Abstract
Human endogenous retroviruses (HERVs) are genetic elements, derived from their exogenous retroviral counterpart by a process of germline infection and proliferation within the human genome, and their integration as proviruses led to the fixation and the vertical transmission, following Mendelian laws. HERVs currently make up ~8% of the genetic material, and some of them have been cooped for physiological functions. Otherwise, their activation in response to environmental factors has been associated with human pathological conditions. In the setting of neurodevelopmental disorders, HERVs have been proposed as contributing factors involved in Autism Spectrum Disorders (ASD), spanning the bridge between genetic susceptibility, environmental risk factors and immune response. We described a distinct expression profile of some HERV families and cytokines in lymphocytes from autistic children and in their mothers suggesting a close mother-child association in ASD. Moreover, in vitro treatment with an antiretroviral drug was able to restore the expression level of HERVs and cytokines providing new insights into the potential role of HERVs as biomarkers of ASD and raising the possibility of using HERVs expression as a therapeutic target for a tailored approach to patient care.
Keywords
- human endogenous retroviruses; HERVs
- biomarker
- mother-child association
- gene expression
- aetiology
- antiretrovirals
1. Introduction
In 1943, the child psychiatrist Leo Kanner described children preferring loneliness with repetitive patterns of behaviour. Similar symptoms were reported by Hans Asperger, an Austrian paediatrician, in 1944 mainly in people of high intelligence [1]. Kanner, first spoke about ‘childhood or early-onset schizophrenia’, and later he called this condition ‘infantile autism’, and concerning the aetiology of autism, he attributed autism to a lack of maternal warmth and attachment. Following this hypothesis, Bruno Bettelheim with his book ‘The Empty Fortress’ popularized the theory of ‘refrigerator mother’ by stating that ‘the infant that misreads the mother’s actions or feelings, or correctly assesses her negative feelings, may retreat from her and the world’. This view was widely criticized and nowadays represents an obsolete thought [2]. From this time, many hypotheses and models emerged to explain this complex condition focusing on symptomatology, phenotype and pathogenesis [3, 4]. However, despite many promising hypotheses, the current literature is made up of controversial findings and lacking of definitive proof about the mechanism underlying the complex aethiopathogenesis of Autism Spectrum Disorder (ASD). ASD is currently referred to as a pervasive neurodevelopmental disorder with an impact on emotional and social behaviour that persists throughout life [5]. The clinical presentation is very heterogeneous, and its incidence is continuously increasing [6]. Despite the consolidated evidence that the main contribution to the increase in the incidence of autism comes from the improvement of the diagnostic process, it has also been hypothesized that at the basis of the onset of autism, there is not a single cause but a set of risk factors acting together to produce the phenotype. Decades of studies have indeed shown that autism is a complex pathology influenced by the combination of genetic, environmental and epigenetic factors, mainly acting during prenatal and/or perinatal phases [7, 8, 9]. The concordance rate of ASD in monozygotic twins much higher than in dizygotic twins seemed to indicate that genetic factors were more likely to contribute to ASD than environmental factors [10]. More than a thousand ASD-associated genes known to be involved in brain development have been identified to date [11], and many genomic copy number variants have been associated with neurodevelopmental disorders including ASD [12, 13]. Several epidemiological studies indicate that potential risk factors for ASD also include various determinants [14, 15], such as the age of the pregnant woman, advancing paternal age [14, 16, 17] and prematurity [18]. However, an ever increasing important role has been attributed to risk factors related to the early foetal environment, including toxicants, diet, air pollution, smoking or chemicals exposure, which have been suggested to induce a prenatal and/or perinatal brain insult able to contribute to the development of autism in genetically predisposed individuals [19]. These environmental insults share in common the activation of the maternal immune system (MIA), which has therefore been recognized as an additional risk factor for ASD [20]. MIA is an inflammatory response triggered by pathogenic infection and autoimmune diseases in the mother. It is known that several microorganisms, vertically transmitted to the foetus, affect its development resulting in severe complications such as miscarriage and malformations [21]. However, even non-vertically transmitted infections during pregnancy can cause harm to the offspring by producing inflammatory cytokines, which directly damage the foetal brain by crossing the placental and blood-brain barrier [22, 23].
