基于 ADA 2026 标准 · 持续更新至 2026 年 5 月Based on ADA 2026 Standards · Updated through May 2026

糖尿病系统知识中心A Systematic Diabetes Knowledge Hub

关于糖尿病的系统知识库 —— 病理生理、诊断、治疗与药物研发前沿A knowledge base on diabetes — pathophysiology, diagnosis, treatment, and drug development frontiers

系统整理糖尿病相关的病理生理、分型与诊断、药物治疗、日常管理以及 2024–2026 年最新临床进展。所有内容均标注权威来源(ADA、EASD、NEJM、Nature、PubMed 等), 面向临床医生、研究者与药物研发团队使用。

A structured overview of diabetes pathophysiology, classification and diagnosis, pharmacotherapy, daily management, and the latest clinical advances of 2024–2026. Every item is referenced to authoritative sources (ADA, EASD, NEJM, Nature, PubMed, etc.), designed for clinicians, researchers, and drug-development teams.

关键流行病学数据Key Epidemiology

5.89 亿589 M
全球 20–79 岁糖尿病患者(2024)Adults aged 20–79 with diabetes worldwide (2024)
IDF Diabetes Atlas, 11th ed.
~90%
为 2 型糖尿病Type 2 diabetes share
WHO / IDF
1.41 亿141 M
中国糖尿病患者数(全球居首)China — largest diabetes population
IDF 2024
38%
未确诊比例Undiagnosed worldwide
IDF 2024
主题导航 · BROWSE BY TOPICBROWSE BY TOPIC

从基础到前沿,结构化呈现From fundamentals to frontiers, structured

知识体系分为六大模块,从分型诊断到最新临床试验,再到药物研发的靶点与管线。

The knowledge base is organized into six modules — from classification and diagnosis to the latest clinical trials, and on to drug-development targets and pipelines.

基础知识Basics
Pathophysiology · Classification · Diagnosis
糖尿病分型(1 型 / 2 型 / 妊娠 / LADA / MODY)、胰岛素信号通路、β 细胞功能障碍、 胰岛素抵抗机制、ADA 2026 诊断标准、急慢性并发症。
Diabetes classification (type 1 / type 2 / gestational / LADA / MODY), insulin signaling pathways, β-cell dysfunction, insulin-resistance mechanisms, ADA 2026 diagnostic criteria, acute and chronic complications.
阅读 →Read →
治疗方案Treatment
Pharmacotherapy · Insulin · Individualization
口服药(二甲双胍、SGLT2i、DPP-4i 等)、GLP-1 受体激动剂、胰岛素治疗策略、 联合用药、心肾保护策略与个体化方案。
Oral agents (metformin, SGLT2i, DPP-4i, etc.), GLP-1 receptor agonists, insulin strategies, combination therapy, cardio-renal protection, and individualized regimens.
阅读 →Read →
日常管理Daily Management
Nutrition · Exercise · Self-monitoring · CGM
营养处方(地中海饮食、低碳水化合物、生酮)、运动处方、血糖监测、 CGM 使用指南、AID 闭环系统、心理调适与体重管理。
Nutrition plans (Mediterranean, low-carbohydrate, ketogenic), exercise prescriptions, glucose monitoring, CGM guidance, AID closed-loop systems, psychological adjustment, and weight management.
阅读 →Read →
最新研究进展Latest Research
Breakthroughs 2024–2026
Vertex zimislecel 干细胞疗法、Lilly retatrutide 三激动剂、口服 GLP-1 orforglipron、 teplizumab 免疫疗法、MASH 治疗、AID 系统等突破。
Breakthroughs including Vertex zimislecel stem-cell therapy, Lilly retatrutide triple agonist, oral GLP-1 orforglipron, teplizumab immunotherapy, MASH treatment, and AID systems.
阅读 →Read →
药物研发参考Drug Development
Targets · Pipeline · Unmet Needs
重点研发靶点(GLP-1/GIP/glucagon、amylin、PYY、FGF21)、多激动剂策略、 肠道菌群与新机制、未满足医学需求、生物标志物、临床试验设计要点。
Key targets (GLP-1/GIP/glucagon, amylin, PYY, FGF21), multi-agonist strategies, gut microbiota and novel mechanisms, unmet medical needs, biomarkers, and clinical-trial design considerations.
阅读 →Read →
参考文献汇总References
All cited sources
所有页面引用的指南、综述、原始研究、临床试验数据库与机构官方资料的完整链接列表。
A complete list of links to the guidelines, reviews, primary studies, clinical-trial registries, and official institutional materials cited across the site.
查看 →View →
2026 年焦点 · 2026 HIGHLIGHTS2026 HIGHLIGHTS

近期临床与监管要事Recent clinical and regulatory milestones

从 ADA 2026 标准更新、Vertex 干细胞 III 期到 Lilly retatrutide III 期数据, 2025–2026 年是糖尿病治疗史上变化最快的一年。

From the ADA 2026 Standards update to Vertex's phase III stem-cell data and Lilly's retatrutide phase III readouts, 2025–2026 has been the fastest-moving period in the history of diabetes treatment.

