Effect of DNA methylation on inhibitor development in Hemophilia A patients treated with FVIII concentrates.

Himani Chand; Shermarke Hassan; Andrea Cairo; Roberta Palla; Flora Peyvandi; Flora Peyvandi; Pier Mannuccio Mannucci; Isabella Garagiola; Amal El‐Beshlawy; Mohsen Saleh Elalfy; Vijay Ramanan; Peyman Eshghi; Suresh Hanagavadi; Ramabadran Varadarajan; Mehran Karimi; Mamta Manglani; Cecil Ross; Guy Young; Tulika Seth; Shashikant Apte; Dinesh Nayak; Elena Santagostino; Maria Elisa Mancuso; Adriana C. Sandoval Gonzalez; Johnny Mahlangu; Santiago Bonanad; M. Cerqueira; Nadia P. Ewing; Christoph Male; Tarek Owaidah; Ferrell Margaret A.; Verónica Soto Arellano; Nathan L. Kobrinsky; Suvankar Majumdar; Ch . B. M. B.; Rosario Garrido; Anupam Sachdeva; Mindy L. Simpson; Mathew Thomas; Ezio Zanon; Bülent Antmen; Kaan Kavaklı; Marilyn J. Manco‐Johnson; Mònica Martínez; E. Marzouka; Maria Gabriella Mazzucconi; Alexis Diomedi P; Daniela Neme; Ángeles Palomo Bravo; Rogelio Paredes Aguilera; A. Prezotti; Klaus Schmitt; Brian M. Wicklund; Bülent Zülfikar; Frits R. Rosendaal

doi:10.1016/j.rpth.2025.102858

Abstract

1 min read

Background Hemophilia A (HA) is a hereditary X-linked hemorrhagic disorder. Following the first treatment with exogenous factor (F)VIII, one-third of patients with severe HA develop anti-FVIII antibodies (inhibitors), which render treatment ineffective. Recent findings underlined the critical role of DNA methylation in several autoimmune diseases by altering gene expression profiles. This study was designed to evaluate potential differences in DNA methylation profiles of previously untreated patients (PUPs) who develop inhibitors against FVIII and those who do not, with the aim of identifying immune-regulatory genes that may contribute to the risk of inhibitor formation. Objectives In this study, we aimed to understand whether CpG sites are differentially methylated in peripheral blood mononuclear cells (PBMCs) of PUPs and have a role in inhibitor development to better understand the biological pathways that lead to inhibitor development. Methods A case-control study was performed using 45 inhibitor-positive and 67 inhibitor-negative PUPs from the Survey of Inhibitors in Plasma-Product Exposed Toddlers study cohort. Enrichment bisulfite sequencing was performed on DNA samples from PBMCs of HA patients and differentially methylated CpG sites (DMCs) were identified with bioinformatic approach. Results Overall, information on 621,121 CpG sites was obtained. Two thousand seven hundred seventy-two sites were significantly differentially methylated (unadjusted P value < .05). Association of CpG sites to a few genes involved in active immune response (JAK1, CD1C, PIGR, TOLLIP, BLNK, CD44, IL23R, IFNLR1, SOCS2, TLR1, etc.) was seen in inhibitor-positive patients, but it did not indicate specific pathways associated with inhibitor development. Conclusion DMCs were identified in PBMC samples from HA patients with inhibitors. However, our data could not confirm the role of these CpG sites in affecting immune-regulatory pathways.

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