Preclinical studies, using mouse model of MIA induced by prenatal exposure to polyinosinic:polycytidylic acid (Poly I:C), a synthetic double-stranded RNA molecule targeting TLR-3, mimicking viral maternal infection, demonstrated that the exposure to a prenatal insult induced derailed neurodevelopment in offspring. Particularly, in the mothers, the Poly I:C injection leads to the production of interleukin-17 that reaches the foetal brain
Within this interplay among genetic susceptibility, MIA, epigenetic and environmental factors are placed the human endogenous retroviruses (HERVs), which we proposed as novel contributing factors involved in ASD.
2. Human endogenous retroviruses and their co-evolution with the host
In contrast to the prevailing early twentieth century conception of genetic material as fixed, in the 1940s, the Nobel Prize Barbara McClintock discovered in maize the ‘mutable loci’ which were capable to move between chromosomes. This pioneering study paved the way for future research into the role of these ‘jumping genes’ or transposable elements (TEs) in both health and disease conditions [31]. Indeed, it was later discovered that about 46% of the human genome consists of TEs [32]. They consist of repetitive sequences that are able to insert copies of themselves elsewhere in the genome [33]. They are divided, according to their size and functionally related structures, into short interspersed elements (SINEs), long interspersed elements (LINEs), long terminal repetition retrotransposons (LTR) and DNA transposons [34]. The major subset of LTR retrotransposons is represented by HERVs, which together with their derivative sequences comprise at least 8% of the human genome [32, 35].
These elements have their origin in the numerous environmental events that shaped the human genome during evolution, including the occasional infection of germ cells of our ancestors by exogenous retroviruses and the insertion of their RNA genome as proviruses into the cell’s chromosomal DNA [36]. Hence, HERVs are transmitted in a Mendelian manner to all subsequent generations (Figure 1a). Retroviral proviruses share the canonical structure of retroviruses consisting of an internal region of four essential viral genes (gag, pro, pol and env), flanked at either side by long terminal repeats sequences (the 5′ and 3′ LTRs) that are identical at the time of integration and contain promoter, enhancer and polyadenylation signals that shape the cellular transcriptome (Figure 1a) [37].
A non-coding sequence containing a tRNA-specifc primer-binding site (PBS) is usually present between the end of the 5′ LTR and the first codon of the gag gene, and HERVs are classified into families on the basis of the tRNA that binds to the viral primer-binding site to prime reverse transcription.
During human evolution, HERVs invaded the human genome undergoing amplification, retrotransposition and/or reinfection events, and resulting in the presence of multiple copies fixed in the DNA of all nucleated cells [36]. While a majority of these sequences have accumulated mutations and/or deletions and are mostly defective, several HERVs preserve the properties of the ancient viruses and, still being transcriptionally active and competent to produce some retroviral proteins, have been co-opted for physiological functions [36, 38, 39] (Figure 1a). In the light of the current knowledge, what Weiss stated in 2016 ‘If Charles Darwin reappeared today, he might be surprised to learn that humans are descended from viruses as well as from apes’ [40] is still current.
