key: cord-0750405-uajretl7
authors: Ortona, Elena; Malorni, Walter
title: Long COVID: to investigate immunological mechanisms and sex/gender related aspects as fundamental steps for a tailored therapy
date: 2021-09-16
journal: Eur Respir J
DOI: 10.1183/13993003.02245-2021
sha: bb1411e364b451a3248208b5337af479c497ab2b
doc_id: 750405
cord_uid: uajretl7

Long COVID was detected in both adults and children and is characterized by immunological dysregulation. Autoimmune reactions in adult patients and allergic reactions in children appear as critical factors.

dysfunction (brain fog), tachycardia, intestinal disorders and skin manifestations. It can affect anyone but women appear to be twice as likely to develop Long COVID as men, but only until around age 60, when the risk level becomes similar [2] [3] [4] . Long COVID has also been described in paediatric age [5] . An Italian study reported that at least one symptom persisted 4 months after COVID-19 infection [6] whereas an Australian analysis suggested that only 8% of children had ongoing symptoms 3-6 months after mild SARS-Cov-2 infection [7] . No gender difference was observed in the prevalence of Long-COVID in this population [5] .

Long COVID etiology. The Long COVID syndrome has a similarity to the postinfectious syndromes that followed the outbreaks of chikungunya [8] and Ebola [9] .

What are the factors responsible for this syndrome? They could be many and different. Organ damage caused by an excessive inflammatory response activated by the virus, persistent reservoirs of SARS-CoV-2 in certain tissues that could trigger post-infection morbidity, re-activation of pathogens due to immune dysregulation, host microbiome alterations, clotting/coagulation issues and autoimmunity due to molecular mimicry between SARS-CoV-2 and self-proteins have been hypothesized to play a role [10] . Furthermore, it has also been suggested that Long COVID symptoms may not be a direct result of the SARS-CoV-2 infection but may be the consequence of COVID-19 inflammation-induced Epstein Bar virus reactivation [11] . The search for fine molecular mechanisms underlying Long COVID is also underway. Some insights derive from metabolic studies, e.g. an altered tryptophan absorption and metabolism that could underlie the post-infection disease [12] , whereas further hypotheses derive from cytopathological studies that suggest that SARS-CoV-2 could be capable of hindering autophagic processes of host cells thus favouring the "journey" of viral particles inside the cell cytoplasm and their survival. As a consequence, it has been argued that modulators of cellular metabolism or agents bolstering autophagy could represent a therapeutic strategy against post-COVID sequelae helping to eliminate viral particles or fragments potentially immunogenic and active [13] . However, to date, the plethora of different Long COVID symptoms and disturbs seems to indicate that different concurrent mechanisms could be involved ( Figure 1) and that different therapeutic approaches should be settled in order to cure these patients.

As concerns paediatric population, clinical data on Long COVID-19 are limited. The most common complications were muscle and/or joint pain, headache, chest pain or a feeling of chest tightness, palpitations, respiratory problems and sleep disturbances [5, 6] . In their study, Osmanov and co-workers [5] , thanks to a standardized follow-up data collection protocol developed by the International Severe Acute Respiratory and Emerging Infection Consortium (ISARIC)

[https://isaric.org/research/covid-19-clinical-research-498 resources/paediatricfollow-up/], observed that older age and allergic diseases were associated with higher risk of persistent symptoms at follow-up. Osmanov and colleagues suggested that, at least in children, immunological mechanisms may be responsible for an increased risk of long-term consequences of infection. In particular, COVID-19 sequelae could be linked with the mast cell activation syndrome and the Th-2 biased immunological response in children with allergic diseases [5] . Importantly, these findings are in line with a recent case report describing an adolescent with persisting symptoms with first documentation of ongoing immune dysfunction and lung perfusion defects after mild COVID-19 [14] .

Gender disparity: a "Black hole" for Long COVID. As mentioned above, Long COVID and its symptoms reporting is more frequent by women than men [2] . This is both a gender and sex disparity that is being discussed and underscored from public health policy makers in different terms. One deals with the fact that women frequently pay more attention to their body and to its alterations. This often leads to a more rapid diagnostic and therapeutic intervention. Unfortunately, there is also "a school of thought" sustaining that the Long COVID gender skew could simply represent an artefact: it could just be conceived by "hysterical, middleaged women". This sexist approach could certainly represent a strong bias from both an ethical and a clinical point of view and it could also impact the healthcare and working rights for female patients with Long COVID.

