A retrospective study of glucose homeostasis, insulin secretion, sensitivity/resistance in non- transfusion-dependent β-thalassemia patients (NTD- β Thal): reduced β-cell secretion rather than insulin resistance seems to be the dominant defect for glucose dysregulation (GD).

Acta bio-medica : Atenei Parmensis Pub Date : 2023-12-05 DOI:10.23750/abm.v94i6.15001

Vincenzo De Sanctis, Shahina Daar, Ashraf Soliman, Ploutarchos Tzoulis, Mohamed Yassin, Christos Kattamis

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Abstract

Aims: Non-transfusion - dependent β-thalassemias (NTD-βThal) can cause iron overload and serious iron-related organ complications as endocrine dysfunction, including glucose dysregulation (GD).

Patients and methods: We retrieved data of all NTD- β Thal patients referred consecutively to a single Outpatient Italian Clinic from October 2010 to April 2023. All patients underwent a standard 3-h oral glucose tolerance test (OGTT) for analysis of glucose homeostasis, insulin secretion and sensitivity/resistance (IR), using conventional surrogate indices derived from the OGTT. The collected data in NTD- β Thal patients were compared to 20 healthy subjects.

Results: Seventeen of 26 (65.3 %) NTD- β Thal patients (aged: 7.8 -35.1 years) had normal glucose tolerance, 1/26 (3.8 %) had impaired fasting glucose (IFG), 5/26 (19.2 %) impaired glucose tolerance (IGT), 1/26 (3.8%) IFG plus IGT and 2/26 (7.6%) plasma glucose (PG) level ≥155 mg/dL 1-h after glucose load. GD was observed exclusively in young adult patients; none of them had diabetes mellitus (DM). These findings were associated with a low insulinogenic index (IGI) and oral disposition index. HOMA-IR and QUICKI were not significantly different compared to controls. Interestingly, in young adult patients, ISI-Matsuda index was statistically higher compared to the control group, suggesting an increased insulin sensitivity.

Conclusions: This study reported a high prevalence of GD in young adults with NTD- β Thal. The documented reduction of IGI rather than the presence of IR, indicates reduced insulin secretory capacity as the pathophysiological basis of dysglycemia that may represent a novel investigational path for future studies on the mechanism(s) responsible for GD in NTD- β Thal patients.

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一项关于非输血依赖型β地中海贫血患者（NTD- β Thal）葡萄糖稳态、胰岛素分泌、敏感性/抵抗性的回顾性研究显示：β细胞分泌减少而非胰岛素抵抗似乎是葡萄糖失调（GD）的主要缺陷。

目的：非输血依赖型β地中海贫血（NTD-βThal）可导致铁过载和严重的铁相关器官并发症，如内分泌功能障碍，包括血糖失调（GD）：我们检索了 2010 年 10 月至 2023 年 4 月期间连续转诊到一家意大利门诊部的所有 NTD-βThal 患者的数据。所有患者都接受了标准的 3 小时口服葡萄糖耐量试验（OGTT），以分析葡萄糖稳态、胰岛素分泌和敏感性/抵抗性（IR），并使用从 OGTT 得出的常规替代指标。收集到的 NTD-β Thal 患者数据与 20 名健康受试者进行了比较：结果：26 名 NTD- β Thal 患者（年龄：7.8 -35.1 岁）中有 17 人（65.3%）糖耐量正常，1/26（3.8%）空腹血糖受损（IFG），5/26（19.2%）糖耐量受损（IGT），1/26（3.8%）IFG 加 IGT，2/26（7.6%）葡萄糖负荷 1 小时后血浆葡萄糖（PG）水平≥155 mg/dL。GD仅在年轻的成年患者中观察到，他们中没有人患有糖尿病（DM）。这些发现与低胰岛素生成指数（IGI）和口服处置指数有关。与对照组相比，HOMA-IR 和 QUICKI 没有明显差异。有趣的是，与对照组相比，青壮年患者的 ISI-Matsuda 指数在统计学上更高，这表明胰岛素敏感性有所提高：结论：这项研究发现，在患有 NTD-β Thal 的年轻成人中，GD 的发病率很高。IGI的降低而非IR的存在，表明胰岛素分泌能力的降低是导致血糖异常的病理生理基础，这为今后研究NTD- β Thal患者GD的机制提供了一条新的研究途径。

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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Acta bio-medica : Atenei Parmensis

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