胰高血糖素样1肽受体激动剂(GLP-1RAs)在新版NICE指南中的地位——发生了什么?

IF 0.4 Q4 ENDOCRINOLOGY & METABOLISM British Journal of Diabetes Pub Date : 2022-12-21 DOI:10.15277/bjd.2022.381
Stephen C. Bain
{"title":"胰高血糖素样1肽受体激动剂(GLP-1RAs)在新版NICE指南中的地位——发生了什么?","authors":"Stephen C. Bain","doi":"10.15277/bjd.2022.381","DOIUrl":null,"url":null,"abstract":"The article by Miles Fisher in this edition of the British Journal of Diabetes discusses cardiovascular outcome trials (CVOTs) which have examined the impact of GLP-1RAs in type 2 diabetes (T2DM). He queries ‘why updated guidance from NICE...fails to acknowledge the evidence-based cardiovascular benefits’. Indeed, clinicians in the UK will be puzzled as to why this class of glucose-lowering therapy is now a first-line option in European and North American guidelines for people with T2DM at high cardiovascular risk, but remains well down the pecking order in NICE guideline (NG) 28.1-3 This editorial will provide a short précis of the history of GLP-1RAs and NICE and try to explain the current impasse. The National Institute of Clinical Excellence (NICE) was established in 1999 to ‘diffuse the postcode lottery’ of healthcare (for example, varying access to medicines according to where people lived) and serves the National Health Services (NHS) in England, Northern Ireland and Wales. Since its set-up, there have been two changes in name, the National Institute for Health and Clinical Excellence (2005) and the National Institute for Health and Care Excellence (2013) but the abbreviation of NICE has stood the test of time and is a globally recognised brand. Well over fifty countries world-wide access guidelines produced by NICE rather than doing their own in-depth assessment of new medicines.4 When it was launched, NICE inherited various guidelines for the management of T2DM, which were rebadged. It produced its first clinical guideline for T2DM (CG66) in 2008.5 This was rapidly followed by the release of CG87 in May 2009, which was a short update on the ‘newer agents’ for blood glucose lowering.6 This guideline included exenatide, given twice daily, which was the first GLP-1RA to be licensed in the UK (in 2007). Exenatide was positioned as a third-line ‘alternative’ add-on therapy to be considered after insulin, a thiazolidinedione or a dipeptidyl peptase-4 inhibitor and it was only sanctioned for use with metformin and a sulfonylurea. CG87 introduced the body mass index (BMI) cut-off of 35 Kg/m2 for GLP-1RAs, which was not based on data from clinical trials but was the BMI at which the average cost of a long-acting insulin analogue was the same as BD exenatide. NICE also introduced ‘stopping rules’ where exenatide should be withheld when a reduction of at least 1% (11mmol/mol) in HbA1c and weight loss of at least 3% initial body weight was not achieved after six months. Stopping rules have not been recommended for any other glucose-lowering class. The next NICE guidance for the management of T2DM (NG28) was published in 2015 and is best remembered for the furore created by the recommendation of repaglinide as firstline treatment for people intolerant of metformin.7,8 In the preceding six years, GLP-1RAs had been added to the glucoselowering algorithm by means of single technology appraisals (TAs). These individual assessments by NICE had a more binding legal status than their guidelines, in that a positive TA recommendation mandated that funding should be made available by clinical commissioning groups. Thus, liraglutide (TA203, 2010), exenatide extended-release (TA248, 2012) and lixisenatide (2013) were all sanctioned