key: cord-0053040-g0wrspho authors: Kaslow, David C. title: Malaria vaccine research & innovation: the intersection of IA2030 and zero malaria date: 2020-11-20 journal: NPJ Vaccines DOI: 10.1038/s41541-020-00259-3 sha: 89ab856a895b768e5d8106609cd42e61e3be7416 doc_id: 53040 cord_uid: g0wrspho nan PROBLEM AND OPPORTUNITY STATEMENT Despite a~30% reduction in clinical cases and~60% reduction in lives lost from Plasmodium ssp. infections over the past two decades, malaria continues to relentlessly sap the well-being of an estimated 228 million people worldwide (95% confidence interval [CI] : 206-258 million) and result in the global demise of an estimated 405,000 persons annually. The effort, supported by a US$ 2.7-3.2 billion annual investment, to "bend the curve" towards zero malaria by 2030 has stalled over the past five years 4 . This plateau is reminiscent of the decades-long effort to break through the~80% ceiling on reaching the goal of fully immunizing every child worldwide. Despite immunization of 116 million children annually, 20 million infants fail to receive a full course of essential vaccines and 13 million infants receive no vaccines whatsoever-these "zero dose" children are highlighted in the Immunization Agenda 2030 3 (IA2030), recently adopted by the World Health Assembly 5 . The shared state of stalled progress towards equity and coverage of effective malaria interventions and essential vaccines has a common solution-new tools. The early promise of innovative vector control and single-dose radical cure for malaria have yet to deliver the impact needed to achieve "zero malaria". That said, steadily over the last two decades, as reviewed by Duffy and Gorres, a pipeline of vaccine candidates against the most lethal human malaria, P. falciparum, and the most prevalent, P. vivax, has been assembled 6 . Novel vaccine platforms (e.g., P. berghei sporozoite-based human vaccine candidates 7 ), better defined correlates of protection in nonhuman primates 8 , and orthogonal learnings from other mosquitotransmitted pathogens (e.g., West Nile Virus) 9 portend an even more robust pipeline of needed new tools, if adequate investments are made. Malaria vaccine targets are typically assigned to one of three sequential stages of the parasite's lifecycle: blood stage-through which the parasite causes all human pathology; sexual and sporogony stage-through which the parasite is transmitted from human host to female mosquito vector; and, pre-erythrocytic stage-through which the parasite infects humans during a subsequent bloodmeal by an infected mosquito (see Fig. 1 , ref. 6 ). Despite decades of efforts directed against targets throughout the lifecycle, only one vaccine candidate, the pre-erythrocytic circumsporozoite (CSP)-based RTS,S/AS01 E , has advanced through licensure and pilot implementation 6 . A myriad of biological and technical barriers have been encountered; however, step-by-step, these barriers have been chipped away. Advances include: new insights into the evolution of the immune response to the major pre-erythrocytic target, CSP 10 , and into the role of complementfixing antibodies in blood stage clinical immunity 11 ; the ability to express and manufacture full length versions of blood stage targets, e.g., the highly promising, highly conserved reticulocytebinding protein homolog 5 (PfRH5) 12 , as well as the 196-kDa merozoite surface protein 1 (the primary structure first described by Holder, et al. in 1985 13 ) , the latter of which demonstrated favorable safety and immunogenicity in a first-in human study 14 ; and, the delivery of target malaria parasite antigens by measles vectors to overcome the barrier of waning immune responses, resulting in durable memory and protection, at least in a murine model 15 . To be clear, significant challenges remain-for example, immune interference when concomitantly administering other vaccines, such as BCG for tuberculosis 16 , or administering multistage targets by multiple vaccine platforms, as observed with an adjuvanted virus-like particle, RTS,S/AS01 B , and viral-vectors expressing the multiple-epitope thrombospondin-related adhesion protein (ME-TRAP) 17 . That said, molecular approaches to identify and direct immune responses to specific promising epitopes 18 and use of novel particle-forming lipid-based adjuvants 19 provide paths forward for poorly immunogenic targets, including those designed to interrupt transmission from human to