Autosomal Dominant, Long-Standing Dysglycemia in 2 Families with Unique Phenotypic Features.

IF 2.7 Q3 ENDOCRINOLOGY & METABOLISM
Aaron Hanukoglu, Ehud Banne, Dorit Lev, Julio Wainstein
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Abstract

We describe 2 families with 5 members from 2 generations whose clinical and laboratory characteristics over up to 15 years were consistent with dysglycemia/impaired glucose tolerance. In both families (2 probands and 3 family members), long-term follow-up excluded diabetes type 1 and type 2. Diabetes type 1 antibodies were persistently negative and C-peptide levels were normal. In Family 1, the proband, during a follow-up of 7 years (10.3-17.5 years of age), exhibited persistently high HbA1c (>5.7%) with fasting blood glucose levels mostly higher than 100 mg/dl and postprandial glucose levels up to 180 mg/dl. She eventually required oral anti-diabetics with an improvement in glycemic balance. The father and sister also had persistent mild hyperglycemia with borderline high HbA1c (mostly > 5.7%) levels over 15 and 6.2 years respectively. In Family 2, the proband exhibited borderline high fasting hyperglycemia (>100 mg/dl) at age 16.2 years with increasing HbA1c levels (from 5.6%-5.9%) and impaired glucose tolerance at age 18.3 years (2 h blood glucose 156 mg/dl after 75 g glucose). His sister also exhibited borderline hyperglycemia with borderline high HbA1c over 2 years (13.6-15.4 years). These subjects shared a unique phenotype. They are tall and slim with decreased BMI. Three subjects from Generation II failed to thrive during infancy. In view of the data from 2 generations suggesting maturity-onset diabetes of the young (MODY) with autosomal dominant inheritance, we sought to analyze the MODY genes. In Family 1, the molecular analysis by the MODY panel including 11 genes and whole exome sequencing did not detect any mutation in the proband. In Family 2, the MODY panel was also negative in the proband's sister. These families may represent a hitherto unidentified syndrome. Unique features described in this report may help to reveal additional families with similar characteristics and to decipher the molecular basis of this syndrome. In selected cases, oral antidiabetics in adolescents may improve the glycemic balance.

具有独特表型特征的两个家族中的常染色体显性长效糖耐量减低症
我们描述了两个家族两代 5 名成员在长达 15 年的时间里的临床和实验室特征,他们都患有血糖异常/糖耐量受损。在这两个家族(2 个原发性糖尿病患者和 3 个家庭成员)中,长期随访排除了 1 型和 2 型糖尿病。1 型糖尿病抗体持续阴性,C 肽水平正常。在家族 1 中,原发性糖尿病患者在 7 年(10.3-17.5 岁)的随访中表现出持续的高 HbA1c(>5.7%),空腹血糖水平大多高于 100 毫克/分升,餐后血糖水平高达 180 毫克/分升。她最终需要口服抗糖尿病药物,血糖平衡情况有所改善。父亲和姐姐也有持续的轻度高血糖,HbA1c(多数>5.7%)水平也处于边缘高水平,分别持续了15年和6.2年。在家族 2 中,探查者在 16.2 岁时出现边缘性空腹高血糖(>100 毫克/分升),HbA1c 水平不断升高(从 5.6% 到 5.9%),在 18.3 岁时出现糖耐量受损(75 克葡萄糖后 2 小时血糖为 156 毫克/分升)。他的姐姐也表现出边缘性高血糖,在两年多的时间里(13.6-15.4 岁)HbA1c 水平处于边缘高水平。这些受试者具有独特的表型。他们身材瘦高,体重指数(BMI)下降。第二代中有三名受试者在婴儿期未能茁壮成长。鉴于两代人的数据表明成熟期发病的年轻糖尿病(MODY)为常染色体显性遗传,我们试图对 MODY 基因进行分析。在家族 1 中,包括 11 个基因在内的 MODY 面板分子分析和全外显子测序均未在原告体内检测到任何突变。在家族 2 中,原告妹妹的 MODY 染色体也呈阴性。这些家庭可能代表了一种迄今尚未发现的综合征。本报告中描述的独特特征可能有助于发现更多具有类似特征的家族,并破译该综合征的分子基础。在选定的病例中,青少年口服抗糖尿病药物可改善血糖平衡。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
4.30
自引率
0.00%
发文量
15
审稿时长
8 weeks
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