Systematic review of TCF2 anomalies in renal cysts and diabetes syndrome/maturity onset diabetes of the young type 5
Chen, Yi-zhi, Gao, Qing, Zhao, Zue-zhi, Chen, Ying-zhang, Bennett, Craig L., Xiong, Xi-shan, Mei, Chang-lin , Shi, Yong-quan, and Chen, Xiang-mei (2010) Systematic review of TCF2 anomalies in renal cysts and diabetes syndrome/maturity onset diabetes of the young type 5. Chinese Medical Journal, 123 (22). pp. 3326-3333.
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Abstract
Objective: There is a paucity of published works that systematically evaluate gene anomalies or clinical features of patients with renal cysts and diabetes syndrome (RCAD)/maturity onset diabetes of the young type 5 (MODY5). The purpose of this review was to systematically assess the detection rate, genetic and phenotypic implications of heterozygous autosomal dominant TCF2 anomalies. Data sources: MEDLINE database was searched to select articles recorded in English from 1997 to 2008. The focus was monoallelic germline TCF2 gene mutations/deletions. Biallelic inactivation, polymorphisms, DNA modification (hypomethylation and hypermethylation), loci associated with cancer risk, and somatic TCF2 anomalies were all excluded.
Study selection: After searching the literature, 50 articles were selected.
Results: The detection rate of TCF2 anomalies was 9.7 and varied considerably among MODY (1.4), renal structure anomalies (RSA) (21.4) and RSA with MODY (41.2) subgroups. Mutations were strikingly located within the DNA binding domain and varied among exons of the DNA binding domain: exons 2 and 4 were the hottest spots, while mutations were sporadically distributed in exon 3. The consistent phenotypes were RSA (89.6) and diabetes mellitus (DM) (45.0). However, the concurrence of RSA and DM was relatively low (27.5), which hinders the optimal performance of genetic testing and obtainment of timely diagnosis. Other organ involvements were complementary and necessary for the early identification of patients with TCF2 anomalies. Analysis of phenotypes of TCF2 point mutations showed significant differences in the detection rates of RSA, impaired renal function (IRF) and DM according to mutation type but not mutation location.
Conclusion: These valuable features of TCF2 anomalies that previously did not receive sufficient attention should not be neglected.
Item ID: | 35699 |
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Item Type: | Article (Research - C1) |
ISSN: | 0366-6999 |
Keywords: | genetic heterogeneity; hepatocyte nuclear factor 1-beta; phenotype; renal cysts and diabetes syndrome |
Date Deposited: | 30 Oct 2014 03:56 |
FoR Codes: | 06 BIOLOGICAL SCIENCES > 0604 Genetics > 060499 Genetics not elsewhere classified @ 50% 11 MEDICAL AND HEALTH SCIENCES > 1109 Neurosciences > 110999 Neurosciences not elsewhere classified @ 50% |
SEO Codes: | 92 HEALTH > 9201 Clinical Health (Organs, Diseases and Abnormal Conditions) > 920199 Clinical Health (Organs, Diseases and Abnormal Conditions) not elsewhere classified @ 100% |
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