Singh Swati, Badiger Vaishnavi Ashok, Balan Suma, Nampoothiri Sheela, Rao Anand Prahalad, Shah Hitesh, Bhavani Gandham SriLakshmi, Narayanan Dhanya Lakshmi, Girisha Katta M
Department of Medical Genetics, Kasturba Medical College, Manipal, Manipal Academy of Higher Education, Manipal, Karnataka.
Department of Rheumatology and Clinical Immunology, Amrita Institute of Medical Sciences and Research Centre.
Clin Dysmorphol. 2024 Oct 1;33(4):152-159. doi: 10.1097/MCD.0000000000000500. Epub 2024 Mar 22.
Camptodactyly-arthropathy-coxa vara-pericarditis (CACP) syndrome (MIM# 208250) is a rare monogenic disorder, characterized by early onset of camptodactyly, progressive coxa vara, bilateral arthropathy and constrictive pericarditis. The syndrome is caused by biallelic loss-of-function variants in PRG4 . Deficiency of PRG4 results in progressive worsening of joint deformity with age. Thirteen individuals with CACP syndrome from eight consanguineous Indian families were evaluated. We used exome sequencing to elucidate disease-causing variants in all the probands. These variants were further validated and segregated by Sanger sequencing, confirming the diagnosis of CACP syndrome in them. Seven females and six males aged 2-23 years were studied. Camptodactyly (13/13), coxa vara (11/13), short femoral neck (11/13) and arthritis in large joints (12/13) [wrists (11/13), ankle (11/13), elbow (10/13) and knee (10/13)] were observed commonly. Five novel disease-causing variants (c.3636G>T, c.1935del, c.1134dup, c.1699del and c.962T>A) and two previously reported variants (c.1910_1911del and c.2816_2817del) were identified in homozygous state in PRG4 . We describe the phenotype and mutations in one of the large cohorts of patients with CACP syndrome, from India.
屈曲指-关节病-髋内翻-心包炎(CACP)综合征(MIM# 208250)是一种罕见的单基因疾病,其特征为屈曲指早发、进行性髋内翻、双侧关节病和缩窄性心包炎。该综合征由PRG4基因的双等位基因功能丧失变异引起。PRG4缺乏导致关节畸形随年龄增长而逐渐加重。对来自8个印度近亲家庭的13名CACP综合征患者进行了评估。我们使用外显子组测序来阐明所有先证者中的致病变异。这些变异通过桑格测序进一步验证和分离,证实了他们患有CACP综合征。研究了7名女性和6名男性,年龄在2至23岁之间。常见的表现有屈曲指(13/13)、髋内翻(11/13)、股骨颈短(11/13)和大关节关节炎(12/13)[腕关节(11/13)、踝关节(11/13)、肘关节(10/13)和膝关节(10/13)]。在PRG4基因中鉴定出5个新的致病变异(c.3636G>T、c.1935del、c.1134dup、c.1699del和c.962T>A)和2个先前报道的变异(c.1910_1911del和c.2816_2817del),均为纯合状态。我们描述了来自印度的一大组CACP综合征患者中的表型和突变情况。