Actually, females have both innate and acquired immunological responses stronger than males and both genes and hormones are involved in this sex difference [15, 16] . These sex-based immunological differences contribute to variations in the incidence of autoimmune diseases, higher in females than in males and in susceptibility to malignancies and infectious diseases, more frequent in males than in females, and probably represent the major cause of female prevalence of Long COVID in adults. Finally, as happens with Lyme disease in which the pathogen remains hided and generates higher levels of inflammatory cytokines in women than men [17] , it can be hypothesized that fragments of SARS-Cov-2 could remain hidden on reservoirs such as kidney or brain igniting some chronic inflammation-associated cascade giving rise to symptoms such as pain or brain fog experienced by patients with Long COVID. Importantly, as mentioned above, no significant difference was reported to date between youngest male and female patients [5] . This could reinforce the hypothesis that sex hormones and their immunomodulating activity could play a role in adult Long COVID patients [18, 19] .

Autoimmunity and Long COVID. It has been observed that, compared with uninfected controls and as for Epstein-Barr virus, cytomegalovirus and human immunodeficiency virus, SARS-Cov-2 infection is associated with the generation of a wide range autoantibodies that can attack tissues of infected subjects [20] .

Some of the infected individuals had autoantibodies against proteins involved in several immunological activities including interferon responses, leukocyte trafficking, and lymphocyte function/activation [21] . Other autoantibodies are tissue-specific including autoantibodies specific to blood vessels, heart and brain.

The propensity of patients to develop over 15 separate types of autoantibodies and above 10 distinct autoimmune diseases have been observed [22] . The main mechanisms that may contribute to the development of autoimmunity in COVID-19 are the following: i) the hyper-activation the immune system, ii) the induction of excessive neutrophil extracellular traps formation, and iii) SARS-CoV-2 crossreaction with self-components of the host. In fact, SARS-CoV-2 has been shown to cross-react with gut, kidney, lung, heart, and brain antigens and SARS-CoV-2 proteins can share homology with some self-protein epitopes leading to molecular mimicry paths [22] . Furthermore, under conditions of inflammation, other organisms of the microbiome/virome communities, that could vary widely between different patients, may also contribute to autoantibody production and cause the great variety of autoantibody reactivity. This complex scenario could explain the significant percentage of clinical variations detected in patients with Long COVID Conclusions. Long COVID is characterized by specific long-lasting inflammatory/immunological dysregulation and can not be considered as a unique pathology but a huge series of different morbidity states. Hence, a better understanding of the heterogeneity of this pathology, assessing the appearance of autoantibodies in the serum of adult patients, in particular women, and evaluating the Th2 immune response and plasma IgE levels in children could be an important goal to begin to identify personalized and specific treatments for patients with Long COVID.

Longterm consequences of COVID-19: research needs

Attributes and predictors of long COVID

Defining Post-COVID symptoms (Post-Acute COVID, Long COVID, Persistent Post-COVID): an integrative classification

Fresh evidence of the scale and scope of Long COVID

Risk factors for long covid in previously hospitalised children using the ISARIC Global follow-up protocol: A prospective cohort study

Preliminary evidence on long COVID in children

Post-acute COVID-19 outcomes in children with mild and asymptomatic disease

Chikungunya-induced arthritis in Reunion Island: a Long-term observational follow-up study showing frequently persistent joint symptoms, some cases of persistent chikungunya immunoglobulin M positivity, and no anticyclic citrullinated peptide seroconversion after 13 years

Long-term sequelae after Ebola virus disease in Bundibugyo, Uganda: a retrospective cohort study

Long COVID or Post-acute Sequelae of COVID-19 (PASC): An Overview of Biological Factors That May Contribute to Persistent Symptoms

Investigation of Long COVID Prevalence and Its Relationship to Epstein-Barr Virus Reactivation

Altered tryptophan absorption and metabolism could underlie long-term symptoms in survivors of coronavirus disease 2019 (COVID-19)

SARS-CoV-2-mediated dysregulation of metabolism and autophagy uncovers host-targeting antivirals

Evidence of lung perfusion defects and ongoing inflammation in an adolescent with post-acute sequelae of SARS-CoV-2 infection

Immune response and autoimmune diseases: a matter of sex

Sex differences in immune responses

Lyme borreliosis reinfection: might it be explained by a gender difference in immune response

Immunological aspects and gender bias during respiratory viral infections including novel Coronavirus disease-19 (COVID-19): A scoping review

Long Covid Kids study group. Long COVID: an estrogen-associated autoimmune disease?

Rogue antibodies could be driving severe COVID-19

Diverse functional autoantibodies in patients with COVID-19

The SARS-CoV-2 as an instrumental trigger of autoimmunity