Your search keyword '"Donohue syndrome"' showing total 2 results

1. One Novel 2.43Kb Deletion and One Single Nucleotide Mutation of the INSR Gene in a Chinese Neonate with Rabson-Mendenhall Syndrome.

Author

Xiang Chen, Wenhao Zhou, Huijun Wang, Bingbing Wu, Xinran Dong, Bo Liu, Hongbo Chen, Yulan Lu, and Lin Yang

Subjects

*DONOHUE syndrome, *CHROMOSOME abnormalities, *FETAL growth retardation, *GENETIC polymorphisms, *HOMEOSTASIS, *HYPERINSULINISM, *GENETIC mutation, *POLYMERASE chain reaction, *PROTEIN-tyrosine kinases, *TESTOSTERONE, *GENETIC testing, *SEQUENCE analysis, *GENETICS

Abstract

Mutations in the insulin receptor (INSR) gene are responsible for Donohue syndrome (DS) and Rabson-Mendenhall syndrome (RMS). Insulin resistance is a feature of both diseases. Our patient was a Chinese neonate suffering from abnormal glucose homeostasis, hyperinsulinemia, dry skin, heavy hair, growth retardation and an elevated testosterone level. To search for candidate point mutations, small insertions or deletions and copy number variants, 2742 inherited disease-gene panel sequencing was performed. One pathogenic mutation (c.3355C>T, p.Arg1119Trp) and a novel 2.43Kb deletion (chr19:7150507-7152938) in INSR were found. The patient was diagnosed as RMS. Sanger sequencing and real-time quantitative polymerase chain reaction (PCR) confirmed the missense variant and microdeletion, respectively. We therefore supposed that these variants were candidate mutations in this case. We report a novel 2.43Kb deletion in INSR gene and provide further proof of the power of next generation sequencing in rare disease diagnosis. [ABSTRACT FROM AUTHOR]

Published

2018

2. Clinical and Functional Characterization of Novel INSR Variants in Two Families With Severe Insulin Resistance Syndrome.

Author

Zhou Q, Yu J, Yuan X, Wang C, Zhu Z, Zhang A, and Gu W

Subjects

Acanthosis Nigricans complications, Acanthosis Nigricans genetics, Animals, CHO Cells, Child, Child, Preschool, China, Cricetulus, DNA Mutational Analysis, Diabetes Complications genetics, Donohue Syndrome complications, Donohue Syndrome genetics, Family, Female, Humans, Male, Metabolic Syndrome complications, Mutation, Missense, Patient Acuity, Pedigree, Syndrome, Antigens, CD genetics, Insulin Resistance genetics, Metabolic Syndrome genetics, Receptor, Insulin genetics

Abstract

Objective: Defects in the insulin receptor ( INSR ) gene cause various severe insulin resistance conditions, including Donohue syndrome (DS), Rabson-Mendenhall syndrome (RMS) and type A insulin resistance (type A-IR). This study aimed to investigate the clinical characterization and molecular defects in three Chinese children with INSR -related insulin resistance syndrome., Methods: We reviewed the clinical data of three Chinese children with INSR -related insulin resistance syndrome from two unrelated kindreds. Genetic analysis was performed using whole-exome sequencing and the effects of the novel variants were further assessed by in vitro functional assays., Results: The proband with type A-IR presented with acanthosis nigricans, hypertrichosis, and euglycemia with mild insulin resistance in early childhood. His sister presented with features typical of type A-IR and was diagnosed with diabetes mellitus with severe insulin resistance at the age of 9.8 years. The proband with DS showed typical dysmorphic characteristics, severe intrauterine growth retardation, extreme insulin resistance, fasting hypoglycemia and postprandial hyperglycemia from birth. The heterozygote variants c.[3670G>A]; c.[3614C>T] were identified in both siblings with type A-IR; and c.[749_751del]; c.[3355C>T] in the patient with DS. In vitro studies showed that the novel variant c.749_751del [p.(Thr250del)] in the α-subunit, reduced expression of the mature INSR protein and severely impaired INSR function. In contrast, the novel variant c.3670G>A [p.(Val1224Met)] in the β-subunit had no effect on total protein expression and phosphorylation of INSR and Akt, suggesting that the variant p.Val1224Met appeared to be tolerated and was not responsible for the severe insulin resistance., Conclusion: Our study detailed the clinical features of three patients with type A-IR and DS, and identified two novel variants in the INSR gene. Functional assays indicated the novel variant p.Thr250del was pathogenic. In contrast, the novel variant p.Val1224Met was suggested to be tolerated by our experimental data, even though bioinformatics analyses predicted the variant as deleterious., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Zhou, Yu, Yuan, Wang, Zhu, Zhang and Gu.)

Published

2021