for use, although NICE limited the dose of liraglutide to a maximum of 1.2mg OD on the basis that this dose had the same acquisition cost as BD exenatide.9-11 The overall position of GLP-1RAs in the glucose-lowering algorithm was unchanged, however. They remained a third-line option for consideration after various triple oral combinations or insulin and were not even mentioned for people who could not tolerate metformin or for whom it was contra-indicated. The first CVOT of a glucose-lowering therapy to demonstrate superiority was the EMPA-REG OUTCOME study of empagliflozin, a sodium-glucose co-transporter 2 (SGLT2) inhibitor, and this trial was published three months before NG28 was launched in December 2015.12 NG28 did not take into account these positive data, but this was not thought to be important since NICE had committed to regular updates every two years and more CVOT data were in the pipeline. Indeed, in 2016 there were positive CVOTs for both liraglutide (LEADER) and onceweekly semaglutide (SUSTAIN 6).13,14 The positive superiority CVOT for dulaglutide (REWIND) was published in 2019 and there 1 Swansea University Medical School, Swansea, UK","PeriodicalId":42951,"journal":{"name":"British Journal of Diabetes","volume":null,"pages":null},"PeriodicalIF":0.4000,"publicationDate":"2022-12-21","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"The place of Glucagon-like 1 peptide receptor agonists (GLP-1RAs) in the new NICE guidelines – what is going on?\",\"authors\":\"Stephen C. Bain\",\"doi\":\"10.15277/bjd.2022.381\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"The article by Miles Fisher in this edition of the British Journal of Diabetes discusses cardiovascular outcome trials (CVOTs) which have examined the impact of GLP-1RAs in type 2 diabetes (T2DM). He queries ‘why updated guidance from NICE...fails to acknowledge the evidence-based cardiovascular benefits’. Indeed, clinicians in the UK will be puzzled as to why this class of glucose-lowering therapy is now a first-line option in European and North American guidelines for people with T2DM at high cardiovascular risk, but remains well down the pecking order in NICE guideline (NG) 28.1-3 This editorial will provide a short précis of the history of GLP-1RAs and NICE and try to explain the current impasse. The National Institute of Clinical Excellence (NICE) was established in 1999 to ‘diffuse the postcode lottery’ of healthcare (for example, varying access to medicines according to where people lived) and serves the National Health Services (NHS) in England, Northern Ireland and Wales. Since its set-up, there have been two changes in name, the National Institute for Health and Clinical Excellence (2005) and the National Institute for Health and Care Excellence (2013) but the abbreviation of NICE has stood the test of time and is a globally recognised brand. Well over fifty countries world-wide access guidelines produced by NICE rather than doing their own in-depth assessment of new medicines.4 When it was launched, NICE inherited various guidelines for the management of T2DM, which were rebadged. It produced its first clinical guideline for T2DM (CG66) in 2008.5 This was rapidly followed by the release of CG87 in May 2009, which was a short update on the ‘newer agents’ for blood glucose lowering.6 This guideline included exenatide, given twice daily, which was the first GLP-1RA to be licensed in the UK (in 2007). Exenatide was positioned as a third-line ‘alternative’ add-on therapy to be considered after insulin, a thiazolidinedione or a dipeptidyl peptase-4 