In humans increase in intrapancreatic adipose tissue predicts beta-cell dedifferentiation score before diabetes onset: A pilot study

IF 7.4 3区 医学 Q1 ENDOCRINOLOGY & METABOLISM Diabetes research and clinical practice Pub Date : 2025-02-10 DOI:10.1016/j.diabres.2025.112029
Francesca Cinti , Teresa Mezza , Ilenia Severi , Simona Moffa , Gianfranco Di Giuseppe , Umberto Capece , Gea Ciccarelli , Laura Soldovieri , Michela Brunetti , Cassandra Morciano , Shawn Gugliandolo , Martina Senzacqua , Adriana Avolio , Giuseppe Quero , Vincenzo Tondolo , Enrico Celestino Nista , Rossana Moroni , Saverio Cinti , Sergio Alfieri , Antonio Gasbarrini , Andrea Giaccari
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Abstract

Background

The role of intrapancreatic fat (WAT) in the development of T2D remains debated. In T2D, β-cell dedifferentiation is one of the mechanisms responsible for β-cell failure but its role in prediabetes is unknown. We aimed to investigate the relation between WAT and β-cell dedifferentiation prior to diabetes onset.

Methods

We evaluated pancreatic samples from patients without history of diabetes, who had previously undergone an oral glucose tolerance test and hyperglycemic clamp. Subjects were divided into 3 glucose tolerance groups: normal (NGT), altered (IGT) or newly diagnosed diabetes (nDM). Dedifferentiation and WAT% were morphologically assessed.

Results

WAT was higher in nDM patients compared to NGT and IGT (WAT nDM 43.79 ± 20.83 %, IGT 10.67 ± 8.5 %, NGT 4.43 ± 4.37 %). We observed a progressive increase in dedifferentiation score, in parallel with worsening glucose tolerance (from NGT to IGT to nDM; 4.8 ± 3.8; 32.37 ± 7.4; 40.38 ± 19 respectively). A strong linear regression established that WAT could statistically significantly predict dedifferentiated β-cells (R = 0.86, p = 0.005), and that the predicted increase in dedifferentiated β-cells was 1.25 points for every extra one-point change in WAT. Interestingly, the WAT and dedifferentiation score variable pair were significantly related to 1-hour post-load glycemia.

Conclusions

The accumulation of WAT might be responsible for dedifferentiation, making it a potential new target to curb diabetes onset.
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人类胰腺内脂肪组织的增加在糖尿病发病前预测β细胞去分化评分:一项初步研究
胰腺内脂肪(WAT)在T2D发展中的作用仍有争议。在T2D中,β细胞去分化是导致β细胞衰竭的机制之一,但其在前驱糖尿病中的作用尚不清楚。我们的目的是研究糖尿病发病前WAT与β细胞去分化之间的关系。方法:我们对无糖尿病病史的患者的胰腺样本进行评估,这些患者之前接受过口服葡萄糖耐量试验和高血糖钳夹。受试者被分为3个糖耐量组:正常(NGT)、改变(IGT)或新诊断的糖尿病(nDM)。形态学评估去分化和WAT%。结果nDM患者的swat高于NGT和IGT (WAT nDM 43.79±20.83%,IGT 10.67±8.5%,NGT 4.43±4.37%)。我们观察到去分化评分逐渐增加,同时糖耐量也在恶化(从NGT到IGT再到nDM;4.8±3.8;32.37±7.4;40.38±19)。强线性回归证实,WAT能显著预测β-细胞的去分化(R = 0.86, p = 0.005), WAT每增加1点,预测β-细胞的去分化增加1.25点。有趣的是,WAT和去分化评分变量对与负荷后1小时血糖显著相关。结论WAT的积累可能与去分化有关,是抑制糖尿病发病的潜在新靶点。
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来源期刊
Diabetes research and clinical practice
Diabetes research and clinical practice 医学-内分泌学与代谢
CiteScore
10.30
自引率
3.90%
发文量
862
审稿时长
32 days
期刊介绍: Diabetes Research and Clinical Practice is an international journal for health-care providers and clinically oriented researchers that publishes high-quality original research articles and expert reviews in diabetes and related areas. The role of the journal is to provide a venue for dissemination of knowledge and discussion of topics related to diabetes clinical research and patient care. Topics of focus include translational science, genetics, immunology, nutrition, psychosocial research, epidemiology, prevention, socio-economic research, complications, new treatments, technologies and therapy.
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