A novel heterozygous variant of the <scp><i>SALL1</i></scp> gene with atypical <scp>Townes‐Brocks</scp> syndrome phenotypes in Chinese family-Reference-Cited by-同舟云学术

A novel heterozygous variant of the SALL1 gene with atypical Townes‐Brocks syndrome phenotypes in Chinese family

Published:2024-04-07 Issue:8 Volume:29 Page:541-546
ISSN:1320-5358
Container-title:Nephrology
language:en
Short-container-title:Nephrology

Author:

Liu Xuyan¹^ORCID,Wang Hong²,Zhang Yiyin¹,Zhang Ran¹,Zhang Ruixiao³^ORCID,Shi Xiaomeng¹,Pan Fengjiao¹,Qiao Dan⁴,Xin Qing⁵,Liu Zhiying⁶^ORCID,Zhang Yan⁷,Li Changying¹,Lang Yanhua⁸,Shao Leping⁹^ORCID

Affiliation:

1. Department of Nephrology the Affiliated Qingdao Municipal Hospital of Qingdao University Qingdao China

2. Department of Nephrology Qingdao Eighth People's Hospital Qingdao China

3. Department of Emergency, Qingdao Hospital University of Health and Rehabilitation Sciences (Qingdao Municipal Hospital) Qingdao China

4. Department of Nephrology Dalian Medical University Dalian China

5. Department of Nephrology, Xinqiao Hospital Army Medical University (Third Military Medical University) Chongqing China

6. Renal Division Peking University First Hospital Beijing China

7. Department of Nephrology Weifang Medical University Weifang China

8. Department of Materials, Qingdao Hospital University of Health and Rehabilitation Sciences (Qingdao Municipal Hospital) Qingdao China

9. Department of Nephrology, Qingdao Hospital University of Health and Rehabilitation Sciences (Qingdao Municipal Hospital) Qingdao China

Abstract

AbstractTownes‐Brocks syndrome (TBS) is an autosomal dominant disorder characterised by the triad of anorectal, thumb, and ear malformations. It may also be accompanied by defects in kidney, heart, eyes, hearing, and feet. TBS has been demonstrated to result from heterozygous variants in the SALL1 gene, which encodes zinc finger protein believed to function as a transcriptional repressor. The clinical characteristics of an atypical TBS phenotype patient from a Chinese family are described, with predominant manifestations including external ear dysplasia, unilateral renal hypoplasia with mild renal dysfunction, and hearing impairment. A novel heterozygous variant c.3060T>A (p.Tyr1020*) in exon 2 of the SALL1 gene was identified in this proband. Pyrosequencing of the complementary DNA of the proband revealed that the variant transcript accounted for 48% of the total transcripts in peripheral leukocytes, indicating that this variant transcript has not undergone nonsense‐mediated mRNA decay. This variant c.3060T > A is located at the terminal end of exon 2, proximal to the 3′ end of the SALL1 gene, and exerts a relatively minor impact on protein function. We suggest that the atypical TBS phenotype observed in the proband may be attributed to the truncated protein retaining partial SALL1 function.

Funder

National Natural Science Foundation of China

Publisher

Wiley

Link

https://onlinelibrary.wiley.com/doi/pdf/10.1111/nep.14300

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