3. The role of human endogenous retroviruses in physiological conditions
For a long time, HERVs have been considered as junk DNA with no impact on the host. However, during the last decades, the great efforts of the scientific community highlighted that some ‘well preserved’ ERV sequences influence different physiological properties being involved in a variety of biological pathways [41, 42]. The most intriguingly example of the co-option of HERVs during the host evolution comes from the well-studied properties of the syncytins, the products of the Envelope (Env) genes of HERV-W-1 and HERV-FRD. Specifically, Syncytin-1, encoded by the HERV-W-1 gene, is the first retroviral protein found to have a defined physiological function mediating the cell-cell fusion as the terminal differentiation of the trophoblast lineage [43]. As emerging from different reports, the decrease of syncytin expression and the consequential fusion deficiency could contribute to placental anomalies including pre-eclampsia disorder [44]. Moreover, other studies suggested that syncytin-1 also possesses non-fusogenic activities, as the regulation of trophoblast proliferation and apoptosis and indicated a widely expression in different cell types such as granulocytes, T lymphocytes, monocytes, glial cell of the brain and cancer cells [45, 46]. In human, syncytin-1 interacts with the type D mammalian retrovirus receptor ASCT-1/ASCT-2 (sodium-dependent neutral amino acid transporter type 1/2) on cell membranes. Syncytin-2, encoded by the HERV-FRD gene, is also expressed in trophoblasts and able of mediating cell fusion by interacting with a different receptor known as MFSD2 (major facilitator superfamily domain containing 2) [47, 48]. Moreover, Syncytin-2 is involved in maternal immune tolerance towards the semi-allogenic foetus [49]. A similar functional domestication emerged for ERV-encoded GAG gene, involved in the memory consolidation in the mammalian brain, including long-term potentiation and depression [50]. Given the abundance of HERVs in the human genome, they represent an important source of genomic variability, also providing potential coding and regulatory elements for the acquisition of new cellular functions [51, 52]. In line, growing evidence has been obtained regarding the general expression of HERVs in normal tissues [53, 54], and in this context, we demonstrated an age-related transcriptional activity of HERV-H, HERV-K and HERV-W in peripheral blood mononuclear cells (PBMCs) from a large cohort of healthy human subjects aged between 1 and 80 years, reinforcing the hypothesis of a physiological correlation between HERV activity and the different stages of life in human [55]. Among the proposed mechanisms by which HERVs could contribute to the human physiology, it is recognized that various sequences, concentrated in the LTRs, are involved in the regulation of the expression of neighbouring genes acting as promoters, enhancers, polyadenylation signals, regulators of chromatin folding and binding sites for transcriptional factors [56, 57]. In the genome, most HERVs reside as solo-LTRs, resulting from homologous recombination between the LTRs of a full-length HERV [58] able to act as alternative tissue-specific promoters to drive the expression of host genes [59, 60, 61]. During embryo development, some HERV sequences are also engaged by the host for the regulation of gene expression [62]. In particular, non-coding RNA expressed by the HERV-H group and the recruitment of specific cellular transcriptional factors on HERV-H LTRs seem to be involved in the conservation of stem cell identity [57, 63]. Of note, the HERV-H loci seem to be more preserved in a full-length state than other HERV families, suggesting that the full-length elements rather than solo-LTRs are useful to the host and that the internal regions of HERV-H may be involved in the process of exaptation [64]. Similarly, an ancestral env gene named HEMO [human endogenous MER34 (medium reiteration-frequency-family-34) ORF] has been found highly expressed in embryos, already in the early stages of development and in all subsequent differentiation periods as well as in the placenta and in the blood of pregnant women [65]. Finally, in the regulation of stem cell function, HERV-K ENV was highly expressed in the cell membrane of pluripotent stem cells and signals
To conclude, the more profound insight into the mechanisms explaining the roles of HERVs in various biological/physiological contexts will help to clarify the contribution of HERVs in pathological conditions.
4. The activation of human endogenous retroviruses
In addition to their physiological role, HERVs have been also proposed as possible cofactors in the aetiology of several human diseases. Proviruses are known to remain dormant for long periods of time within the host, but they may occasionally be triggered by factors present in the environment. Indeed, one of the peculiar features of HERVs is their intrinsic responsiveness to microenvironmental stress and various stimuli likely
Thus, HERVs have been found particularly responsive to environmental stimuli that can determine their dysregulation at transcriptional levels and/or encoded protein expression that could influence the onset of complex diseases.
5. The contribution of human endogenous retroviruses in disease development
HERV expression is tightly controlled in normal adult tissues but is reported to be aberrantly expressed in cancer [68], inflammatory and autoimmune diseases [91], aging [92], type 1 diabetes [93] neurological disorders [94] and recently also viral disease [83, 95, 96]. Most of the diseases in which HERVs play a role as cofactor are characterized by a multifactorial aetiology and an inflammatory landscape. As such, HERVs have been proposed as spanning the bridge between environment and genetic background and as shapers of the immune system.
