Author:
Li Ang,Gao Er-Zhi,Cui Ying-Xia,Liu Jian-Hong,Lv Xing,Wei Xiu-Xiu,Xia Xin-Yi,Gao Chun-Lin,Liu Feng-Xia,Xia Zheng-Kun,Asan ,Liu Zhi-Hong,Li Xiao-Jun
Abstract
Thin basement membrane nephropathy (TBMN), autosomal dominant Alport syndrome (ADAS), and focal segmental glomerulosclerosis (FSGS) are kidney diseases that differ in clinical diagnosis, treatment, and prognosis. Nevertheless, they may result from the same causative genes. Here, we report 3 COL4A4 heterozygous mutations (p.Gly208Arg, p.Ser513Glufs*2, and p.Met1617Cysfs*39) that lead to 3 different collagen type IV kidney disease phenotypes, manifesting as TBMN, ADAS, and FSGS. Using bioinformatics analyses and pedigree verification, we show that these novel variants are pathogenetic and cosegregate with TBMN, ADAS, and FSGS. Furthermore, we found that the collagen type IV-associated kidney disease phenotypes are heterogeneous, with overlapping pathology and genetic mutations. We propose that COL4A4-associated TBMN, ADAS, and FSGS should be considered as collagen type IV kidney disease subtypes that represent different phases of disease progression.
Subject
Genetics(clinical),Genetics,Molecular Biology
Cited by
2 articles.
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