Diabetes Center, Massachusetts General Hospital, Harvard Medical School, Boston, MA, USA.
Diabetologia. 2021 May;64(5):1049-1058. doi: 10.1007/s00125-021-05397-4. Epub 2021 Feb 6.
The introduction of insulin in the treatment of juvenile-onset, now type 1, diabetes mellitus transformed a rapidly fatal disease into a chronic degenerative one. During the insulin-treatment era, long-term microvascular and cardiovascular complications proved to be the bane of existence for people with type 1 diabetes, leading to blindness, kidney failure, amputations, cardiovascular disease (CVD) and premature mortality. The nascent understanding of the link between non-physiologically regulated glucose levels and these complications led to the development of new treatment tools in the 1970s and 1980s that facilitated the delivery of insulin to achieve glucose levels closer to non-diabetic levels. These therapeutic advances set the stage for definitive testing of the glucose hypothesis. The Diabetes Control and Complications Trial (DCCT), supported by the National Institute of Diabetes Digestive and Kidney Diseases, National Institutes of Health (NIH), definitively established the benefits and risks of intensive therapy that substantially lowered mean blood glucose levels, measured by HbA, over a mean 6.5 years of therapy. Intensive therapy in the DCCT, resulting in a mean HbA of ~7% (53 mmol/mol), reduced the development and progression of early microvascular and neurological complications associated with diabetes by 34-76% compared with the conventional-treatment group, which maintained an HbA of ~9% (75 mmol/mol). Intensive therapy was also associated with weight gain and a threefold increased risk for hypoglycaemia. At the end of the DCCT, a long-term observational follow-up study, the Epidemiology of Diabetes Interventions and Complications (EDIC) study, commenced. Despite the convergence of HbA levels between the two groups during EDIC, owing to the adoption of intensive therapy by the original DCCT conventional-treatment group and the return of all participants to their own healthcare providers for diabetes care, the development and progression of complications continued to be substantially less in the original intensive-treatment group vs the conventional-treatment group; this phenomenon was termed 'metabolic memory'. The DCCT demonstrated a major reduction in early-stage complications with intensive therapy and the metabolic memory phenomenon during EDIC contributed to a substantially lower burden of advanced complications over time. These included a 57% lower risk of CVD events and 33% lower rate of mortality in the original intensive-treatment group compared with the conventional-treatment group. DCCT/EDIC has ushered in the intensive-treatment era, which has been universally adopted and includes the goal of achieving HbA levels less than 7% (53 mmol/mol) for most patients. Although the challenge of making intensive therapy (with the aim of achieving normoglycaemia) as widely accessible and safe as possible remains, continuing improvements in insulin therapy 100 years after its introduction promise a brighter future for people with type 1 diabetes.
胰岛素的引入治疗青少年起病的、现称 1 型糖尿病,将这种迅速致命的疾病转变为慢性进行性疾病。在胰岛素治疗时代,长期的微血管和心血管并发症被证明是 1 型糖尿病患者生存的祸根,导致失明、肾衰竭、截肢、心血管疾病 (CVD) 和过早死亡。人们对非生理调节的血糖水平与这些并发症之间的联系的初步认识,导致了 20 世纪 70 年代和 80 年代新治疗工具的发展,这些工具促进了胰岛素的输送,以实现更接近非糖尿病水平的血糖水平。这些治疗进展为血糖假说的确定性检验奠定了基础。美国国立卫生研究院(NIH)国家糖尿病、消化和肾脏疾病研究所(NIDDK)支持的糖尿病控制和并发症试验(DCCT)明确证实了强化治疗的益处和风险,强化治疗在 6.5 年的治疗中显著降低了平均血糖水平,以 HbA 衡量。DCCT 中的强化治疗导致平均 HbA 为7%(53mmol/mol),与常规治疗组相比,早期微血管和神经并发症的发展和进展降低了 34-76%,常规治疗组的 HbA 为9%(75mmol/mol)。强化治疗还与体重增加和低血糖风险增加三倍有关。在 DCCT 结束时,开始了一项长期观察性随访研究,即糖尿病干预和并发症流行病学 (EDIC) 研究。尽管 EDIC 期间两组的 HbA 水平趋于一致,这是由于最初的 DCCT 常规治疗组采用了强化治疗,以及所有参与者都回到自己的医疗保健提供者那里接受糖尿病护理,但最初的强化治疗组与常规治疗组相比,并发症的发展和进展仍然明显减少;这种现象被称为“代谢记忆”。DCCT 表明强化治疗可显著降低早期并发症的发生,而 EDIC 中的代谢记忆现象导致随着时间的推移,晚期并发症的负担大大降低。与常规治疗组相比,这包括心血管疾病事件风险降低 57%和死亡率降低 33%。DCCT/EDIC 开创了强化治疗时代,该时代已被普遍采用,包括大多数患者 HbA 水平低于 7%(53mmol/mol)的目标。尽管使强化治疗(旨在实现正常血糖)尽可能广泛地普及和安全仍然是一个挑战,但胰岛素治疗在引入 100 年后的持续改进有望为 1 型糖尿病患者带来更美好的未来。
