapy and photodynamic therapy, induction of the immune response to the selected antigen, and enhancement of this response). There are constant enormous demands on new, advanced, multifunctional nanomaterials to be used in the future of medicine. First of all, they should be biodegradable and biocompatible. They are also supposed to be very stable in the body, have optimal pharmacokinetics and biodistribution, ensure the protection of healthy tissues, and accumulate drugs in diseased tissue at the right time of the disease process. Additionally, they should deliver chemically diverse compounds for including small drugs (antibiotics, cytostatics), nucleic acids, peptides, proteins, and magnetic nanoparticles. Appropriate synthesis methods should allow the biological activity of transported drugs to be preserved. It is especially important when providing active therapeutic proteins (enzymes, cytokines) or antigens that are the essential components of vaccines. The purpose of this work is to present the latest scientific reports on polymeric nanocarriers for medical applications. We selected papers that were published in 2016-2020. We describe nanomaterials whose biological assessment has been carried out at least in vitro. Most of them have also been tested in vivo. A literature search (PubMED) revealed that polymeric nanocarriers are most often used as drug delivery systems. Since effective cancer treatment still seems to be the most significant medical challenge, most of the new nanomaterials that have recently been obtained and characterized are primarily anti-cancer drug carriers ( Figure 1 ). In this work, we also present less numerous polymer nanomaterials to treat other diseases such as diabetes, atherosclerosis, or diseases based on chronic inflammation. We focused primarily on these polymeric nanocarriers, which in our opinion, can be described as multifunctional, with high capacity as innovative diagnostic and therapeutic systems for the clinical field in the treatment of various diseases, and with the considerable potential for improving human health. Nanocarriers are generally considered as particulate structures with a diameter smaller than 1000 nm. Depends on the morphology, nanoparticles, nanospheres, and nanocapsules can be defined as presented in Figure 2 . Nanoparticles/nanospheres are generally homogenous matrix systems in which the drug is dispersed in the material, forming them or can be adsorbed in their pores or at their surface, or the drug can be conjugated to them. On the other hand, nanocapsules' structure can be divided into two parts, the core and the shell. 15 The core material can be solid, liquid, or gas, depending on the type of application, while the shell is usually formed from the polymeric material. Generally, the drug is located in the core part, while the shell protects them from the external environment. However, incorporation in shell material and adsorption at their surface is also possible, allowing simultaneous delivery of one or several drugs in different nanocapsule compartments. The shell may be made permeable, semi-permeable, or impermeable, depending on the application. Permeable or semi-permeable shells are used for controlled release applications. The release rate from capsules is governed mainly by the shell's thickness, its pore's size, and the core's material. There are three main classical polymeric nanocarriers preparations: layer-by-layer method, nanoprecipitation method, and emulsion templated method. Emulsion templated methods mainly include emulsification-diffusion, emulsification-evaporation, emulsification-coacervation, multiple emulsification, and emulsion/polymer coating. [15] [16] [17] [18] [19] Nevertheless, other methods have been used, such as methodologies for preparing polymer-coated liposomes, polymersomes, dendrimers, or self-assembled polymeric micelles inorganic The main biomedical application of polymeric nanocapsules/nanocarriers. Notes: PubMed resources searched in all fields using the term "polymeric nanocapsules" filtered on "in the last five years" (2016-2020). Seven hundred seventy results were obtained (on March 25, 2020), and the authors selected 320 publications in which nanocapsules were used in the biomedical field (excluding diagnostic application and review papers). (A) Polymer nanocapsules were divided into three categories depending on their application in medicine. (B) Since the vast majority were nanocapsules used as a drug delivery system (294 from 320 publications), the authors present the types of transported drugs, w/o drugs stand for nanocapsules which were obtained empty and have potential as drug transporter. nanoparticles modified with polymeric materials as well as protein/peptide self-assembled nanocarriers. 20-29 Sketches of selected polymeric nanocarriers are presented in Figure 3 . On the other hand, the mentioned methods of preparation of polymeric nanocarriers could be divided mainly by two approaches: (i) dispersion of the preformed polymers; and (ii) polymerization of monomers. The commonly used polymers are: Arabian gum, gelatin, ethylcellulose, hydroxypropylmethylcellulose phthalate, poly-e-caprolactone (PCL), poly(lactide) (PLA), poly(lactide-co-glycolide) (PLGA), poly(alkyl cyanoacrylate) (PACA), while the polyelectrolytes are: polyethyleneimine (PEI), polyacrylic acid (PAA,), poly(diallyldimethylammonium, chloride) (PDADMAC), poly(sodium 4-styrene sulfonate) (PSS), and poly(allylamine hydrochloride) (PAH), dextran sulfate (DS), poly(glutamic acid) (PGA), alginates and alginic acid (ALG), hyaluronic acid (HYL), chitosan (CHIT), poly(lysine) (PLL). Synthetic polymers have higher purity and better reproducibility than natural ones, while natural ones possess better biocompatibility. 17, 19, 30 Another class of polymeric nanoparticles is based on proteins or peptides. They are biological macromolecules composed of amino acids, with proved biocompatibility and bioavailability. Protein/peptide nanoparticles are widely used to enhance the bioavailability of drugs. 27 Surface modification of nanocarriers for the preparation of multifunctional drug delivery systems eg for passive, active, and physical targeting, are performed. 21, 31, 32 Polymeric nanocarriers have been increasing in interest and applied in the pharmaceutical field, especially as drug delivery systems ( Figure 1 ). Since several specialized reviews have already discussed nanotechnology and polymeric materials for the formulation of nanocarriers, [15] [16] [17] 19, 26 in this review, we present a brief introduction of the classical formulation techniques. The sequential adsorption of oppositely charged nanoobjects (Layer-by-Layer (LbL) method) is a powerful approach for fabricating multilayer thin films. 33, 34 The origin of multilayered adsorption can be traced back to the mid-1960s when Iler proposed deposition of microparticles onto solid substrates in the LbL manner. 35 In the 1990s, Decher and Hong expended the LbL by using a combination of linear polycations and polyanions. 33 The layer-by-layer adsorption of charged nanoobjects like polyelectrolytes, nanoparticles, proteins, organic molecules, etc., is considered as a convenient method to obtain multilayer "nanocarriers" shells on colloidal cores (Figure 4) , and those types of capsules have been the subject of intensive research since 1998 when Sukhoukovr proposed the method of forming polyelectrolyte multilayers shell on solid microparticles. 36 Furthermore, the layer-by-layer method was applied for liquid and gas cores. 37, 38 The layer-by-layer (LbL) method's main advantage are the ease of manipulation and the multifunctionality that comes from the possibility of modifying the polyelectrolyte shell by organic molecules, polymers, inorganic nanoparticles, carbon nanotubes, antibodies, lipids, or nanoparticles. [39] [40] [41] That multifunctionality is of fundamental importance for the preparation of multifunctional drug delivery systems. For passive targeting, the polyelectrolyte shell is modified by the adsorption of so-called "stealth" polymers like poly(ethylene glycol) (PEG), poly-(acrylamide), poly(vinylpyrrolidone), polysaccharides, or dextrans. [42] [43] [44] That modification prolongs circulation time and allows nanocarriers' accumulation in the targeted area through an EPR effect. 