5.1 Human endogenous retroviruses as shapers of the immune system
HERVs can modulate the human immune response by different mechanism. In fact, being integrated as proviruses within the genome and physiologically expressed, HERV antigens can be recognized by the innate immune system as ‘self-determinants’ but also as potential pathogens. Probably due to their similarity with exogenous viral proteins they are able to activate pathogen recognition receptors (PRRs) by evoking the production of pro-inflammatory mediators (such as IFN, cytokines and chemokines), which in turn can activate and trigger the adaptive immune response [42]. Moreover, the involvement of HERVs in the host antiviral immune system seems to be linked to the Interferon pathway by acting as enhancer elements to directly affect the expression of adjacent interferon-stimulated genes [53, 54, 97]. Since HERVs are an integral part of host immunity, they protect the host from exogenous retroviral infections by PRRs, of which a major class are the Toll-like receptors (TLRs), the first line of defence in detecting a wide variety of pathogens. TLRs’ engagements with viral components lead to the activation of MAP kinase and NF-kB resulting in the production of pro-inflammatory cytokines, involved in the infection control. It is also known that HERV RNAs are able to activate the immune system, thus stimulating the production of pro-inflammatory cytokines, which in turn can activate and prime the adaptive immune response [42]. This mechanism could be explained by the presence of transcriptional regulatory elements within retroviral long terminal repeats LTRs [98, 99]. This feedback loop made by HERV upregulation, inflammatory mediators and epigenetic dysregulation could be one way in which HERVs could have pathogenic potential leading to chronic stimulation of the immune system that could sustain the development and/or the progression of several human diseases.
5.2 The role of human endogenous retroviruses in neuroinflammatory and neuropsychiatric disorders
Outdated scientific evidence has reported the possibility of different viruses such as herpesviruses, HIV and Ebola virus to reach the central nervous system (CNS) contributing to the development of diseases. As such, despite the inaccessibility of CNS and the immunological structure that makes it a ‘privileged district’, the viral replication can occur by exceeding controls and can also happen multiple times during an individual’s lifetime increasing the risk of developing neuropathologies [100]. In the last few decades, many researchers demonstrated that the activation of endogenous viral sequences in response to exogenous stimuli, especially viruses, can contribute to a variety of neuroinflammatory and neuropsychiatric disorders, including multiple sclerosis (MS), amyotrophic lateral sclerosis (ALS), schizophrenia (SCZ) and bipolar disorder (BD). The pathways in which retroelements are involved in derailment of the nervous system are diverse: HERVs mainly interact with innate and adaptive immunity [52, 101], LINE activity is linked to neurogenesis, in particular neuronal differentiation and cognitive processes, both in adult brain and in progenitor cells [102, 103], and Alu elements, the most common member of SINEs, are involved in neurogenesis, brain development and cognition pathways [102, 104]. The first paper describing the involvement of HERVs in neurological disorders, especially in MS, dates back to the late 1900s when Perron and colleagues discovered retroviral elements in the leptomeningeal cells of MS patients [105]. From this initial work, several studies succeeded, both
6. Human endogenous retroviruses in neurodevelopmental disorders
The first article pioneering the hypothesis of the possible involvement of HERVs in the aetiopathogenesis of neurodevelopmental disorders was published by us 10 years ago. Specifically, we hypothesized a link between HERV activity and ASD highlighting a distinct expression profile in Italian autistic children in which HERV-H was highly expressed in peripheral lymphocytes, when compared with controls, with higher levels in younger children, supporting the hypothesis that HERV-H overexpression might be regarded as a potential early biomarker of ASD. This view was even more supported by the fact that ASD children with more severe impairments in Communication and Motor Psychoeducational Profile-3 showed the highest expression levels of HERV-H [124]. The analysis of HERV expression profile was then replicated in a cohort of Albanian ASD children who showed HERV-H high expression level in peripheral lymphocytes as already found in Italian ASD children. This allowed us to conclude that HERV-H could be considered as a molecular signature of the disease unrelated to ethnicity [125]. These findings opened a challenging scenario to extend the study to a cohort of attention deficit hyperactivity disorder (ADHD) children in order to verify whether the peculiar HERV expression profile could also be identified in a ‘twin disorder’ of ASD. Indeed, the two