| Literature DB >> 29485195 |
Bahadur Singh Gurjar1, Tholu Manikanta Sriharsha2, Angika Bhasym3,4, Savit Prabhu5, Mamta Puraswani6, Priyanka Khandelwal6, Himanshi Saini6, Savita Saini6, Anita Kamra Verma7, Priyadarshini Chatterjee3, Prasenjit Guchhait3, Vineeta Bal1,5, Anna George1, Satyajit Rath1,5,8, Arvind Sahu2, Amita Sharma6, Pankaj Hari6, Aditi Sinha6, Arvind Bagga6.
Abstract
We previously reported that Indian paediatric patients with atypical haemolytic-uraemic syndrome (aHUS) showed high frequencies of anti-complement factor H (FH) autoantibodies that are correlated with homozygous deletion of the genes for FH-related proteins 1 and 3 (FHR1 and FHR3) (FHR1/3-/- ). We now report that Indian paediatric aHUS patients without anti-FH autoantibodies also showed modestly higher frequencies of the FHR1/3-/- genotype. Further, when we characterized epitope specificities and binding avidities of anti-FH autoantibodies in aHUS patients, most anti-FH autoantibodies were directed towards the FH cell-surface anchoring polyanionic binding site-containing C-terminal short conservative regions (SCRs) 17-20 with higher binding avidities than for native FH. FH SCR17-20-binding anti-FH autoantibodies also bound the other cell-surface anchoring polyanionic binding site-containing region FH SCR5-8, at lower binding avidities. Anti-FH autoantibody avidities correlated with antibody titres. These anti-FH autoantibody characteristics did not differ between aHUS patients with or without the FHR1/3-/- genotype. Our data suggest a complex matrix of interactions between FHR1-FHR3 deletion, immunomodulation and anti-FH autoantibodies in the aetiopathogenesis of aHUS.Entities:
Keywords: complement factor H autoantibodies; genetic predisposition to autoimmunity; haemolytic-uraemic syndrome
Year: 2018 PMID: 29485195 PMCID: PMC6050217 DOI: 10.1111/imm.12916
Source DB: PubMed Journal: Immunology ISSN: 0019-2805 Impact factor: 7.397