4, 5, 45 For active targeting, polyelectrolyte shells can be functionalized by adsorption/incorporation of targeting ligands like antibodies or folic acids present on the surface of the targeted cells; for physical targeting, by the incorporation of stimuli-responsive building blocks in multilayered shell eg pH-responsive polymers, magnetic nanoparticles, etc. For example, the incorporation of magnetic nanoparticles that allows controlling magnetically responsive nanocarriers using an external magnetic field could be indicated. [46] [47] [48] That incorporation allows the application of such nanocarriers as a tool for cell-biology research to separate and purify cell populations, tissue repair, magnetic drug delivery, magnetic resonance imaging (MRI), magnetic hyperthermia, etc. [49] [50] [51] [52] [53] [54] Excellent books and comprehensive reviews of LbL nanocarriers have been written. [55] [56] [57] [58] The Nanoprecipitation Method The nanoprecipitation method is also known as solventdisplacement, or interfacial deposition method, or solvent shifting method. According to Fessi et al, the nanocarrier synthesis needs both solvent and non-solvent phases (usually, the solvent and non-solvent phases are called organic and aqueous phases, respectively). 59 A polymer and active substance solution in a miscible organic solvent or a mixture of solvents (ie ethanol, acetone, hexane, methylene chloride, or dioxane) is added to a nonsolvent or mixture of nonsolvents supplemented with one or more surfactants. It can be performed either by dialysis or by the dropping technique ( Figure 5 ). After adding the organic phase to the water phase, the polymer diffuses with the organic solvent and precipitates at the interface between oil and water, forming nanocarriers. 60 The principle of nanocarriers formation by nanoprecipitation is a fluctuation of polymer concentration at the interface between solvent and precipitant during the solvent to nonsolvent exchange. 61 The initial supersaturation at the interface layer occurs, followed by the interfacial deposition of the polymer. 17 The nanocarriers' characteristics can be mainly influenced by polymer concentration, injection method of the organic phase (dialysis or dropping), the volume ratios components, and the nature of materials. 61 The interfacial deposition method has been used intensively in the last decade, due to the simple operation without applied external high energy force and extensive applicability for various payloads. The studies of polymeric nanocarriers formulation by the nanoprecipitation method are excellently summarized in the following review. [61] [62] [63] [64] The Nanoemulsion Templated Methods Nanoemulsions are thermodynamically unstable but kinetically stabilized systems. 65, 66 For nanoemulsion preparation, the organic or aqueous phase is emulsified in the aqueous or organic phase in the presence of a surfactant (stabilizing agents). During the nanoemulsion formation, surfactants are self-assembled at the interface between two immiscible phases to reduce the interfacial tension, thereby achieving a stable state. The various methods of formation of nanoemulsion including a high energy ones (eg, ultrasonication, high mechanical shear forces) and low energy ones (eg, phase inversion composition, phase inversion temperature, membrane emulsification, selfemulsification) have been developed. 65, 66 The size of the droplets of nanoemulsion is in the range of about 20-500 nm with a low polydispersity index. Nanodroplets found application as a template for polymeric nanocarrier synthesis both from preformed polymers and monomers in a polymerization process. The second approach is generally restricted to synthetic polymer materials, in which case one of the phases usually contains monomers, which in the polymerization process form polymeric nanocarriers. Here four main methods ( Figure 6 ): emulsification-diffusion, emulsification-evaporation, emulsification-coacervation, multiple emulsification will be described; nevertheless, other nanoemulsions templating methods have been used such as nanoemulsion/polymer coating or nanoemulsion polymerization. 19, [67] [68] [69] In this method, the polymer and active substance containing the oil phase are emulsified into an aqueous solution in the presence of surfactants to make oil in water nanoemulsion. After the formation of nanoemulsion, the organic solvent is evaporated either by increasing the temperature/under pressure or by continuous stirring results in polymeric nanocarriers' formation. Nanocarriers are formed by polymer precipitation during an evaporation procedure. The influence of process parameters on the properties of prepared polymeric nanocarriers has been discussed. 16, 17, 19, 26, 32 In this method, the oil phase contains polymers and active substances dissolved in the organic solvent (eg dichloromethane or chloroform) and another solvent that is miscible with water (eg acetone, ethanol, or ethyl acetate), thereby removing them by diffusion into water. 16, 17, 19, 26, 32 Such an oil phase is emulsified into the aqueous solution in the presence of surfactants to make oil in water nanoemulsion; subsequently, due to the spontaneous diffusion of water-miscible solvent, nanocarriers are formed by a combination of polymer precipitation and interfacial phenomena. In the emulsification-coacervation method, polymeric nanocarriers are formed and stabilized by physical coacervation or chemical crosslinking at the interface. This method is principally used for materials (monomers or polymers) possessing crosslinking function groups. Physical coacervation (eg based on electrostatic interaction), as well as chemical ones (eg by chemical crosslinking or interfacial polymerization), have been proposed. 16, 17, 19, 26, 32 Multiple emulsions are heterodisperse systems called "emulsions of emulsions" formed when oil droplets in a continuous water phase contain dispersed water droplets (w/o/w). 19 A hydrophilic active substance is dissolved in water, that is dispersed into the oil phase containing a dissolved polymer in the presence of a stabilizer. This primary/internal emulsion containing hydrophilic active substance is emulsified in an outer water phase again in the presence of a stabilizer. The procedure for obtaining the polymeric nanocarriers is similar to the single nanoemulsion technique for solvent removal, ie, diffusion, evaporation, coacervation, or a combination of these approaches. A reverse system w/o/w may also be formed ( Figure 7) . 19, 70 Chemotherapy remains one of the most important treatments for all cancer types, but its efficacy is lower than expected. The right approach to improve it seems to be developing better formulations, including nanoformulations of already approved drugs. However, the clinic's nanoformulations are less toxic than conventional therapy; their therapeutic efficiency remains unchanged. Therefore, even better nanoformulations of anti-cancer drugs are continually being sought. Various polymeric nanocarriers have recently been successfully obtained and characterized in vivo and seem promising as the oral or intravenous transporters of the following chemotherapeutic agents: gemcitabine, diphenyl diselenide, etoposide, thiazolidinediones, imiquimod, methotrexate, or tamoxifen (Table 1) . Very complex nanocarriers have been developed to deliver some drugs, eg, doxorubicin, to simultaneously increase drug delivery and precisely control drug release in the tumor. The free doxorubicin may cause cardiotoxicity in some patients leading to the discontinuation of therapy. 71 Wang et al proposed the use of polymer nanocarriers made of reduction-responsive arginine-tethered amphiphilic copolymers and microwave absorbing ammonium bicarbonate for doxorubicin encapsulation. These nanocarriers can easily penetrate the tumor and are efficiently taken up by cancer cells. After irradiation by the pulsed microwave in the cell, in nanocarriers, ammonium bicarbonate converts the adsorbed energy to kinetic energy, which may generate thermocavitation and production of gas bubbles in cells. Consequently, intracellular structures are destroyed, and the doxorubicin releases from nanocarriers immediately target tumor cells. 72 Still, other polymeric nanocarriers have been designed to release doxorubicin under the influence of reactive oxygen species (ROS). Because the oxidative environment is characteristic of tumors or tissues affected by chronic inflammation, the release of drugs can be most active there. It has been demonstrated for nanocarriers made of a biocompatible copolymer, namely phenylboronic acid pinacol ester-functionalized poly (ethylene glycol)-blockpoly (phthalic anhydride-alter-glycidyl propargyl ether). Due to the phenylboronic acid ester's presence, this nanocarrier was sensitive to oxidative stress and demonstrated an improved anti-cancer effect in a breast cancer mouse model. 73 Another exciting approach is multidrug therapy using optimally selected agents, simultaneously or sequentially administered, to achieve a synergistic therapeutic effect. Attempts are being made to develop various nanomaterials, including polymeric nanocarriers, that would allow more than one drug to be delivered efficiently. 