disorders are highly correlated [126], and ADHD often occurs in conjunction with ASD [127]. ADHD children showed the highest expression levels of HERV-H in peripheral lymphocytes correlated with inattention and hyperactivity symptoms, suggesting HERV-H a molecular biomarker also for ADHD [128]. All the evidence emerged from these initial papers was always obtained by studying drug-naϊve children considering that, as indicated at the time by other research groups, HERV activity could be strongly influenced by drugs exposure [90]. And it is from all of this that the subsequent work arose, in which the intention was to evaluate HERV-H as a potential biomarker of response to treatment in ADHD patients undergoing methylphenidate (MPH) therapy. As such, the reduction of HERV-H expression levels H in peripheral lymphocytes from ADHD children was found after only 1 week of MPH therapy with a further decrease at 24 weeks of treatments in parallel with improvement in symptoms. These findings suggested HERV-H as a predictive marker of the response to MPH therapy despite the awareness that the absence of a non-responsive patient group is a major limitation of this research preventing definitive conclusions [129]. The validation of early results about HERV expression profile in ASD children and new evidence came from a paper we published in 2019 in which we also included the parents of children in order to investigate the parent-of-origin effects in ASD in terms of HERVs and immune deregulation. ASD children and their mothers shared common expression levels of HERV-H and HEMO and of the cytokines such as TNF-α, IFN-γ and IL-10 in peripheral lymphocytes. Therefore, the abnormal expression of HERVs and cytokines was not an exclusive trait of autistic patients but also of their mothers, suggesting a close mother-child association within the ASD families. Taken together, these findings support the potential use of selected HERVs and cytokines in a set of biomarkers that accounts for the multifaceted nature of the disorder and can complement existing clinical methods [130]. A subgroup of this cohort was also used to conduct a proof of concept study in which lymphocytes from ASD children and their parents were exposed to stimulating factors (Interleukin-2/Phytohaemagglutinin) or drugs, such as the antiepileptic drug valproic acid (VPA) and the antiretroviral drug efavirenz (EFV) with the intent to investigate whether the expression level of HERVs and cytokines could be modulated. Lymphocytes from ASD children and their mothers share intrinsic responsiveness to stimulating factors and VPA in expressing HERVs and cytokines. EFV specifically restored the HERV activity with a concomitant modulation of cytokines, in particular lowering the pro-inflammatory while maintaining high regulatory ones. This evidence provided new insights into the potential role of HERVs as biomarkers of ASD and raising the possibility of using HERV expression as a therapeutic target for a tailored approach to patient care [86].
With the intent of deciphering other factors linked to HERV activity that could contribute to ASD pathogenesis, the expression of epigenetic effectors known to regulate HERV expression and brain functions has been evaluated in ASD children. The authors found a correlation among the overexpression of these elements and several HERVs suggesting their involvement in pathogenetic mechanisms leading to ASD [131]. All the studies above described were conducted using peripheral lymphocytes from ASD cohorts in agreement with the findings of various research studies that there is a shared gene expression profile between whole blood and brain tissues, suggesting that the cautious and thoughtful use of peripheral gene expression may be a useful surrogate for analysis in the brain. Of course, the brain remains the district of choice for studying neurodevelopmental alterations and to circumvent the issue, different preclinical models of ASD have been developed enabling studies on the aetiology, pathogenesis and possible prevention and treatment modalities of ASD. The main categories of models comprise genetic animal models, idiopathic strain, models of infection/inflammation and chemically induced animal models displaying robust and well-replicated social deficits and repetitive behaviours [132]. The idiopathic strain BTBR T+tf/J (BTBR) and the prenatally CD-1 VPA-induced models of ASD have been extensively studied to characterize the expression profile of ERV and immune mediators. As such, whole embryos at about half of gestation, brain and blood tissues at different postnatal ages have been analysed. Both ASD models showed higher expression levels of ERVs beginning from intrauterine life and up to adulthood (Figure 2). Moreover, the aberrant expression of some ERV families correlated with expression levels of pro-inflammatory cytokines and TLR-3 and TLR-4 in embryos and brain tissues, supporting the interplay between ERVs and neuroinflammation as contributing factors in the appearance of ASD-like phenotype [133]. Subsequently, we