用于 1 型糖尿病实际研究的生物工程和 omics 方法:进展与制约因素。

Annals of medicine Pub Date : 2025-12-01 Epub Date: 2024-12-20 DOI:10.1080/07853890.2024.2322047
Xi Peng, Ling Li, Yihua Peng, Guangju Zhou, Zhenmei An
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摘要

胰岛素依赖症源于针对胰腺β细胞的自身免疫,从而导致1型糖尿病(T1D)。尽管 T1D 患者需要胰岛素维持生命,但胰岛素并不能治愈这种疾病或预防其并发症。尽管多年来对 T1D 进行了广泛的基因、分子和细胞研究,但将这些认识转化为有效的临床疗法仍然是一个重大障碍。因此,如果没有对疾病病理生理学的透彻了解,就很难制定出有效的临床治疗策略。人类 T1D 的胰腺组织生物工程模型为研究和控制胰岛功能提供了一种有价值的方法,同时还能解决该疾病的各方面问题。近年来,由于高通量组学分析技术的进步,T1D 的基因型和分子谱变得更加精细。本文将探讨这些领域的最新进展及其在 T1D 领域的应用和制约因素。
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Bioengineering and omics approaches for Type 1 diabetes practical research: advancements and constraints.

Insulin dependency arises from autoimmunity that targets the β cells of the pancreas, resulting in Type 1 diabetes (T1D). Despite the fact that T1D patients require insulin for survival, insulin does not provide a cure for this disease or prevent its complications. Despite extensive genetic, molecular, and cellular research on T1D over the years, the translation of this understanding into effective clinical therapies continues to pose a significant obstacle. It is therefore difficult to develop effective clinical treatment strategies without a thorough understanding of disease pathophysiology. Pancreatic tissue bioengineering models of human T1D offer a valuable approach to examining and controlling islet function while tackling various facets of the condition. And in recent years, due to advances in high-throughput omics analysis, the genotypic and molecular profiles of T1D have become finer tuned. The present article will examine recent progress in these areas, along with their utilization and constraints in the realm of T1D.

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