74 Zhou et al proposed an attractive approach for sequential co-delivery of gefitinib (a small-molecule inhibitor of the epidermal growth factor receptor -EGFR) and doxorubicin. They obtained nanocarriers based on drug-polymer conjugation and ion pairing. Gefitinib was complexed with dioleoyl phosphatidic acid (DOPA) and encapsulated by coprecipitation with doxorubicin-conjugated poly (L-lactide)-block-polyethylene glycol (DOX-PLA -b-PEG). The biological activity of these nanocarriers was compared in vitro with Doxil (PEGylated liposome with doxorubicin -FDA approved doxorubicin nanoformulation), demonstrating a better anti-cancer effect against A549 (human non-small cell lung cancer) and MDA-MB -468 (human mammary adenocarcinoma, triple-negative breast cancer cells). Moreover, the analysis of pharmacokinetic and biodistribution in the mouse model confirmed the high nanocapsule accumulation inside the breast tumors. However, the authors have not yet conducted studies on the developed nanocarriers' anti-tumor activity in vivo. 75 There are many examples of polymeric nanocarriers equipped with more than one chemotherapeutic. Nanoparticles with popular drugs, eg, doxorubicin, paclitaxel, curcumin, 5-fluorouracil, were proposed. In all cases, more than one anti-cancer agent's encapsulation allows a better therapeutic effect than one drug (summarized in Table 2) . A more complex multifunctional nanocarrier system, namely RGD-PS-PEG calcium phosphate nanoparticles, was obtained and characterized previously by the team of Dong et al. They used the polymer RGD-PS-PEG (RGD corresponds to peptide H-(D-Val) -Arg-Gly-Asp-Glu-OH; PS-PEG is organic phosphatidylserine-polyethylene glycol) self-assembling into micelles to encapsulate the anti-cancer drug Novantrone (mitoxantrone hydrochloride). Moreover, calcium phosphate that adsorbs Verapamil was used to form an inorganic shell on the organic core (RGD-PS-PEG with Novantrol) to stabilize these nanoparticles. 76 Because Verapamil is a P-gp inhibitor, these nanocarriers co-deliver a chemotherapeutic and anti-multidrug resistance agent. It is worth emphasizing that, in this case, the carrier was additionally actively targeted by the covalent coupling of PS-PEG with the RGD peptide. RGD is a cell adhesion motif displayed on extracellular matrix and is a ligand, for example, for αvβ3 or α5β3 integrins. The expression of these integrins is high on the tumor endothelium cells. Therefore RGDfunctionalized nanocarriers may increase drug delivery to the tumor. 77 In vivo studies performed after intravenous administration of RGD-PS-PEG calcium phosphate nanoparticles to animal bearing MCF7/MDR tumors (multidrug-resistant human breast cancer cells MC7) indeed revealed the increased concentration of encapsulated drugs in tumors, improved therapeutic effect, and submit your manuscript | www.dovepress.com International Journal of Nanomedicine 2020:15 showed the beneficial effect of functionalization on drug accumulation, resulting in better therapeutic efficacy and lower toxicity to healthy tissues. 78, 79 There are also attempts at dual encapsulation of chemotherapy and inorganic nanoparticles. Jeon et al obtained paclitaxel loaded nanocarriers coated with crosslinked gold nanoparticles and poly(amidoamine) dendrimers. The therapeutic efficacy of this combination was confirmed in a mouse tumor model. 80 Besides, superparamagnetic iron oxide nanoparticles (SPIONs) can be used for magnetic targeting. PLGA-PEG nanocarriers with SPION and docetaxel showed faster and stronger accumulation, followed by better tumor growth inhibition after local exposure to the magnetic field. 81 Because encapsulated inorganic compounds are predominantly applied as contrast agents, PLGA-PEG nanocarriers were also used as a magnetically-targeted triple-modal imaging system. This time SPIONs and indocyanine green (fluorescence near-infrared dye) were encapsulated in the hydrophobic core, and diethylene triamine penta acetic acid was conjugated to PLGA-PEG in order to Indium-111 (radioisotope) chelation. This approach was tested on a mice model after intravenous injection and allowed for successful tumor visualization via fluorescence, MRI, and nuclear imaging. Furthermore, the accumulation of nanocarriers, hence the signal intensity, was more significant after adding an external magnetic field around the tumor. 82 Other examples of MRI contrast agents are semicrystalline polyurea nanocarriers with Gadobutrol (commercial contrast agent of gadolinium(III) complex), which poses enhanced tissue contrast compared to the free agent. 83 Also, PEGylated nanocarriers with cubic cobalt ferrite nanocubes were detectable via MRI in the tumor tissue after its intratumoral injection. 84 An exciting example is actively targeted perfluoropropane filled covered with gold nanoshelled PLGA nanocarriers functionalized with anti-VEGFR2 (vascular endothelial growth factor receptor type 2 overexpressed on tumor surrounding vascular endothelial cells) and anti-p53 antibodies for precise ultrasound molecular imaging of breast cancer. The authors have shown that dual-targeted nanocarriers accumulate in the tumor (orthotopic mice breast cancer) about two times more than nontargeted, ensuring accurate breast cancer detection. Interestingly, regardless of double targeting, the amount of the injected dosage detected in the tumor was 5%, which is still lower than expected. 85 The easily modifiable thickness of the polymeric shell allows, for example, to obtain thin-shelled nanocarriers to deliver perfluorooctyl bromide, which finds application in ultrasonography as a contrasting agent. The liquid core of nanocarriers and the appropriately thin shell made of PLGA-PEG ensure very good echogenicity and acoustic response. Besides, nanocarriers' surface functionalization with a monoclonal therapeutic antibody specific for EGFR (Cetuximab) improves the accumulation of capsules within tumors that overexpress this receptor. 86 Anti-cancer theranostics uses advanced nanomaterials to simultaneously and accurately detect disease processes in the patient's body and deliver drugs directly to areas affected by the disease. An interesting example is amphiphilic nanocarriers synthesized using block copolymer, succinic anhydride functionalized poly (2-diisopropylaminoethyl methacrylate) -block poly (2-aminoethyl methacrylate hydrochloride) with hydrophobic ruthenium entrapped in the core. The acidic tumor environment allows this compound's active release, a known inhibitor of DNA replication with fluorescent properties. 87 Exciting examples of anti-cancer theranostics are multifunctional polymeric PLGA nanocarriers designed for the High-Intensity Focused Ultrasound (HIFU) combined with transarterial chemoembolization treatment of hepatocellular carcinoma model in rabbits. The nanocapsule shell contained magnetic Fe 3 O 4 as a contrast compound for MRI, and hydrophobic perfluorohexane was encapsulated into the core. HIFU is a method for local cancer treatment based on high temperatures leading to tissue destruction. Because perfluorohexane may increase energy deposition in cancer tissue, it is an enhancing agent for HIFU. Simultaneously, the embolization of blood vessels in the tumor allows retaining more nanocarriers within a tumor and improving therapy's efficacy. 88 Multifunctional, intelligent, and dual-stimulus responsive nanocarriers, functionalized with folate for active delivery of doxorubicin and indocyanine green (ICG), have also been obtained using PLGA -polyethylene glycol -poly (N-isopropyl acrylamide). ICG is known as a near-infrared fluorescence (NIR) imaging agent, as well as the photosensitizer in photodynamic therapy (PDT), or photothermal agent in photothermal therapy (PTT). At the same time, Fe/FeO nanocrystals were tethered with PLGA polymer, finally forming the shell of multifunctional nanocarriers. Fe/FeO nanocrystals are MRI contrasting agents, and they may provide additional, precise diagnostic information about the exact tumor location and size. After irradiation with NIR laser, nanocarriers shrink and degrade, releasing doxorubicin and ICG while Fe/FeO simultaneously degrades in the acidic tumor environment, leading to the overproduction of ROS as a result of the Fenton reaction. Results obtained in mouse tumor models suggest that it may help overcome hypoxia-related tumor resistance to PDT. 89 Wang et al showed that the problem of insufficient oxygen in the tumor significantly limited the effectiveness of PDT, which can be solved by the simultaneous delivery of a photosensitizer, in this case, meso-tetra (p-hydroxyphenyl) porphine and catalase, an enzyme that decomposes endogenous tumor H 2 O 2 into water and oxygen. This approach was possible due to the use of unique polymeric nanocarriers obtained due to the covalent coupling of catalase, meso-tetra (p-hydroxyphenyl) porphine, and PEG, and additionally labeled with 99 in vivo single-photon emission computed tomography imaging. 