inhibitor and it was only sanctioned for use with metformin and a sulfonylurea. CG87 introduced the body mass index (BMI) cut-off of 35 Kg/m2 for GLP-1RAs, which was not based on data from clinical trials but was the BMI at which the average cost of a long-acting insulin analogue was the same as BD exenatide. NICE also introduced ‘stopping rules’ where exenatide should be withheld when a reduction of at least 1% (11mmol/mol) in HbA1c and weight loss of at least 3% initial body weight was not achieved after six months. Stopping rules have not been recommended for any other glucose-lowering class. The next NICE guidance for the management of T2DM (NG28) was published in 2015 and is best remembered for the furore created by the recommendation of repaglinide as firstline treatment for people intolerant of metformin.7,8 In the preceding six years, GLP-1RAs had been added to the glucoselowering algorithm by means of single technology appraisals (TAs). These individual assessments by NICE had a more binding legal status than their guidelines, in that a positive TA recommendation mandated that funding should be made available by clinical commissioning groups. Thus, liraglutide (TA203, 2010), exenatide extended-release (TA248, 2012) and lixisenatide (2013) were all sanctioned for use, although NICE limited the dose of liraglutide to a maximum of 1.2mg OD on the basis that this dose had the same acquisition cost as BD exenatide.9-11 The overall position of GLP-1RAs in the glucose-lowering algorithm was unchanged, however. They remained a third-line option for consideration after various triple oral combinations or insulin and were not even mentioned for people who could not tolerate metformin or for whom it was contra-indicated. The first CVOT of a glucose-lowering therapy to demonstrate superiority was the EMPA-REG OUTCOME study of empagliflozin, a sodium-glucose co-transporter 2 (SGLT2) inhibitor, and this trial was published three months before NG28 was launched in December 2015.12 NG28 did not take into account these positive data, but this was not thought to be important since NICE had committed to regular updates every two years and more CVOT data were in the pipeline. Indeed, in 2016 there were positive CVOTs for both liraglutide (LEADER) and onceweekly semaglutide (SUSTAIN 6).13,14 The positive superiority CVOT for dulaglutide (REWIND) was published in 2019 and there 1 Swansea University Medical School, Swansea, UK\",\"PeriodicalId\":42951,\"journal\":{\"name\":\"British Journal of Diabetes\",\"volume\":null,\"pages\":null},\"PeriodicalIF\":0.4000,\"publicationDate\":\"2022-12-21\",\"publicationTypes\":\"Journal Article\",\"fieldsOfStudy\":null,\"isOpenAccess\":false,\"openAccessPdf\":\"\",\"citationCount\":\"0\",\"resultStr\":null,\"platform\":\"Semanticscholar\",\"paperid\":null,\"PeriodicalName\":\"British Journal of Diabetes\",\"FirstCategoryId\":\"1085\",\"ListUrlMain\":\"https://doi.org/10.15277/bjd.2022.381\",\"RegionNum\":0,\"RegionCategory\":null,\"ArticlePicture\":[],\"TitleCN\":null,\"AbstractTextCN\":null,\"PMCID\":null,\"EPubDate\":\"\",\"PubModel\":\"\",\"JCR\":\"Q4\",\"JCRName\":\"ENDOCRINOLOGY & METABOLISM\",\"Score\":null,\"Total\":0}","platform":"Semanticscholar","paperid":null,"PeriodicalName":"British Journal of Diabetes","FirstCategoryId":"1085","ListUrlMain":"https://doi.org/10.15277/bjd.2022.381","RegionNum":0,"RegionCategory":null,"ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"Q4","JCRName":"ENDOCRINOLOGY & METABOLISM","Score":null,"Total":0}
引用次数: 0

摘要