conceived a study to evaluate the multigenerational impact of prenatal VPA exposure, demonstrating transgenerational changes in both behaviour and ERV expression that last, with fading of epigenetic memories across generations, till the third one that lacks a direct exposure to the drug (Figure 2). Of note, offspring from maternal lineages showed more marked transcriptional effects compared with paternal lineages both in the second and in third generations suggesting the hypothesis of maternal imprinting as a contributing factor in increasing susceptibility to ASD [134]. Moreover, these findings also suggest ERV blood transcriptional levels as a stable peripheral biomarker, even at early life stages, of derailed brain development [135]. In our last paper, we demonstrated that MIA induced abnormal expression of ERVs and immune mediators in mouse off-spring in a sex-dependent fashion. Specifically, we demonstrated that the prenatal exposure to Poly I:C in C57BL6/J mice induced a tissue-specific expression of several ERVs, ERV-related genes and inflammatory mediators with ERVs as the main carriers of the peculiar profile found in brain areas from Poly I:C mice. In addition, Poly I:C induced larger effects on the expression of some retroviral elements only in pre-frontal cortex from female offspring reinforcing the view on sex bias as a possible risk factor for ASD [136].
Taken together, these findings candidate ERV activation as common feature shared by several risk factors of appearance of ASD and suggest ERVs as main carriers of changes occurring in brain from autistic mice, primarily in female offspring. These papers could represent the starting point to set up a new preclinical experimental design to verify the chance to inhibit ERV activity to rescue ERV activation, immune dysregulation and ASD-like phenotype observed in offspring trying to figure out cause and effect in this complex interplay. Moreover, a deep characterization of the molecular mechanisms by which gender differences could affect the neurodevelopment will help in identifying gender-specific diagnosis and personalized treatment strategies.
7. Human endogenous retroviruses: from aetiological to therapeutic implications in neurological diseases
Given the now well-established knowledge regarding the implication of HERVs in different pathological conditions, new avenues for the development of targeted therapies directed against HERV products have been opened. In this direction, a humanized monoclonal antibody (mAb) directed against HERV-W ENV, called GNbAC1 or temelimab, has been developed. The drug targets a linear non-glycosylated epitope of the surface unit domain of the HERV-W Env, blocking its interaction with the TLR-4 receptor and thus, the release of pro-inflammatory mediators and the inhibition of the myelin repair process. Different
Taken together, these findings provide the background for hypothesizing other therapeutic approaches targeting HERVs in different clinical setting towards a personalized medicine.
8. Conclusions and new future perspectives
The physiological roles of HERVs in pregnancy and embryogenesis, their intrinsic responsiveness to external stimuli and the interaction with the immune system support the hypothesis that their deregulation affects the neurodevelopmental process (Figure 3). Nevertheless, it is still debated if HERVs are cofactors or epiphenomenon in neurodevelopmental disorders, and more efforts are needed to investigate the potentially detrimental effect of HERV products in the aetiopathogenic processes. In this complex landscape, the use of animal models could offer countless advantages to deeply investigate the embryonic phase that is certainly crucial for the onset of ASD, and brain district, mostly inaccessible in human studies. Since the brain remains the district of choice for the study of neurodevelopmental alterations, preclinical models of ASD allow to explore and characterize this anatomical district in depth, helping clinical research to make further progress towards the identification of new biomarkers, potentially useful for diagnosis and pharmacological intervention. Moreover, HERVs seem to be a reliable biomarker for ASD, readily detectable in peripheral blood, representing a potential efficient diagnostic tool to complement the current clinical behavioural diagnosis. Furthermore, a biomarker detectable before the onset of symptoms could facilitate early screening and timely initiation of treatment by improving the long-term prognosis of the mental health of affected individuals. Further studies are needed and could represent a new approach to unravel the aethiopathogenesis of ASD, bearing in mind that the retroelements cannot be appropriately understood only through a virologic or genetic approach, since their complex roles in physiology as well in diseases. Both preclinical models and human studies indicate that the abnormal expression of ERVs could represent a molecular signature of neurodevelopmental disorders.
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