90 ICG converts NIR light energy into local heat leading to cancer tissue ablation. However, cellular stress-induced during this therapy may activate autophagy in cancer cells, which is a complex process that eliminates damaged cellular structures. It can promote tumor cell survival and further tumor progression. That is why Wu et al have proposed yet another multifunctional system for the delivery of ICG and improve PTT's effectiveness. It uses nanocarriers made of malPEG-b-poly (l-phenylalanine-co-l-aspartic acid), loaded with ICG and primaquine -autophagy inhibitor. The nanocarriers' surface has been modified by covalently attaching to the polymer the so-called cell-penetrating peptide (CPP, Cys-KRPTMRFRYTWNPMK), allowing shielding of the entire capsule as a result of hyaluronic acid (HA) binding. HA actively directs nanocarriers to the tumor due to interaction with CD44 (HA receptor). Then, HA corona is decomposed in the tumor's acidic environment, exposing CPP that facilitates nanocarriers uptake. The anti-cancer effects of these nanocarriers have already been confirmed by in vivo studies. 91 The intelligent, PEGylated bismuth selenide nanocarriers were designed to deliver doxorubicin and yet another agent used in PDT/PTT, namely chlorin (Ce6). The entrapment of small drugs in bismuth selenide is simple because of their mesoporous and hollow structure (sponge-like structure). It is worth emphasizing that because previous studies confirmed the usefulness of bismuth selenide as a computed tomography contrasting agent, these nanocarriers enabled bimodal imaging of tumors, fluorescence, and CT. Fluorescence imaging confirmed efficient tumor accumulation of nanocarriers and remarkable tumor eradication. It resulted from the synergistic effect of doxorubicin and PTT/PDT-induced tumor ablation. At the same time, toxicity analysis revealed, the nanocarriers were not harmful to healthy tissues. The high therapy specificity resulted from the selective drug release primarily in the tumor. Protonation of the amino group of DOX under acidic tumor conditions altered, leading to increased drug hydrophilicity and its release from nanocarriers. Additionally, upon NIR laser irradiation, there was also a release of drugs from the nanocarriers in the tumor. 92 PEGylated, biodegradable hollow mesoporous organosilica nanocarriers were obtained to deliver up to 3 different anti-cancer compounds. In addition to ICG, they contained gemcitabine and 17 AAG, the heat-shock protein 90 inhibitors. The use of 17AAG allows to overcome tumor thermoresistance, the phenomenon regulated by heat shock proteins that are responsible for the proper functioning of selected cancer defense mechanisms, that affect anti-cancer effects of PTT. 93 A unique example of theranostic nanocarriers can be peptide nanoparticles that possess fluorescent properties. The team of Fan et al obtained self-assembling nanoparticles based on octa-peptide cyclo -[(D-Ala-L-Glu-D-Ala-L-Trp) 2-] and Zn 2+ ions and used them to deliver a chemotherapeutic compound, epirubicin. Studies performed on the mouse esophagus cancer model demonstrated that Zn 2 + -coordinated cyclic peptides forming these nanoparticles emit NIR fluorescence due to quantum confinement within the nanostructures allowing tumors to be imaged without the use of any other imaging compounds. The presence of RGD on their surface ensured sufficient accumulation of nanocapsules in cancer. 29 It is worth asking why so few polymeric nanocarriers intended for the transport of cancer drugs are functionalized with specific ligands (ie anti-CD19 or anti-Her2 /ErbB2 monoclonal antibodies for active targeting of nanocarriers to cancer cells overexpressing these antigens). 94 It is believed that actively targeted nanoparticles more effectively affect cancer. However, retention of even modified nanomaterials in tumors depends on EPR. 95 Since most studies on the EPR effect have been conducted on rodent models, it is doubtful whether this effect occurs in humans and whether its functioning depends on the type of cancer. 96, 97 Also, in the case of human-emerging tumors, significant tumor volumes are elements of the so-called tumor microenvironment such as tumor-associated fibroblasts, immune cells, and extracellular matrix, which impede the nanoformulation of penetration into the tumor. 98 Additionally, intratumor heterogeneity makes it difficult to select the appropriate molecular target and hampers actively targeted nanoparticles. 99 It should also be mentioned that the vast majority of ligands for actively targeted nanodrugs only affect cancer cells without considering other tumor microenvironment forming cells. The problem is also the lack of efficient and cheap methods ensuring the attachment of ligands, especially those with a complex structure than RGD or folate (eg antibodies) while maintaining their biological activity. This makes the production of targeted nanodrugs expensive and costinefficient. 100 These factors probably contribute to the phenomenon observed in the clinic, indicating the lack of submit your manuscript | www.dovepress.com International Journal of Nanomedicine 2020:15 improvement in the effectiveness of many drugs given in nanoformulation compared to their free forms. The application of nanomaterials in anti-cancer therapies is not limited to the transport of chemotherapeutics. Numerous studies indicate that nanomaterials, including polymeric nanocarriers, may also be used in cancer immunotherapy. Briefly, immunotherapy's essential goal is to stimulate immune cells, primarily cytotoxic T lymphocytes (CTL), capable of eliminating cancer cells. Since strict CTL activation depends on their cooperation with antigen-presenting cells such as dendritic cells (DC) and macrophages, it is crucial to properly stimulate these cells' activity, eg, by specific adjuvants. An interesting approach was using intradermally administered nanocarriers made of PLGA for providing low-molecular agonists (imidazoquinoline-based esters) of endosomal pathogen recognizing Toll-like receptor 7/9 (TLR7/9). Due to encapsulation, these compounds underwent effective delivery and uptake by DC, enhancing on their surface the expression of CTL co-stimulatory molecules (CD80, CD40, CD86) and inducing the expression of selected cytokines. This activation of dendritic cells led to CTL stimulation and a better anti-tumor immune response. 101 In turn, the use of poly (β-amino ester)s copolymers assembling into nanocarriers with encapsulated IL-12 were efficiently delivered to the tumor after intravenous administration. This approach provides reversion of the tumor infiltrated macrophages from M2 to M1 phenotype, which resulted in a more effective anti-tumor response. It is worth emphasizing that the administration of IL-12 in nanocarriers allowed for a significant reduction of side effects resulting from this proinflammatory cytokine's systemic activity. 102 With the help of polymeric nanocarriers, cancer cells' surface can also undergo modification by exposing them to specialized immune cells such as natural killer cells (NK cells). This approach effectively stimulates immune cells, but limits their activity only to the tumor, bypassing other tissues. Zheng et al received very complex polymeric nanocarriers, in which the first layer was made of bovine serum albumin, with a covalently attached antibody and phenylboronic acid. The outer layer was glucose-modified poly (2-methacryloyloxyethyl phosphorylcholine) -b-poly (N-(3-aminopropyl) -methacrylamine) associated with the albumin layer due to the interaction between phenylboronic acid and glucose. Because this interaction is fragile in the acid environment of the tumor, it is possible to disassemble the outer layer easily. It results in simultaneous exposure of phenylboronic acid capable of binding sialic acids present on the surface of the cancer cells. Then, nanocarriers bind to the surface of cancer cells, and due to the presence of an antibody to lure NK cells. These cells may employ a direct killing mechanism involving antibody-dependent cell-mediated cytotoxicity. 103 As demonstrated recently, an interesting and even more comprehensive approach to overcoming tumor tolerance may be possible using nanocarriers whose shell is made of antigen (e.g, protein, overexpressed on tumor cells). Simultaneously, inside the carriers, there are two different adjuvants (resiquimod and muramyl dipeptide) stimulating DC. Such complex nanocarriers are, therefore, a therapeutic anti-cancer nano-vaccine. However, the immunostimulatory activity of these nanocarriers still requires verification in vivo. 102 Nanoparticles indeed offer many advantages as modern therapeutic and preventive vaccines for tumor, viral, and bacterial antigens (e.g, recombinant proteins and nucleic acid) delivering. They might help effectively protect the integrity of the antigen, increase its immunogenicity, and, as a consequence, improve vaccine efficacy. For example, incorporating the antigen into the nanoparticles allows for more effective delivery primarily from the injection site (subcutaneous or intramuscular injection) via the lymphatic system to secondary lymphoid organs where adaptive immune response develops. However, not without significance is the fact that nanomaterials with antigen, due to their size, shape, density, surface charge, and chemical complexity, can mimic the pathogen. Thus nano-vaccines more effectively stimulate immune cells (B cells and T cells), leading to efficient antibody synthesis and long-term immunity. This approach has already been successfully implemented to prepare clinically approved the influenza vaccine Inflexal/Crucell, where virus haemagglutinin was incorporated into liposomes. 