New or vanishing frontiers: LACC1- associated juvenile arthritis

Sulaiman M Al-Mayouf; Mada Yateem; Haya Al-Dusery; Dorota Monies; Salma Wakil; Manal AlShiakh; Abdullatif AlEnazi; Boshra Aladaileh; Raed Alzyoud; Brian Meyer

doi:10.1016/j.ijpam.2020.11.005

New or vanishing frontiers: LACC1- associated juvenile arthritis

Int J Pediatr Adolesc Med. 2021 Mar;8(1):44-47. doi: 10.1016/j.ijpam.2020.11.005. Epub 2020 Nov 12.

Authors

Sulaiman M Al-Mayouf^{1

2}, Mada Yateem^{1

2}, Haya Al-Dusery², Dorota Monies², Salma Wakil², Manal AlShiakh², Abdullatif AlEnazi³, Boshra Aladaileh⁴, Raed Alzyoud⁴, Brian Meyer²

Affiliations

¹ Department of Pediatric Rheumatology, Riyadh, Saudi Arabia.
² King Faisal Specialist Hospital and Research Center, Riyadh, Saudi Arabia.
³ King Fahad Medical City, Riyadh, Saudi Arabia.
⁴ Queen Rania Children Hospital, Amman, Jordan.

Abstract

Background: The classification and pathogenic basis of juvenile idiopathic arthritis (JIA) are a subject of some controversy. Essentially, JIA is an exclusion diagnosis that represents a phenotypically heterogeneous group of arthritis of unknown origin. Familial aggregation of JIA supports the concept of genetic influence in the pathogenesis of JIA.

Objective: To present the spectrum of laccase domain-containing 1 (LACC1)-associated juvenile arthritis with clinical, biochemical, and molecular genetic data of a cohort of 43 patients, including 11 previously unpublished cases.

Methods: We studied 11 patients with different categories of juvenile idiopathic arthritis from 5 consanguineous families, all from Saudi Arabia, except 2 patients who were of Jordanian ethnicity. Whole-exome sequencing was used to identify the disease-causing variant of LACC1. We also reviewed the clinical spectrum and molecular genetic data of previously published cases of LACC1-associated juvenile arthritis.

Results: This study describes 43 (29 females, 14 males) patients from consanguineous multiplex families. Most of the included patients were of Arab origin with 86% having early onset disease. The most frequent categories were systemic (19 patients) and rheumatoid factor-negative polyarticular (19 patients). Thirty-seven (86%) had progressive erosive arthritis and 10 (23.3%) had persistent limb lymphedema. None of the patients had features of macrophage activation syndrome. Genetic analysis confirmed LACC1 variant in all patients; 22 patients had common founder mutation (LACC1: c.850T > C,p.C284R), while the others showed different LACC1 variants. All patients were treated aggressively with methotrexate and sequential biologic agents. Most of them showed a poor response to treatment.

Conclusion: This report expands the pathogenic variants of LACC1 and the clinical spectrum associated with this genetic subset of juvenile arthritis. The predominance of autosomal-recessive inheritance and strong genetic evidence allowed us to propose LACC1-associated juvenile arthritis as a distinct disorder.

Keywords: Arthropathy; Familial arthritis; Juvenile idiopathic arthritis; LACC1 associated juvenile arthritis.