mosquito. The longstanding mindset that vaccine evaluation during pregnancy should be delayed to post-licensure studies is obsolete. Even when pregnant women and their offspring do not have a higher risk of disease, there is an ethical rationale to evaluate at least vaccine safety pre-licensure 20 . Pregnancy malaria presents an even clearer case for prioritizing vaccine development as both mother and offspring have a well-described higher risk of disease 6 . More than two decades ago, antibodies to VAR2CSA, a member of the P. falciparum erythrocyte membrane protein 1 (PfEMP1) family, were associated with protection, identifying VAR2CSA as a promising vaccine target 21 . Placenta malaria vaccine (PMVs) research and innovation continues to progress 6 , including through the development of new animal models 22 and down-selection of lead PVM candidates 23 . Despite being the most prevalent human malaria parasite, investments in P. vivax vaccine development have been significantly smaller than that in the more lethal, albeit similarly morbid, falciparum cousin. Many P. falciparum vaccine targets have homologs in P. vivax 6 , so a fast follow-on vivax malaria vaccines based on safe, effective, affordable falciparum malaria vaccines have a reasonable, high likelihood of success. That said, several distinct differences in P. vivax biology, such as liver stage hypnozoites and rapid development of sexual stages directly from liver schizonts, require a P. vivax-specific vaccine research and innovation strategy. A critical differential feature of blood-stage vivax parasites is the use of Duffy antigen receptor for chemokines (DARCs) on human reticulocytes as a major invasion pathway. Recent insights into the structural basis of anti-P. vivax Duffy Binding Domain (PvDBP) immunity 24, 25 and early clinical results from a PvDBP vaccine candidate 26 are encouraging; however, given the parasite's gene amplification mechanisms to evade anti-PvDBP immunity 27 , developing a blood stage vivax malaria vaccine won't be trivial. The promising P. falciparum and P. vivax vaccine pipeline faces a significant resource shortfall as candidates head into late-stage development-this increasingly more apparent resource gap, or second "Valley of Death", is also faced by most, if not all, late stage vaccine candidates for pathogens afflicting primarily those living in low resource settings 28 . Hopefully, the recent global adoption of the Research and Innovation pillar of IA2030 and the growing African continent-led commitment to zero malaria will lead to the investments needed to generate the evidence that support the compelling value proposition required to build bridges for promising malaria vaccine candidates to become affordable, effective, sustainable new tools-part of the solution to regain the prior trajectory towards zero malaria. ✉ email: dkaslow@path.org Malaria Starts with Me (RBM & UNOPS Partnership to End Malaria Annual Report 2019 (RBM & UNOPS WHO. 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Vaccine S0264-410X Maternal antibodies block malaria Malaria in pregnancy: the relevance of animal models for vaccine development Down-selection of the VAR2CSA DBL1-2 expressed in E. coli as a lead antigen for placental malaria vaccine development Structural basis for inhibition of Plasmodium vivax invasion by a broadly neutralizing vaccine-induced human antibody Structural basis for neutralization of Plasmodium vivax by naturally acquired human antibodies that target DBP Malaria vaccine candidate based on Duffy-binding protein elicits strain transcending functional antibodies in a Phase I trial Amplification of Duffy binding protein-encoding gene allows Plasmodium vivax to evade host anti-DBP humoral immunity Vaccine candidates for poor nations are going to waste DCK conceived, wrote, reviewed, approved submission of, and is accountable for this paper. DCK is an employee of PATH (a not-for-profit organization), has no financial interest in any for-profit organization, and declares no competing interests. PATH is funded to innovate and partner in developing and implementing malaria vaccines and other interventions to control and eliminate malaria. Correspondence and requests for materials should be addressed to D.C.K.Reprints and permission information is available at http://www.nature.com/ reprintsPublisher's note Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. 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