104 Currently, there are various polymeric nanocarriers in development for the delivery of vaccine components. In that case, an antigen is displayed on the nanocarrier surface. It associates with shell-forming polymers already after the synthesis. The effectiveness of International Journal of Nanomedicine 2020:15 submit your manuscript | www.dovepress.com DovePress this process is monitored by analyzing changes in the zeta potential values. The research carried out on the mouse model revealed that the polymers that build nanocarrier shells are essential for the antigen's immunogenicity embedded in/on the surface. Peleteiro et al confirmed the higher efficacy of protamine nanocarriers over polyarginine ones in the induction of an immune response against the recombinant hepatitis B antigen. Vaccination of animals with protamine nanocarriers resulted in the higher production of antigen-specific antibodies and selected cytokines, including IL-17A and IL-1β. These cytokines, due to their proinflammatory activity, play a fundamental role in creating the right environment for the developing immune response. 105 An effective, but the slightly different solution is the use of two-layer nanocarriers, in which the antigen is trapped between two polymeric layers with opposite charges. Thus, an antigen is not exposed on the surface of the nanocarriers. Crecente-Canto analyzed in vivo on the mice model two different nanocapsule types: nanocarriers made of chitosan associated with bacterial antigen and nanocarriers in which the antigen bound to the chitosan layer was covered with a second layer of dextran sulfate. He concluded that coating the antigen with an additional layer of polymer may induce a better immune response. It is probably due to the increased stability of the delivered antigen, which is longer available for antigenpresentingcells. 106 It is worth emphasizing that the effectiveness of many vaccines based on the polymeric nanocarriers, although satisfactory, still seems lower than vaccines based on the antigen administered together with the standard adjuvant Alum. 105 Many researchers claim the effectiveness of nanovaccines can be significantly increased by additional encapsulation molecules that modulate the immune response, such as imiquimod, CpG or polyI: C. 107, 108 Interestingly, Fichter et al proposed the use of nanocarriers built exclusively from hepatitis C virus nonstructural protein 5A and functionalized with adjuvant monophosphoryl lipid A (MPLA) as a vaccine against the hepatitis C virus. Studies conducted on a mouse model showed that after intravenous administration, these nanocarriers efficiently and preferentially accumulated primarily in the liver, and thanks to MPLA, which is a ligand for TLR4, were detectable in liver-resident antigen-presenting cells such as Kupffer cells (specialized macrophages located in the liver) or DCs leading to induction of intrahepatic immune response specific to the viral antigen. The authors also emphasized that an essential advantage of using nanocarriers made solely of antigen is the lack of induction of an immune response directed against the additional material present in nanocarriers providing viral antigen. 109 Finally, polymeric nanocarriers can be useful in immunotherapy, aiming to induce immune tolerance to allergens (antigens). Briefly, this therapy involves supplying the body with a small amount of antigen to inhibit the synthesis of the underlying allergy molecules, namely IgE class antibodies and cytokines such as IL-4, IL-5, and IL-13. In vivo tests carried out by Smarr et al have shown that an effective and safe approach for the abrogation of allergen-specific response and inhibition of allergic inflammation can be the use of antigen-conjugated biodegradable PLGA, and antigen-encapsulated PLGA. It is worth emphasizing that, in this case, the antigen is encapsulated or covalently bound to the nanocapsule-building polymer. 110 Nanomaterials have also found a broad application in regenerative medicine, which aims to develop and apply therapies that support the healing of tissue injuries resulting from diseases or mechanical damage. Encapsulation of phenytoin (stimulate fibroblast for cytokine and growth factor production) into PCL nanocarriers significantly reduced drug skin permeabilization compared to a free drug when supplied with chitosan hydrogel. 111 Another example of polymeric nanocarriers embedded in a hydrogel was utilized as local anesthesia of the intraoral mucosa. The standard application of EMLA (a mixture of lidocaine and prilocaine) is limited because it inconveniences the patient (eg bitter taste and burning). Muniz et al proposed PCL nanocarriers for double encapsulation of lidocaine and prilocaine trapped in CARBOPOL (acrylic acid copolymer matrix) hydrogel. Studies in a rat model have shown that nanoformulation provides a better anesthesia duration compared to commercially available EMLA and free drugs embedded in the hydrogel. 112 At the same time, tissue regeneration is a multistep process, and the use of more than one active agent and long-term sequential release of the drug at the appropriate stage of the healing process is required. An interesting example of a nanosystem used for wound healing is dual encapsulation of bromelain and salvianolic acid B into an ultrafine core-shell nanofiber built from PCL, poly (vinyl alcohol), and gelatin. The nanofibers were designed to submit your manuscript | www.dovepress.com International Journal of Nanomedicine 2020:15 release bromelain sequentially at an early stage, and salvianolic acid B at a later stage of tissue healing. It is essential because bromelain poses anti-inflammatory, antimicrobial, and anticoagulant properties necessary at the initial inflammation phase. Salvianolic acid B promotes wound healing by stimulating angiogenesis, reepithelialization, and cell proliferation at proliferative, maturation, and remodeling phases of skin regeneration. During the in vitro evaluation, the authors proved biocompatibility, antibacterial, and proangiogenic properties of tested nanofibers. Besides, they confirmed that the subsequent sequential release of two compounds provides accelerated wound healing in rats compared to saline control and unloaded nanofibers. 113 Because in the late phase of bone healing, the surrounding environment becomes more alkaline Tian et al proposed pH-dependent nanocarriers with growth factorbone morphogenic protein-2 (nBMP-2). The authors used free-radical polymerization of N-(3-aminopropyl) methacrylamide, acrylamide, and glycerol dimethacrylate (degradable cross-linker) to synthesize alkalinedegradable polymeric shells. This solution provides a sustained release of BMP-2 at the therapeutic window. During research on the posterolateral spinal fusion in rats, nBMP-2 poses superior characteristics upon free BMP-2 and provides a better quality of newly formed bone and reduced undesirable inflammatory edema. 114 Additionally, proteins like growth factors are sensitive to tissue proteases, which provide their short half-life in the body. Thus, the nanocarriers application also reduces the risk of transported cargo proteolysis. Due to their pleiotropic properties, polyphenols were proposed for osteoarthritis treatment. To dual transport resveratrol and curcumin, self-assembling lipid-core nanocarriers with grape seed oil cores and PCL shells were proposed. Because of differences in the polyphenols solubility in oil, these drugs pose subsequent sequential releases from nanocarriers. The results indicate that this combination of polyphenols administered in nanocarriers protects chondrocytes against oxidative stress and shows better therapeutic efficacy against rat arthritis without undesired toxicity. 115, 116 There are also examples of the use of gene therapy in the treatment of osteoporosis. Sezlev Bilecen et al successfully proposed PLGA nanocarriers with siRNA inhibiting RANK expression (Receptor activator of nuclear factor κ B) protein, essential in the activation of osteoclasts. 117 Furthermore, nanocarriers built of amphiphilic gelatin with encapsulated TGF-β1 (transforming growth factor-β1) and magnetic nanoparticles were proposed for cartilage regeneration. This approach combines magnetic guidance with chondrocyte stimulation via growth factor. 