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胰岛素治疗的黑人与白人儿童糖尿病发病机制异质性的证据。

Evidence for heterogeneous pathogenesis of insulin-treated diabetes in black and white children.

作者信息

Libman Ingrid M, Pietropaolo Massimo, Arslanian Silva A, LaPorte Ronald E, Becker Dorothy J

机构信息

Department of Pediatrics, Children's Hospital of Pittsburgh, Pittsburgh, Pennsylvania 15213, USA.

出版信息

Diabetes Care. 2003 Oct;26(10):2876-82. doi: 10.2337/diacare.26.10.2876.

Abstract

OBJECTIVE

We have previously reported differences in the prevalence of beta-cell autoantibodies (AAs) in black and white children with insulin-treated diabetes, suggesting that the disease pathogenesis may be more heterogeneous among racial groups than previously thought. To further explore this issue, we compared clinical, biochemical, and autoimmune characteristics at disease diagnosis and follow-up treatment in an expanded number of black and white children with and without the presence of AAs.

RESEARCH DESIGN AND METHODS

The study cohort of 130 black children and adolescents, aged <19 years, diagnosed with diabetes and treated with insulin at time of diagnosis (January 1979 to December 1998) were matched with an equal number of white children by age at onset, sex, and year of diagnosis.

RESULTS

The black children had a higher prevalence of obesity (43 vs. 11%) and acanthosis nigricans (21 vs. 1%) than white children and a lower prevalence of AAs. Compared with black children who had AAs, those with no AAs were older and had a higher prevalence of obesity, acanthosis nigricans, and parental diabetes. However, one of four of the black children with AAs was obese and/or had acanthosis nigricans. Among white children, the absence of AAs was not associated with any differences in terms of obesity or acanthosis nigricans compared with those with AAs. Similar to their black counterparts, white children without antibodies were older and had a higher prevalence of parental diabetes. Although treatment with an insulin sensitizer was used, insulin therapy was rarely discontinued on follow-up.

CONCLUSIONS

These pediatric subjects, irrespective of autoimmunity, often showed characteristics associated with type 2 diabetes. These characteristics were more frequently displayed in black than in white children. Our data suggest that childhood diabetes may constitute a spectrum of pathogenic mechanisms that may overlap, including those typically associated with both type 1 and type 2 diabetes. This finding could have therapeutic implications.

摘要

目的

我们之前报道过接受胰岛素治疗的糖尿病黑人和白人儿童中β细胞自身抗体(AAs)患病率存在差异,这表明疾病发病机制在不同种族群体中可能比之前认为的更加异质。为了进一步探讨这个问题,我们比较了更多有或没有AAs的黑人和白人儿童在疾病诊断和后续治疗时的临床、生化和自身免疫特征。

研究设计与方法

选取1979年1月至1998年12月期间诊断为糖尿病并在诊断时接受胰岛素治疗的130名19岁以下黑人儿童和青少年作为研究队列,根据发病年龄、性别和诊断年份与同等数量的白人儿童进行匹配。

结果

黑人儿童肥胖(43%对11%)和黑棘皮病(21%对1%)的患病率高于白人儿童,而AAs的患病率较低。与有AAs的黑人儿童相比,没有AAs的黑人儿童年龄更大,肥胖、黑棘皮病和父母患糖尿病的患病率更高。然而,有AAs的黑人儿童中有四分之一肥胖和/或患有黑棘皮病。在白人儿童中,与有AAs的儿童相比,没有AAs在肥胖或黑棘皮病方面没有任何差异。与黑人儿童类似,没有抗体的白人儿童年龄更大,父母患糖尿病的患病率更高。尽管使用了胰岛素增敏剂进行治疗,但随访时胰岛素治疗很少中断。

结论

这些儿科患者,无论是否存在自身免疫,常表现出与2型糖尿病相关的特征。这些特征在黑人儿童中比在白人儿童中更常见。我们的数据表明,儿童糖尿病可能构成一系列可能重叠的致病机制,包括那些通常与1型和2型糖尿病相关的机制。这一发现可能具有治疗意义。

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