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痛风(gout)是由于血清尿酸盐水平升高引起单钠尿酸盐(monosodium urate,MSU)晶体沉积所致的一种炎性关节疾病。
嘌呤代谢紊乱和/或尿酸排泄减少所致的高尿酸血症(hyperuricemia,HUA)与疾病直接相关。
该病的临床特点主要包括:反复发作的急、慢性关节炎,痛风石形成,严重者可出现关节破坏、畸形及功能障碍。
研究证实,痛风与多种并发症密切相关,尤其是心血管系统疾病、肾功能不全和代谢综合征等。
因此,降尿酸治疗(urate-lowering therapy,ULT)对于各类并发症,尤其是慢性肾脏病(chronic kidney disease,CKD)方面的影响非常重要。
本文对近年来ULT在CKD方面的相关研究做一综述。
目前,可选用的降尿酸药物共有3大类:(1)抑制尿酸生成药〔黄嘌呤氧化酶抑制剂(xantine oxidase inhibitors,XOI)〕,如别嘌醇、非布司他;(2)促尿酸排泄药,如丙磺舒、苯溴马隆、雷西那德(lesinurad);(3)重组尿酸氧化酶(催化尿酸转化为水溶性和易排泄的尿囊素),如普瑞凯希(pegloticase)、拉布立酶(rasburicase)。
临床中常用的是前两类。
其中,别嘌醇、非布司他、苯溴马隆分别为两类药物中的代表,在实际临床工作中占有重要的治疗地位。
一、别嘌醇对CKD的作用效果别嘌醇是最为熟知的一种XOI,其代谢产物可竞争性占据钼蝶呤基团,抑制黄嘌呤氧化酶活性,从而减少尿酸的合成。
然而,别嘌醇分子中含有的嘌呤基团,可影响嘌呤代谢的其他通路,引起诸多不良反应,表现为别嘌醇超敏反应综合征(allopurinolhypersensitivitysyndrome,AHS),患者可出现发热、皮疹、红斑、脱屑、肾功能损伤、急性肝损伤等,病情严重可危及生命。
既往多项研究证实别嘌醇能够减缓CKD的疾病进程以及提高eGFR。
SIU等进行的一项前瞻性随机对照试验,纳入54例伴有HUA的CKD患者,使用别嘌醇剂量为100~300 mg/d,经过12 个月的治疗周期,发现血尿酸(SUA)水平显著降低,从(9.75±1.18)mg/dl〔(0.58±0.07)mmol/L〕降至(5.88±1.01)mg/dl〔(0.35±0.06)mmol/L〕(P<0.001);在血肌酐水平方面治疗组较安慰剂组有下降的趋势,尽管其差异无统计学意义;肾功能改善方面治疗组优于安慰剂组(P=0.015)。
Advances in Clinical Medicine 临床医学进展, 2021, 11(4), 1925-1928Published Online April 2021 in Hans. /journal/acmhttps:///10.12677/acm.2021.114277以重度低钾血症首诊的干燥综合征致肾小管酸中毒1例王慧1*,王珺1,李菁1,张赛2,孙慧31青岛大学附属医院急诊内科,山东青岛2青岛市市立医院急诊科,山东青岛3青岛大学附属医院康复医学科,山东青岛收稿日期:2021年3月22日;录用日期:2021年4月20日;发布日期:2021年4月27日摘要目的:目前干燥综合征致肾小管酸中毒引起的重度低钾血症病例较少,本文将结合病例对此类患者的诊断、治疗及预后进行分析、探讨。
方法:回顾性分析急诊就诊的1例重度低钾血症首诊的干燥综合征致肾小管酸中毒患者的临床表现、诊治思路、治疗结局,并进行相关文献复习。
结果:患者经过积极补钾及激素治疗后,血钾逐渐恢复正常,病情平稳。
结论:低钾血症患者的临床表现和病因复杂多样。
如临床上疑似该病,应尽早明确干燥综合征诊断,及早、充分有效地治疗,可明显改善患者的预后。
关键词干燥综合征,肾小管酸中毒,低钾血症Severe Hypokalaemia Due to RenalTubular Acidosis in a Patient withSjogren’s SyndromeHui Wang1*, Jun Wang1, Jing Li1, Sai Zhang2, Hui Sun31Department of Emergency Medicine, Affiliated Hospital of Qingdao University, Qingdao Shandong2Department of Emergency Medicine, Qingdao Municipal Hospital, Qingdao Shandong3Department of Rehabilitation Medicine, Affiliated Hospital of Qingdao University, Qingdao ShandongReceived: Mar. 22nd, 2021; accepted: Apr. 20th, 2021; published: Apr. 27th, 2021*通讯作者。