118 The mentioned nanoformulation still requires evaluation of toxicity as well as therapeutic efficiency in vivo. An interesting example is drug delivery as eye drops, which is limited due to the rapid dilution and clearance of the drug that follows tear production and blink reflex. The effectiveness of nanoparticles in this area is due to their improved corneal interaction. Reimondez-Troitiño et al presented oil nanodroplets surrounded by cell-penetrating cationic polypeptides -protamine or polyarginine for corneal wound healing. Even empty nanocarriers administered in eye drops were able to accelerate wound healing in vivo process similarly to commercially available Cacicol ® . The use of protamine nanocarriers resulted from a decrease degree of corneal haze following tissue healing compared to polyarginine. This effect was probably due to the antifibrotic activity of protamine. However, additional encapsulation of cyclosporin A or vitamin A did not improve the therapy's effectiveness compared to empty nanocarriers. All nanoformulations were non-toxic in a mouse ocular tolerance test. 119 Recently published papers indicate that polymeric nanocarriers could be used in the future for the oral delivery of drugs, in particular biological drugs such as peptides and proteins. Oral administration requires developing a formulation that will protect them from degradation and loss of biological activity in the gastrointestinal tract and allow their effective absorption. Lifestyle diseases are a combination of diet, physical inactivity, and consumption of stimulants. They emerge more often each year, and polymeric nanocarriers have already been proposed as a drug delivery system for venous thromboembolism, hypertension, peripheral arterial disease, and inflammatory bowel disease (summaries in Table 3 ). Among these diseases, diabetes requires a new drug formulation improvement of patient safety. Many studies involve the development of an oral insulin formulation. This peptide hormone is widely used in treating type I diabetes and advanced type II diabetes when patients have inefficient insulin synthesis resulting from the destruction of the pancreatic beta-cells caused by prolonged hyperglycemia or dyslipidemia. Because insulin is a drug taken only by subcutaneous injection, developing International Journal of Nanomedicine 2020:15 submit your manuscript | www.dovepress.com an oral formulation would significantly improve patients' comfort of life and reduce therapy costs. Lee et al received insulin loaded pluronic based nanocarriers. Interestingly, to ensure the nanocarriers' best absorption in the small intestine, they armed them with two different ligands: chitosan and hexamer peptide AT-1002. Due to its interaction with the intestinal mucosa, chitosan allows nanocarriers to adhere to epithelial cells and improves interstitial permeability. Its activity is synergistic with the activity of AT-1002. AT-1002 is a peptide derived from zonula occludens toxin (ZOT), a virulence factor of Vibrio cholera, a pathogen responsible for the diarrhoeal disease cholera. 120 Because AT-1002, like ZOT reversibly and transiently enhances the intestinal permeability by rearranging the intestinal cell cytoskeleton strategically located to modulate tight intercellular junctions, ensuring effective transport of nanocarriers across the epithelium to the blood. 121 In vivo studies conducted in diabetic rats confirmed that the nanocarriers prepared in this way were effectively absorbed and that the encapsulated insulin retained biological activity. The slow insulin release profile from nanocarriers allowed normal blood glucose levels to be maintained up to 12 hours after oral administration. 120 Later, Sun et al proposed a unique synthesis method termed flash nanocomplexation to obtain polyelectrolyte nanocomplexes to deliver insulin. First, insulin-loaded N-(2-hydroxy) -propyl-3-trimethylammonium-7-chloride modified chitosan/sodium tripolyphosphate nanocomplexes were produced as a nanocore. In the next step, they encapsulated nanocores into enteric Eudragit L100-55 polymer (polymer with mucoadhesive properties). Its task is to protect nanocomplexes with the drug against degradation in the digestive system and achieve a specific release of nanocomplexes in the ileum. Importantly, the authors claimed that nanocarrier synthesis's optimized process is a scalable manner allowing easy clinical translation. The effectiveness of the obtained nanocarriers revealed studies on diabetic rats. 122 Nasal polymeric oil-core nanocarriers with shells covered with Eudragit RS100 (poly (ethyl acrylate-co-methyl methacrylate-co-trimethylamine methacrylate chloride) and with encapsulated steroid triamcinolone acetonide revealed excellent efficacy for the treatment of allergic rhinitis. Unique mucoadhesive properties of Eudragit polymers enabled excellent retention of nanocarriers in the nasal cavity, high local absorption of the drug, which limited its systemic distribution, and the resulting side effects. 123 As other numerous studies have shown, polymeric nanocarriers could be used to formulate and deliver a wide variety of anti-inflammatory drugs (Table 4) . Gene therapy is a sophisticated approach to the treatment of different diseases based on nucleic acid delivery. A new method of CRISPR gene editing was developed. Chen et al utilized polymeric nanocarriers to transport the preassembled complex of Cas9 nuclease and a singleguide RNA (Cas RNP), which provided safe and effective CRISPR-mediated therapeutic gene editing. Because Cas RNP was surrounded by oppositely charged polymers, imidazole-containing monomer, covalently crosslinked glutathione, and acrylate methoxy poly(ethylene glycol), nanocarriers underwent endosomal escape followed by cytoplasmatic degradations. Subsequently, Cas RNP was able to enter the nucleus. Moreover, for in vivo experiments, nanocarriers were decorated with all-trans retinoic acid, which binds to the interphotoreceptor retinoidbinding protein. Results obtained for either subretinal or intramuscular injection have shown more effective genome editing compared to unencapsulated Cas RNP. 124 One of the biggest challenges of modern medicine is undoubtedly treating central nervous system diseases such as neurodegenerative disease and cancer. The fundamental problem is a weak blood-brain barrier (BBB) permeability for small molecule drugs and therapeutic proteins. Hence, many studies on developing systems that allow the effective transport of therapeutics through BBB-forming endothelial cells. One of the more interesting approaches is the use of nanocarriers obtained from the degradable crosslinker, poly (lactide) -b-poly (ethylene glycol) -b-poly (lactide) -diacrylate triblock copolymer and 2-methacryloyloxyethyl phosphorylcholine. The latter compound is made of choline and acetylcholine analogs. Receptors for these neurotransmitters are commonly found on cells located within the central nervous system and on endothelial barrier cells of the brain; hence they can facilitate transcytosis of functionalized nanocarriers carrying therapeutic proteins (monoclonal antibodies or growth factors supporting the regeneration of damaged brain areas). 125, 126 Other examples of polymeric nanocarriers transporting drugs for neurological disorders are summarized in Table 5 . Furthermore, polymer nanocarriers have been used to treat various infectious diseases as transporters of antibacterial, antifungal, and anti-parasitic compounds (summarized in Table 6 ). The requirements that medicine places in modern therapies, especially those useful in treating such complex diseases as cancer, chronic inflammatory diseases, or autoimmune diseases, lead scientists to seek more and more advanced therapeutics. Modern therapies are simultaneously based on many drugs, often biochemically different, but their administration is expected to be safe and as low as possible for the patient. Hence the necessity to design biocompatible drug nanocarriers efficiently delivering drugs to the diseased tissue and ensuring their specific release. Recently performed studies indicate that polymeric nanomaterials could help in developing such nanocarriers and therapies of the future. The biocompatible polymers used to synthesize polymeric nanomaterials ensure low toxicity and allow obtaining complex and various nanocarriers. Polymeric nanocarriers are flexible in size, efficiently transport, and rapidly release cargo in the target tissue dependent on pH or temperature stimuli. However, these nanocarriers are often so complicated that it is difficult to predict the cost of mass production and how stable in vivo they would ultimately be. The usefulness of many polymeric nanomaterials has not even been studied in biological systems. Therefore, our knowledge about numerous advanced and complex nanosystems is still low. It is necessary to develop optimal schemes allowing for a detailed characterization of toxicity and verifying these nanomaterials' effectiveness in vivo. Nanostructured