首页> 外文OA文献 >Insulin therapy in diabetes and cancer risk: current understanding and implications for future study: proceedings from a meeting of a European Insulin Safety Consensus Panel, convened and sponsored by Novo Nordisk, held Tuesday October 5, 2010 at The Radisson Edwardian Heathrow Hotel, Hayes, Middlesex, UK.
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Insulin therapy in diabetes and cancer risk: current understanding and implications for future study: proceedings from a meeting of a European Insulin Safety Consensus Panel, convened and sponsored by Novo Nordisk, held Tuesday October 5, 2010 at The Radisson Edwardian Heathrow Hotel, Hayes, Middlesex, UK.

机译:糖尿病和癌症风险中的胰岛素治疗:当前的理解和对未来研究的意义:由诺和诺德(Novo Nordisk)召集和赞助的欧洲胰岛素安全共识小组会议的会议记录,会议于2010年10月5日星期二在海斯的Radisson Edwardian Heathrow Hotel举行,英国米德尔塞克斯。

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摘要

INTRODUCTION: Interest in the possibility of certain insulin treatments having the potential to modify cancer development and prognosis was reawakened in 2009, following publication of several epidemiological studies addressing this issue. This interest extends to how diabetes itself and cancer might be linked, and makes desirable an exchange of expert views and knowledge to enhance understanding in this subject among those treating diabetes and cancer, or those developing diabetes therapies. METHODS: A European meeting was convened with participants invited based on known relevant interests in endocrinology, oncology, epidemiology, and insulin analog design and investigation. Experts in these fields were invited to present on relevant topics, with open discussions held after each presentation. RESULTS: Concern over the potential mitogenic properties of certain insulin analogs has arisen from some (but not all) epidemiological studies, although confounding factors render interpretation controversial. Future epidemiological studies are likely to strengthen confidence in drawing conclusions. Meanwhile, pharmacological studies, and a consideration of cancer pathophysiology, implicate increased insulin-like growth factor-1 receptor affinity, and/or deranged insulin receptor interaction/signaling properties as possible a priori causes for concern with some insulin analogs. Again, interpretation of the body of pharmacological evidence is confounded by the array of test systems and methodologies used, and by studies frequently succumbing to methodological pitfalls. Reassuringly, most available insulin analogs do not differ in their receptor interaction response profile to human insulin, and for those that do there are reasons to question any potential clinical relevance. Nevertheless, it is desirable that new experimental models are devised that can better determine the likely clinical consequences of any variance in receptor response profile versus human insulin. CONCLUSION: More data are required to increase our understanding of this issue. To facilitate and disseminate such understanding, close cooperation and communication between diabetologists, epidemiologists, oncologists, and insulin engineers will be essential.
机译:简介:在针对这一问题的几项流行病学研究发表后,对某些胰岛素治疗可能改变癌症发展和预后的可能性的兴趣在2009年重新引起人们的注意。这种兴趣扩展到了糖尿病本身与癌症之间的联系方式,并希望交流专家的观点和知识,以增进那些在治疗糖尿病和癌症的人或正在开发糖尿病疗法的人对该学科的理解。方法:根据内分泌学,肿瘤学,流行病学以及胰岛素类似物设计和研究的已知相关兴趣,召集了欧洲会议并邀请了与会人员。邀请了这些领域的专家就相关主题进行演讲,每次演讲后进行公开讨论。结果:一些(但不是全部)流行病学研究引起了对某些胰岛素类似物潜在促有丝分裂特性的担忧,尽管混杂因素使解释存在争议。未来的流行病学研究可能会增强对得出结论的信心。同时,药理学研究以及对癌症病理生理学的考虑暗示胰岛素样生长因子-1受体亲和力的增加和/或胰岛素受体相互作用/信号特性的紊乱可能是某些胰岛素类似物引起关注的先验原因。再次,对药理学证据的解释被所使用的一系列测试系统和方法论以及经常屈服于方法论陷阱的研究所混淆。可以放心的是,大多数可用的胰岛素类似物在与人胰岛素的受体相互作用中没有差异,对于那些胰岛素类似物,有理由质疑任何潜在的临床意义。然而,希望设计新的实验模型,以更好地确定与人胰岛素相比受体反应谱的任何变化的可能的临床后果。结论:需要更多数据以增进我们对这个问题的理解。为了促进和传播这种理解,糖尿病学家,流行病学家,肿瘤学家和胰岛素工程师之间的密切合作和交流将至关重要。

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