已批准Approved T1D

ADA 2026 指南:AID 闭环系统成首选ADA 2026 guidelines: AID closed-loop systems become first choice Standards of Care

2026 版 ADA 标准取消了 1 型糖尿病启动自动胰岛素输送(AID)的多项限制 (包括 C-肽水平、自身抗体、胰岛素治疗时长),并首次推荐 GLP-1 类药物用于 合并肥胖的 T1D 患者。

The 2026 ADA Standards removed several restrictions on initiating automated insulin delivery (AID) in type 1 diabetes (including C-peptide level, autoantibodies, and duration of insulin therapy), and for the first time recommend GLP-1 drugs for T1D patients with comorbid obesity.

来源:Source: ADA Press Release, Dec 2025 · Diabetes Care 2026

III 期Phase III T1D

Vertex zimislecel:12/12 患者恢复 C-肽分泌Vertex zimislecel: 12/12 patients restored C-peptide secretion Stem-cell islet therapy

FORWARD 试验更新数据(ADA 2025):全剂量组 10/10 患者一年后无需外源性胰岛素, 时间在范围内(TIR)> 90%。Vertex 计划 2026 年向 FDA / EMA / MHRA 提交注册申请。

Updated FORWARD trial data (ADA 2025): 10/10 patients in the full-dose group were free of exogenous insulin at one year, with time in range (TIR) > 90%. Vertex plans to file for registration with the FDA / EMA / MHRA in 2026.

来源:Source: Vertex Newsroom, Jun 2025 · CGTLive

III 期Phase III T2D

Retatrutide:三激动剂 III 期 T2D 数据公布Retatrutide: triple-agonist phase III T2D data released GLP-1/GIP/glucagon

Eli Lilly 的 retatrutide 在 40 周时使 HbA1c 平均下降 1.7%–2.0%,最高剂量组减重 16.8%(约 36.6 磅)。 TRIUMPH 项目下另有 6 项 III 期研究预计 2026 年底前读出。

Eli Lilly's retatrutide lowered HbA1c by an average of 1.7%–2.0% at 40 weeks, with 16.8% weight loss (about 36.6 lb) in the highest-dose group. Six further phase III studies under the TRIUMPH program are expected to read out before the end of 2026.

来源:Source: CNBC, Mar 2026 · BioSpace

已批准Approved T2D / 肥胖T2D / Obesity

口服 GLP-1 Orforglipron 获批Oral GLP-1 orforglipron approved Oral small-molecule GLP-1RA

Lilly 的 orforglipron(商品名 Foundayo)作为首个口服小分子 GLP-1RA 于 2026 年 4 月获 FDA 批准, ATTAIN-1 III 期试验中减重达 14.7%;A1C 降幅优于司美格鲁肽与达格列净(头对头)。

Lilly's orforglipron (brand name Foundayo), the first oral small-molecule GLP-1RA, was approved by the FDA in April 2026, with 14.7% weight loss in the ATTAIN-1 phase III trial; its A1C reduction was superior to semaglutide and dapagliflozin (head-to-head).

来源:Source: GoodRx, 2026 · IQVIA Outlook 2026

💊 面向药物研发的内容设计 · DRUG DEVELOPMENT FOCUS💊 DRUG DEVELOPMENT FOCUS

本知识库的目标之一是为糖尿病新药研发提供结构化参考。每个模块均关注:

One goal of this knowledge base is to provide a structured reference for diabetes drug development. Each module focuses on:

  • 分子机制与靶点:从胰岛素信号通路到肠促胰素受体家族
  • 未满足的医学需求:β 细胞功能恢复、并发症逆转、口服递送等
  • 临床试验景观:正在进行的关键 II/III 期研究与读出节点
  • 生物标志物:C-肽、自身抗体、CGM 衍生指标(TIR / GMI)
  • 监管路径:FDA / EMA / NMPA 的关键指导原则
  • Molecular mechanisms and targets: from insulin signaling pathways to the incretin receptor family
  • Unmet medical needs: β-cell function restoration, complication reversal, oral delivery, etc.
  • Clinical-trial landscape: key ongoing phase II/III studies and readout milestones
  • Biomarkers: C-peptide, autoantibodies, CGM-derived metrics (TIR / GMI)
  • Regulatory pathways: key guidance from the FDA / EMA / NMPA

详见 药物研发参考 →See Drug Development reference →