porous silicon in preclinical imaging: moving from bench to bedside Key targeting approaches for pharmaceutical drug delivery Vascular permeability in cancer and infection as related to macromolecular drug delivery, with emphasis on the EPR effect for tumor-selective drug targeting Vascular permeability in a human tumor xenograft: molecular size dependence and cutoff size A new concept for macromolecular therapeutics in cancer chemotherapy: mechanism of tumoritropic accumulation of proteins and the antitumor agent smancs Factors and mechanism of "EPR" effect and the enhanced antitumor effects of macromolecular drugs including SMANCS Nanoparticles in the clinic Nanoparticles in the clinic: an update Pharmacokinetics of total and unbound paclitaxel after administration of paclitaxel micellar or nab-paclitaxel: an open, randomized, cross-over, explorative study in breast cancer patients A multi-national, randomised, open-label, parallel, Phase III non-inferiority study comparing NK105 and paclitaxel in metastatic or recurrent breast cancer patients Toward nanotechnology-enabled approaches against the COVID-19 pandemic Immunemediated approaches against COVID-19 Phase 1-2 Trial of a SARS-CoV -2 recombinant spike protein nanoparticle vaccine Multifunctional nanoparticles for multimodal imaging and theragnosis Nanocapsules: the weapons for novel drug delivery systems Nanocapsule technology: a review Polymeric nanocapsules as nanotechnological alternative for drug delivery system: current status, challenges and opportunities Microparticulate drug delivery systems: release kinetic models. Microspheres Microcapsules Liposomes Polymer-based nanocapsules for drug delivery 15 submit your manuscript | www.dovepress.com DovePress 20. Ottenbrite RM, Kim SW. Polymeric Drugs and Drug Delivery Systems Polymeric nanomicelles as versatile tool for multidrug delivery in chemotherapy New developments in liposomal drug delivery Injectable lipid-based depot formulations: where do we stand? Nanoencapsulation I. Methods for preparation of drug-loaded polymeric nanoparticles Nanoencapsulation for drug delivery Biodegradable polymeric nanoparticles as drug delivery devices The application of biomacromolecules to improve oral absorption by enhanced intestinal permeability: A mini-review Self-assembled fluorescent tripeptide nanoparticles for bioimaging and drug delivery applications Near infrared fluorescent peptide nanoparticles for enhancing esophageal cancer therapeutic efficacy An investigation into the role of surfactants in controlling particle size of polymeric nanocapsules containing penicillin-G in double emulsion Multifunctional nanocarriers Nanoparticle-based targeted drug delivery Buildup of ultrathin multilayer films by a self-assembly process: III. Consecutively alternating adsorption of anionic and cationic polyelectrolytes on charged surfaces Fuzzy nanoassemblies: toward layered polymeric multicomposites Multilayers of colloidal particles Layer-by-layer self assembly of polyelectrolytes on colloidal particles Biocompatible long-sustained release oil-core polyelectrolyte nanocarriers: from controlling physical state and stability to biological impact Encapsulation of liquid cores by layer-by-layer adsorption of polyelectrolytes Nanoparticle synthesis in engineered organic nanoscale reactors Monodisperse polyelectrolyte-supported asymmetric lipid-bilayer vesicles Bioinspired colloidal systems via layer-by-layer assembly Which polymers can make nanoparticulate drug carriers long-circulating? Long-circulating and target-specific nanoparticles: theory to practice Surfaces that resist bioadhesion The EPR effect and polymeric drugs: A paradigm shift for cancer chemotherapy in the 21st century stimuli-sensitive nanoparticulate systems for drug delivery Magnetic targeting for site-specific drug delivery: applications and clinical potential Drug targeting Scientific and Clinical Applications of Magnetic Carriers Applications of magnetic nanoparticles in biomedicine Development and experimental use of receptor-specific MR contrast media Characterization of biophysical and metabolic properties of cells labeled with superparamagnetic iron oxide nanoparticles and transfection agent for cellular MR imaging Synthesis and surface engineering of iron oxide nanoparticles for biomedical applications Polymer-Coated Iron Oxide Nanoparticles for Medical Imaging. Massachusetts Institute of Technology Multilayered materials based on biopolymers as drug delivery systems Engineering nanolayered particles for modular drug delivery Layer-By-Layer Films for Biomedical Applications Layer-by-layer engineered capsules and their applications Process for preparing a colloidal and disperse system in the shape of nanocapsules Nanoprecipitation and nanoformulation of polymers: from history to powerful possibilities beyond poly(lactic acid) Nanoparticles based on hydrophobic polysaccharide derivatives-formation principles, characterization techniques, and biomedical applications Physicochemical parameters associated with nanoparticle formation in the salting-out, emulsification-diffusion, and nanoprecipitation methods Synthetic polymeric nanoparticles by nanoprecipitation Nanocapsule formation by interfacial polymer deposition following solvent displacement An overview of nanoemulsion: concepts of development and cosmeceutical applications Nanoemulsions: formation, properties and applications Preparation of polymeric nanocapsules by miniemulsion polymerization Encapsulation through (Mini)Emulsion polymerization Nanoparticles: properties, applications and toxicities Mono-and multilayer covered drops as carriers Doxorubicininduced cardiotoxicity: from mechanisms to development of efficient therapy Explosible nanocapsules excited by pulsed microwaves for efficient thermoacoustic-chemo combination therapy A PEGylated alternating copolymer with oxidation-sensitive phenylboronic ester pendants for anticancer drug delivery Addition of vandetanib to pegylated liposomal doxorubicin (PLD) in patients with recurrent ovarian cancer. A randomized phase I/II study of the AGO study group (AGO-OVAR 2.13) Delayed sequential co-delivery of gefitinib and doxorubicin for targeted combination chemotherapy Incorporation of drug efflux inhibitor and chemotherapeutic agent into an inorganic/organic platform for the effective treatment of multidrug resistant breast cancer The functions and applications of RGD in tumor therapy and tissue engineering Folate receptor-targeted hybrid lipid-core nanocapsules for sequential delivery of doxorubicin and tanespimycin Synthesis of size-tunable hollow polypyrrole nanostructures and their assembly into folate-targeting and pH-responsive anticancer drug-delivery agents Nanoparticle-dendrimer hybrid nanocapsules for therapeutic delivery Magnetic Drug targeting: preclinical in vivo studies, mathematical modeling, and extrapolation to humans Triple-modal imaging of magnetically-targeted nanocapsules in solid tumours in vivo Highly Loaded semipermeable nanocapsules for magnetic resonance imaging Oil core-PEG shell nanocarriers for in vivo MRI imaging Ultrasound molecular imaging of breast cancer in MCF-7 orthotopic mice using gold nanoshelled poly(lactic-co-glycolic acid) nanocapsules: A novel dual-targeted ultrasound contrast agent Thin-shelled PEGylated perfluorooctyl bromide nanocapsules for tumor-targeted ultrasound contrast agent A pH-sensitive nanocarrier for tumor targeting: delivery of ruthenium complex for tumor theranostic by pH-sensitive nanocapsule Nanoparticle-enhanced synergistic HIFU ablation and transarterial chemoembolization for efficient cancer therapy Near-infrared light and tumor microenvironment dual responsive size-switchable nanocapsules for multimodal tumor theranostics Photosensitizer-crosslinked in-situ polymerization on catalase for tumor hypoxia modulation & enhanced photodynamic therapy A cascade-targeting nanocapsule for enhanced photothermal tumor therapy with aid of autophagy inhibition Stimuli responsive PEGylated bismuth selenide hollow nanocapsules for fluorescence/CT imaging and light-driven multimodal tumor therapy Chemodrug-gated biodegradable hollow mesoporous organosilica nanotheranostics for multimodal imaging-guided low-temperature photothermal therapy/chemotherapy of cancer Review on targeting nanoparticles for breast cancer 15 submit your manuscript | www In vivo distribution of polymeric nanoparticles at the whole-body, tumor, and cellular levels Challenges and key considerations of the enhanced permeability and retention effect for nanomedicine drug delivery in oncology Nanodrug delivery: is the enhanced permeability and retention effect sufficient for curing cancer? Stromal biology and therapy in pancreatic cancer Intratumor heterogeneity and branched evolution revealed by multiregion sequencing Early returns from the era of precision medicine Polymeric nanoparticles encapsulating novel TLR7/8 agonists