Miles Fisher在本期《英国糖尿病杂志》上发表的文章讨论了心血管结果试验(CVOT),该试验检测了GLP-1RA对2型糖尿病(T2DM)的影响。他质疑“为什么NICE更新了指南。。。未能承认循证心血管益处”。事实上,英国的临床医生会感到困惑,为什么这类降糖治疗现在是欧洲和北美指南中针对心血管高危T2DM患者的一线选择,但在NICE指南(NG)28.1-3中排名靠后。这篇社论将简要介绍GLP-1RA和NICE的历史,并试图解释目前的僵局。国家临床卓越研究所(NICE)成立于1999年,旨在“分散医疗保健的邮政编码抽签”(例如,根据人们的居住地不同获得药物的机会),并为英格兰、北爱尔兰和威尔士的国家医疗服务体系(NHS)服务。自成立以来,名称发生了两次变化,即国家健康与临床卓越研究所(2005年)和国家健康与护理卓越研究院(2013年),但NICE的缩写经受住了时间的考验,是一个全球公认的品牌。全球有50多个国家制定了NICE获得指南,而不是自己对新药进行深入评估。4当它推出时,NICE继承了T2DM管理的各种指南,这些指南被重新调整了。它于2008年制定了首个T2DM临床指南(CG66)。5随后,CG87于2009年5月迅速发布,这是对降血糖“新药物”的简短更新。6该指南包括艾塞那肽,每天两次,这是第一个在英国获得许可的GLP-1RA(2007年)。艾塞那肽被定位为继胰岛素、噻唑烷二酮或二肽基肽酶-4抑制剂之后考虑的第三线“替代”添加疗法,它只被批准与二甲双胍和磺酰脲一起使用。CG87引入了GLP-1RA的体重指数(BMI)临界值35 Kg/m2,这不是基于临床试验的数据,而是长效胰岛素类似物的平均成本与BD艾塞那肽相同的BMI。NICE还引入了“停止规则”,即当HbA1c减少至少1%(11mmol/mol),且六个月后初始体重未减少至少3%时,应停止使用艾塞那肽。停止规则没有被推荐用于任何其他降血糖类别。下一份NICE关于T2DM(NG28)管理的指南于2015年发布,人们最怀念的是瑞格列奈作为二甲双胍不耐受人群一线治疗的推荐所引起的轰动。7,8在过去的六年里,GLP-1RA通过单一技术评估(TA)被添加到葡萄糖代谢算法中。NICE的这些个人评估比其指导方针具有更具约束力的法律地位,因为TA的积极建议要求临床委托小组提供资金。因此,利拉鲁肽(TA2032010)、艾塞那肽缓释剂(TA2482012)和利西那肽(2013)都被批准使用,尽管NICE将利拉鲁的剂量限制在最大1.2mg OD,因为该剂量与BD艾塞那苷的获取成本相同。9-11然而,GLP-1RA在降糖算法中的总体地位没有变化。在各种三重口服组合或胰岛素后,它们仍然是一种可供考虑的第三线选择,甚至没有提到不能耐受二甲双胍或二甲双胍禁忌的人。证明其优越性的第一个降血糖治疗CVOT是对恩帕列嗪(一种钠-葡萄糖共转运蛋白2(SGLT2)抑制剂)的EMPA-REG结果研究,该试验在2015年12月NG28上市前三个月发表。12 NG28没有考虑这些阳性数据,但这并不重要,因为NICE承诺每两年定期更新一次,而且更多的CVOT数据正在酝酿中。事实上,2016年利拉鲁肽(LEADER)和每周一次的西格鲁肽(SUSTAIN 6)都有阳性CVOT。13,14杜拉鲁肽(REWIND)的阳性优势CVOT于2019年发表,英国斯旺西斯旺西大学医学院1所
本文章由计算机程序翻译,如有差异,请以英文原文为准。
查看原文
分享 分享
微信好友 朋友圈 QQ好友 复制链接
本刊更多论文
The place of Glucagon-like 1 peptide receptor agonists (GLP-1RAs) in the new NICE guidelines – what is going on?
The article by Miles Fisher in this edition of the British Journal of Diabetes discusses cardiovascular outcome trials (CVOTs) which have examined the impact of GLP-1RAs in type 2 diabetes (T2DM). He queries ‘why updated guidance from NICE...fails to acknowledge the evidence-based cardiovascular benefits’. Indeed, clinicians in the UK will be puzzled as to why this class of glucose-lowering therapy is now a first-line option in European and North American guidelines for people with T2DM at high cardiovascular risk, but remains well down the pecking order in NICE guideline (NG) 28.1-3 This editorial will provide a short précis of the history of GLP-1RAs and NICE and try to explain the current impasse. The National Institute of Clinical Excellence (NICE) was established in 1999 to ‘diffuse the postcode lottery’ of healthcare (for example, varying access to medicines according to where people lived) and serves the National Health Services (NHS) in England, Northern Ireland and Wales. Since its set-up, there have been two changes in name, the National Institute for Health and Clinical Excellence (2005) and the National Institute for Health and Care Excellence (2013) but the abbreviation of NICE has stood the test of time and is a globally recognised brand. Well over fifty countries world-wide access guidelines produced by NICE rather than doing their own in-depth assessment of new medicines.4 When it was launched, NICE inherited various guidelines for the management of T2DM, which were rebadged. It produced its first clinical guideline for T2DM (CG66) in 2008.5 This was rapidly followed by the release of CG87 in May 2009, which was a short update on the ‘newer agents’ for blood glucose lowering.6 This guideline included exenatide, given twice daily, which was the first GLP-1RA to be licensed in the UK (in 2007). Exenatide was positioned as a third-line ‘alternative’ add-on therapy to be considered after insulin, a thiazolidinedione or a dipeptidyl peptase-4 inhibitor and it was only sanctioned for use with