Prenatal diagnosis of polycystic kidney caused by biallelic hypomorphic variants in the PKD1 gene

• Published in: Prenatal diagnosis Vol. 44; no. 2; pp. 247 - 250
• Main Authors: Zheng, Yu, Wong, Lo, Kwan, Angel Hoi Wan, Dong, Zirui, Kwok, Ka Yin, Choy, Kwong Wai, Dai, Hongzheng, Cao, Ye
• Format: Report
• Language: English
• Published: 01.02.2024
• ISSN: 1097-0223
• DOI: 10.1002/pd.6419

Heterozygous loss-of-function variants in the PKD1 gene are commonly associated with adult-onset autosomal dominant polycystic kidney disease (ADPKD), where the formation of renal cysts depends on the dosage of the PKD1 gene. Biallelic null PKD1 variants are not viable, but biallelic hypomorphic variants could lead to early-onset PKD. We report a non-consanguineous Chinese family with recurrent fetal polycystic kidney and negative findings in the coding region of the PKHD1 gene or chromosomal microarray analysis. Trio exome analysis revealed compound heterozygous variants of uncertain significance in the PKD1 gene in the index pregnancy: a novel paternally inherited c.7863 + 5G > C and a maternally inherited c.9739C > T, p.(Arg3247Cys). Segregation analysis through long-range PCR followed by nested PCR and Sanger sequencing confirmed another affected fetus had both variants, while the other two normal siblings and the parents carried either variant. Thus, these two variants, both of which were hypomorphic as opposed to null variants, co-segregated with prenatal onset polycystic kidney disease in this family. Functional studies are needed to further determine the impact of these two variants. Our findings highlight the biallelic inheritance of hypomorphic PKD1 variants causing prenatal onset polycystic kidney disease, which provides a better understanding of phenotype-genotype correlation and valuable information for reproductive counseling.