as immunostimulatory adjuvants for enhanced cancer immunotherapy Polymeric nanoparticles enable reversing macrophage in tumor microenvironment for immunotherapy In situ modification of the tumor cell surface with immunomodulating nanoparticles for effective suppression of tumor growth in mice Vaccine delivery: A matter of size, geometry, kinetics and molecular patterns Polymeric nanocapsules for vaccine delivery: influence of the polymeric shell on the interaction with the immune system Bilayer polymeric nanocapsules: a formulation approach for a thermostable and adjuvanted E. coli antigen vaccine Multi-enveloping of particulated antigens with biopolymers and immunostimulant polynucleotides Co-delivery of viral proteins and a TLR7 agonist from polysaccharide nanocapsules: A needle-free vaccination strategy Polymeric hepatitis C virus non-structural protein 5A nanocapsules induce intrahepatic antigen-specific immune responses Biodegradable antigen-associated PLG nanoparticles tolerize Th2-mediated allergic airway inflammation pre-and postsensitization Chitosan hydrogels containing nanoencapsulated phenytoin for cutaneous use: skin permeation/penetration and efficacy in wound healing Hybrid hydrogel composed of polymeric nanocapsules co-loading lidocaine and prilocaine for topical intraoral anesthesia Fabrication of core-shell nanofibers for controlled delivery of bromelain and salvianolic acid B for skin regeneration in wound therapeutics Growth-factor nanocapsules that enable tunable controlled release for bone regeneration Intracellular delivery of poorly soluble polyphenols: elucidating the interplay of self-assembling nanocarriers and human chondrocytes A novel approach to arthritis treatment based on resveratrol and curcumin co-encapsulated in lipid-core nanocapsules: in vivo studies Development of PEI-RANK siRNA complex loaded PLGA nanocapsules for the treatment of osteoporosis Using the interplay of magnetic guidance and controlled TGF-β release from protein-based nanocapsules to stimulate chondrogenesis Polymeric nanocapsules: a potential new therapy for corneal wound healing ZOT-derived peptide and chitosan functionalized nanocarrier for oral delivery of protein drug Zonula occludin toxin, a microtubule binding protein Scalable manufacturing of enteric encapsulation systems for site-specific oral insulin delivery Rationally designed nanocarriers for intranasal therapy of allergic rhinitis: influence of carrier type on in vivo nasal deposition A biodegradable nanocapsule delivers a Cas9 ribonucleoprotein complex for in vivo genome editing A bioinspired platform for effective delivery of protein therapeutics to the central nervous system Efficient delivery of nerve growth factors to the central nervous system for neural regeneration 2-(2-Methoxyphenyl)-3-((Piperidin-1-yl)ethyl)thiazolidin-4-oneloaded polymeric nanocapsules: in vitro antiglioma activity and in vivo toxicity evaluation Antitumor action of diphenyl diselenide nanocapsules: in vitro assessments and preclinical evidence in an animal model of glioblastoma multiforme Mitochondria targeting non-isocyanate-based polyurethane nanocapsules for enzyme-triggered drug release Near-infrared triggered decomposition of nanocapsules with high tumor accumulation and stimuli responsive fast elimination Polyarginine nanocapsules as a potential oral peptide delivery carrier PEGylated polypeptide lipid nanocapsules to enhance the anticancer efficacy of erlotinib in non-small cell lung cancer Preparation and evaluation of etoposide-loaded lipid-based nanosuspensions for high-dose treatment of lymphoma Novel therapeutic mechanisms determine the effectiveness of lipid-core nanocapsules on melanoma models PEGylated squalenoyl-gemcitabine nanoparticles for the treatment of glioblastoma Polymeric glabrescione B nanocapsules for passive targeting of Hedgehog-dependent tumor therapy Mechanisms of the effectiveness of poly(ε-caprolactone) lipid-core nanocapsules loaded with methotrexate on glioblastoma multiforme treatment Nanoencapsulation of psoralidin via chitosan and Eudragit S100 for enhancement of oral bioavailability Resveratrol-loaded nanocapsules inhibit murine melanoma tumor growth Tamoxifen citrate-loaded poly(d,l) lactic acid nanoparticles: evaluation for their anticancer activity in vitro and in vivo New insight into Polydopamine@ZIF-8 Nanohybrids: a zinc-releasing container for potential anticancer activity Nano-co-delivery of berberine and anticancer drug using PLGA nanoparticles: exploration of better anticancer activity and in vivo kinetics Selol nanocapsules with a poly(methyl vinyl ether-co-maleic anhydride) shell conjugated to doxorubicin for combinatorial chemotherapy against murine breast adenocarcinoma in vivo Preparation of biodegradable polymeric nanocapsules for treatment of malignant tumor using coaxial capillary microfluidic device PEGylated lipid bilayer coated mesoporous silica nanoparticles co-delivery of paclitaxel and curcumin leads to increased tumor site drug accumulation and reduced tumor burden Paclitaxel-loaded PEGylated nanocapsules of perfluorooctyl bromide as theranostic agents Ultrasound-induced mild hyperthermia improves the anticancer efficacy of both Taxol ® and paclitaxel-loaded nanocapsules Design of a liquid nano-sized drug delivery system with enhanced solubility of rivaroxaban for venous thromboembolism management in paediatric patients and emergency cases Antidiabetic activity enhancement in streptozotocin + nicotinamide-induced diabetic rats through combinational polymeric nanoformulation Studies on core-shell nanocapsules of felodipine: in vitro-in vivo evaluations In vivo evaluation of enhanced drug carrier efficiency and cardiac anti-hypertrophy therapeutic potential of nano-curcumin encapsulated photo-plasmonic nanoparticles combined polymerized nano-vesicles: A novel strategy Longlasting anti-platelet activity of cilostazol from poly(εcaprolactone)-poly(ethylene glycol) blend nanocapsules Budesonideloaded Eudragit S 100 nanocapsules for the treatment of acetic acid-induced colitis in animal model Curcumin entrapped hyaluronan containing niosomes: preparation, characterisation and in vitro/in vivo evaluation Starch nanocapsules containing a novel neutrophil elastase inhibitor with improved pharmaceutical performance Anti-inflammatory effect of nano-encapsulated nerolidol on zymosan-induced arthritis in mice Orally delivered resveratrol-loaded lipid-core nanocapsules ameliorate LPS-induced acute lung injury via the ERK and PI3K/Akt pathways PEGylated meloxicam-loaded nanocapsules reverse in vitro damage on caspase activity and do not induce toxicity in cultured human lymphocytes and mice Enhanced pharmacological actions of p,p'-methoxyl-diphenyl diselenide-loaded polymeric nanocapsules in a mouse model of neuropathic pain: behavioral and molecular insights 15 submit your manuscript | www A surface modification of clozapine-loaded nanocapsules improves their efficacy: a study of formulation development and biological assessment NFL-lipid nanocapsules for brain neural stem cell targeting in vitro and in vivo Triphenyl phosphonium coated nano-quercetin for oral delivery: neuroprotective effects in attenuating age related global moderate cerebral ischemia reperfusion injury in rats The nasal delivery of nanoencapsulated statins -an approach for brain delivery Effect of free and nano-encapsulated curcumin on treatment and energetic metabolism of gerbils infected by Listeria monocytogenes Design and evaluation of pH-dependent nanosystems based on cellulose acetate phthalate, nanoparticles loaded with chlorhexidine for periodontal treatment In vivo vaginal fungal load reduction after treatment with itraconazole-loaded polycaprolactone-nanoparticles Lychnopholide in poly(D,L-lactide)-block-polyethylene glycol nanocapsules cures infection with a drug-resistant Trypanosoma cruzi strain at acute and chronic phases Biodegradable polymeric nanocapsules prevent cardiotoxicity of anti-trypanosomal lychnopholide Efficacy of lychnopholide polymeric nanocapsules after oral and intravenous administration in murine experimental Chagas disease Lipid-core nanocapsules increase the oral efficacy of quercetin in cutaneous leishmaniasis Effects of surface characteristics of polymeric nanocapsules on the pharmacokinetics and efficacy of antimalarial quinine Artesunate-heparin conjugate based nanocapsules with improved pharmacokinetics to combat malaria Conanoencapsulation of antimalarial drugs increases their in vitro efficacy against Plasmodium falciparum and decreases their toxicity to Caenorhabditis elegans Optimization of curcuma oil/quinine-loaded nanocapsules for malaria treatment Reduced cardiotoxicity and increased oral efficacy of artemether polymeric nanocapsules in Plasmodium berghei-infected mice KSz acknowledges financial assistance from the statutory research fund of ICSC PAS. The authors report no conflicts of interest in this work.