metformin and a sulfonylurea. CG87 introduced the body mass index (BMI) cut-off of 35 Kg/m2 for GLP-1RAs, which was not based on data from clinical trials but was the BMI at which the average cost of a long-acting insulin analogue was the same as BD exenatide. NICE also introduced ‘stopping rules’ where exenatide should be withheld when a reduction of at least 1% (11mmol/mol) in HbA1c and weight loss of at least 3% initial body weight was not achieved after six months. Stopping rules have not been recommended for any other glucose-lowering class. The next NICE guidance for the management of T2DM (NG28) was published in 2015 and is best remembered for the furore created by the recommendation of repaglinide as firstline treatment for people intolerant of metformin.7,8 In the preceding six years, GLP-1RAs had been added to the glucoselowering algorithm by means of single technology appraisals (TAs). These individual assessments by NICE had a more binding legal status than their guidelines, in that a positive TA recommendation mandated that funding should be made available by clinical commissioning groups. Thus, liraglutide (TA203, 2010), exenatide extended-release (TA248, 2012) and lixisenatide (2013) were all sanctioned for use, although NICE limited the dose of liraglutide to a maximum of 1.2mg OD on the basis that this dose had the same acquisition cost as BD exenatide.9-11 The overall position of GLP-1RAs in the glucose-lowering algorithm was unchanged, however. They remained a third-line option for consideration after various triple oral combinations or insulin and were not even mentioned for people who could not tolerate metformin or for whom it was contra-indicated. The first CVOT of a glucose-lowering therapy to demonstrate superiority was the EMPA-REG OUTCOME study of empagliflozin, a sodium-glucose co-transporter 2 (SGLT2) inhibitor, and this trial was published three months before NG28 was launched in December 2015.12 NG28 did not take into account these positive data, but this was not thought to be important since NICE had committed to regular updates every two years and more CVOT data were in the pipeline. Indeed, in 2016 there were positive CVOTs for both liraglutide (LEADER) and onceweekly semaglutide (SUSTAIN 6).13,14 The positive superiority CVOT for dulaglutide (REWIND) was published in 2019 and there 1 Swansea University Medical School, Swansea, UK
求助全文
通过发布文献求助,成功后即可免费获取论文全文。 去求助
来源期刊
British Journal of Diabetes
British Journal of Diabetes ENDOCRINOLOGY & METABOLISM-
自引率
16.70%
发文量
15
期刊最新文献
qualitative study of the experiences of individuals who did not complete the NHS Low Calorie Diet Programme Pilot fresh start with high hopes: a qualitative evaluation of experiences of the Total Diet Replacement phase of the NHS Low Calorie Diet Programme pilot Supporting remission of type 2 diabetes in the real world Re:Mission study. Evaluating the NHS Low Calorie Diet pilot - an overview of service user data collection methods Participant experiences during the NHS Low Calorie Diet Programme pilot. Findings from an online survey
×
引用
GB/T 7714-2015
复制
MLA
复制
APA
复制
导出至
BibTeX EndNote RefMan NoteFirst NoteExpress
×
×
提示
您的信息不完整,为了账户安全,请先补充。
现在去补充
×
提示
您因"违规操作"
具体请查看互助需知
我知道了
×
提示
现在去查看 取消
×
提示
确定
0
微信
客服QQ
Book学术公众号 扫码关注我们
反馈
×
意见反馈
请填写您的意见或建议
请填写您的手机或邮箱
已复制链接
已复制链接
快去分享给好友吧!
我知道了
×
扫码分享
扫码分享
Book学术官方微信
Book学术文献互助
Book学术文献互助群
群 号:481959085
Book学术
文献互助 智能选刊 最新文献 互助须知 联系我们:info@booksci.cn
Book学术提供免费学术资源搜索服务,方便国内外学者检索中英文文献。致力于提供最便捷和优质的服务体验。
Copyright © 2023 Book学术 All rights reserved.
ghs 京公网安备 11010802042870号 京ICP备2023020795号-1