Antibody reactivity to the hres‐1 endogenous retroviral element identifies a subset of patients with systemic lupus erythematosus and overlap syndromes

Perl, András; Colombo, Emanuela; Dai, Huiliang; Agarwal, Rajeev; Mark, Kenneth A.; Bánki, Katalin; Poiesz, Bernard J.; Phillips, Paul E. M.; Hoch, Sallie O.; Reveille, John D.; Arnett, Frank C.

doi:10.1002/art.1780381119

Cited by 89 publications

(59 citation statements)

References 52 publications

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“…HRES-1 is a transcriptionally active HERV that encodes a 28 kDa nuclear autoantigen, HRES-1/p28 and a small GTP-ase, HRES-1/Rab4. Autoantibodies to HRES-1/p28, which are found in half of the patients with SLE [23][24][25][26][27], are cross-reactive with antigens of viruses infecting patients with SLE, such as TTV and EBV [71] and the 70 kDa component of U1 snRNP [24] and may thus contribute to epitope spreading and development of anti-nuclear antibody (ANA). In turn, HRES-1/Rab4 regulates the recycling of CD4, a key component of the IS, which is abnormally assembled in T cells of patients with SLE.…”

Section: Discussionmentioning

confidence: 99%

“…Interestingly, higher expression levels in SLE lymphocytes correlate with production of U1 snRNP [57] which includes a 70 kDa protein with a region of homology to gag antigens of infectious and ERV [24,58]. The 1q42 chromosomal region that has been associated with lupus susceptibility [59] and harbors the HRES-1 ERV [27,60] is genetically unstable [61].…”

Section: Activation Of Erv By Dna Demethylationmentioning

confidence: 99%

“…In addition, TTV cross-reactive lupus sera showed high binding affinity to HRES-1/p28 peptide 121-135 (DRRREGPDRSPRQPP) harboring three consecutive highly charged amino acids (RRE). This RRE triplet is repeated three times in the retroviral gag-like region of 70K U1 snRNP lupus autoantigen and represent crossreactive epitopes between the two proteins [24].…”

Section: Hres-1/p28 With Viral Peptides and The 70 Kda Protein Of U1 mentioning

confidence: 99%

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Molecular mimicry and immunomodulation by the HRES-1 endogenous retrovirus in SLE

et al. 2008

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Genetic and environmental factors are believed to influence development of systemic lupus erythematosus (SLE). Endogenous retroviruses (ERV) correspond to the integrated proviral form of infectious retroviruses, which are trapped within the genome due to mutations. ERV represent a key molecular link between the host genome and infectious viral particles. ERV-encoded proteins are recognized by antiviral immune responses and become targets of autoreactivity. Alternatively, ERV protein may influence cellular processes and the life cycle of infectious viruses. As examples, the HRES-1 human ERV encodes a 28-kDa nuclear autoantigen and a 24-kDa small GTP-ase, termed HRES-1/Rab4. HRES-1/p28 is a nuclear autoantigen recognized by crossreactive antiviral antibodies, while HRES-1/Rab4 regulates surface expression of CD4 and the transferrin receptor (TFR) through endosome recycling. Expression of HRES-1/Rab4 is induced by the tat gene of HIV-1, which in turn down-regulates expression of CD4 and susceptibility to reinfection by HIV-1. CD4 and the TFR play essential roles in formation of the immunological synapse (IS) during normal T-cell activation by a cognate MHC class II peptide complex. The key intracellular transducer of T-cell activation, Lck, is brought to the IS via binding to CD4. T-cell receptorζ (TCRζ) chain binds to the TFR. Abnormal T-cell responses in SLE have been associated with reduced lck and TCRζ chain levels. HRES-1 is centrally located on chromosome 1 at q42 relative to lupus-linked microsatellite markers and polymorphic HRES-1 alleles have been linked to the development of SLE. 1q42 is one of the three most common fragile sites in the human genome, and is inducible by DNA demethylation, a known mechanism of retroviral gene activation. Molecular mimicry and immunomodulation by a ERV, such as HRES-1, may contribute to self-reactivity and abnormal Tand B-cell functions in SLE. (Table I). HERVs are commonly designated as HERV followed by a single letter amino acid code corresponding to a tRNA. The 3′ terminus of tRNA is predicted to initiate reverse transcription by annealing to an 18 nucleotide long primer-binding site (PBS) at the 5′ LTR. While expression of murine ERV can lead to production of infectious virus and cause viremia, no production of infectious virion has been documented by HERV. High copy number of most ERV families makes it difficult to distinguish which members of a group are expressed. Although, no single provirus with intact LTRs and uninterrupted gag, pol, and env ORFs has been identified, the HERV-K ERV, as a family, has been shown to encode gag HHS Public Access Author Manuscript Author ManuscriptAuthor ManuscriptAuthor Manuscript the LTR region, is functionally analogous to the HIV-1 rev and HTLV-I/II rex proteins. HERV-K rev binds to both the nuclear export factor Crm1 and to a cis-acting viral RNA to activate nuclear export of unspliced RNAs [39]. Alternatively, the HERV-K LTR is also recognized by HIV-1 rev, suggesting a potential interaction between these exogeneous a...

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Section: Discussionmentioning

confidence: 99%

Section: Activation Of Erv By Dna Demethylationmentioning

confidence: 99%

Section: Hres-1/p28 With Viral Peptides and The 70 Kda Protein Of U1 mentioning

confidence: 99%

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Molecular mimicry and immunomodulation by the HRES-1 endogenous retrovirus in SLE

et al. 2008

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“…In lupus patients, however, antibody levels to human immunodefi ciency virus type I p24 gag proteins are increased, and endogenous retroviruses are found in sera [65][66][67] . Two studies [66,67] showed a correlation between these antibodies and specifi c antibodies and clinical features (e.g., severe discoid LE). Nevertheless, despite a large number of studies, there is as yet no conclusive evidence to support the direct linkage of LE to endogenous or exogenous retroviruses in humans.…”

Section: Viruses and Other Infectious Agentsmentioning

confidence: 99%

Exogenous Factors in Cutaneous Lupus Erythematosus

Trattner¹

2004

Exog Dermatol

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“…Polyclonal antibodies revealed a 28-kDa protein concordant with the predicted molecular weight of the p25 protein. This product was related to the HRES-1 gag ORF (11).The serum antibody reactivity against the 2 HRES-1 peptides was tested, and the GAG p24 HTLV-1 reactivity, previously observed in autoimmune patient's sera, was subsequently related to anti-HRES-1 antibodies (11)(12)(13).…”

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confidence: 99%

Molecular Analysis of Endogenous Retrovirus HRES-1: Identification of Frameshift Mutations in Region Encoding Putative 28-kDa Autoantigen

Lefranc¹,

Dubucquoi²,

Almeras³

et al. 2001

Biochemical and Biophysical Research Communications

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Antibody reactivity to the hres‐1 endogenous retroviral element identifies a subset of patients with systemic lupus erythematosus and overlap syndromes

Cited by 89 publications

References 52 publications

Molecular mimicry and immunomodulation by the HRES-1 endogenous retrovirus in SLE

Molecular mimicry and immunomodulation by the HRES-1 endogenous retrovirus in SLE

Exogenous Factors in Cutaneous Lupus Erythematosus

Molecular Analysis of Endogenous Retrovirus HRES-1: Identification of Frameshift Mutations in Region Encoding Putative 28-kDa Autoantigen

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