骨科SCI杂志1.【刊名】Osteoarthritis and cartilage / OARS, Osteoarthritis Research Society.【缩写刊名】Osteoarthritis Cartilage【起止年】1993-【出版周期】Eight a year, 2001-【出版商】W.B. Saunders For The Osteoarthritis Research Society【出版国】England【语种】English【ISSN】1063-4584【影响因子】2000年:02.080| 2001年:02.219| 2002年:02.763| 2003年:02.964| 2004年:3.572| 2005年:04.215| 2006年:04.017| 2007年:03.793|【中文简介】《骨关节炎与软骨》【分类】R68, 骨科学(运动系疾病、矫形外科学); R59, 全身性疾病【英文关键词】Orthopedics; Rheumatology【中文关键词】矫形外科学; 风湿病学2.【刊名】Journal of orthopaedic research : official publication of the Orthopaedic Research Soci ety.【缩写刊名】J Orthop Res【起止年】1983-【出版周期】Bimonthly, 1989-【出版商】Wiley,【出版国】United States【语种】English【ISSN】0736-0266【影响因子】2000年:02.233| 2001年:02.193| 2002年:01.846| 2003年:02.167| 2004年: | 2005年:0 2.916| 2006年:02.784| 2007年:02.437|【中文简介】《矫形研究杂志》刊载矫形外科领域各个方面的临床、实验和理论研究论文和简讯。
2020版:美国风湿病学会痛风治疗指南(全文)在2016 年EULAR[1 ]、2017 年英国风湿病协会(The British Society for Rheumatology , BSR ) [2]相继发表痛风治疗管理扌旨南之后,新型治疗痛风的相关证据不断出现。
2020年ACR发布了新的痛风管理扌旨南。
与之前的指南相比,该版指南中更新的观点颇多,共提出42条建议,其中包括16条强烈建议。
主要涉及起始降尿酸治疗(urate-lowering therapies , ULT )的指征,药物的滴定治疗方法,伴随预防发作的抗炎药物疗程等,于2020年6月在Arthritis & Rheumatism杂志正式刊出[3], 现介绍如下,希望能够指导痛风的实际诊疗。
1起始降尿酸药物治疗的指征以及证据等级见表①>1个痛风石、痛风造成的影像学损伤、频繁的痛风发作(>2次/年)。
②选择性建议,起始降尿酸药物治疗的指征是:既往曾经经历过1次以上的痛风发作,但发作频率<2次/年。
③对于首次痛风发作的患者,选择性建议起始降尿酸治疗;但选择性建议伴有慢性肾脏病(chronic kidney disease , CKD ) 期,血清尿酸>90 mg/L ( 540 p mol/L ),或者肾结石患者起始降尿酸治疗。
④对于无症状的高尿酸血症患者,选择性地建议不要开始降尿酸治疗。
ft I 的达WiiFAili-iHf i i MI i.$A•l»««m?zU J fffillSftit l 次卫乳疗叩aftnttn•l«iSH愕不IB打W«awnunM F无任代的础址IKI1L址型/LdUilWft!处中・L (w fWKfi.iifftt*.n annTffln便说不安)r 体. i仙»1他・山陕舒>表1药物降尿酸治疗的适应证随机对照试验显示,对于无症状的高尿酸血症患者,3年期间新发痛风仅为5% ;血清尿酸>90 mg/L (540 pmol/L )的无症状高尿酸血症患者,5年内仅20%出现痛风。
苯溴马隆的药物经济学评价徐茂锦上海长海医院200433随着我国生活水平的提高,饮食结构、节奏和生活方式的不断变化,痛风和高尿酸血症(Hyperuricemia,HUA)的患病率呈现逐年升高和患病率高和年轻化的趋势,特别是沿海和经济发达地区的患病率已经接近欧美发达国家的水平。
2005年意大利一般人群中HUA的患病率为8.54%,2009年上升至11.9%。
2007~2008年的美国国家健康和营养调查(the National Health and Nutrition Examination Survey,NHANES)显示,美国一般人群HUA的总体患病率为21.4% 。
1980年代初北京、上海、广州20周岁以上502例成年人HUA患病率仅为1.4%,1998年2037例上海居民调查HUA患病率为10.1%,2003年南京7888例调查患病率为13.3%,其中男性为17.6%,女性为9.3%。
2006年山东沿海20岁以上5003例常住居民的患病率为13.2%。
2011年广西城镇居民HUA患病率为19.78%,农村为12.31%。
2010年东南大学肾脏病研究所(代表中国慢性肾脏病流行病学调查协作组)采用人群调查的标准设计,多阶段分层随机抽样的方法并进行了严格的质量控制,以确保研究人群的代表性。
研究结果显示,中国成人高尿酸血症的患病率为8.4%(95%CI 8.0%~8.8%)。
据此估计,中国18岁以上人群中有将近9300万高尿酸血症患者。
(1-7)越来越多的流行病学、动物试验和临床研究显示,HUA是代谢综合征、2型糖尿病、高血压、心脑血管疾病、慢性肾病和痛风等疾病发生发展的独立危险因素,从患病人群多发性和广泛性与疾病危害的多系统多脏器而言,HUA将成为高血压、糖尿病和脑卒中之后的“第四高”,必须给予足够的重视。
痛风和高尿酸血症的治疗包括生活方式指导和药理控制两个方面。
一方面,生活方式指导包括健康饮食、限制烟酒、坚持运动和控制体重等。
2008年11月护理学报November,2008第15卷第11期Journal of Nursing(China)Vol.15No.11【药械护理】英夫利昔单抗治疗类风湿关节炎患者的护理董慧娟,何伟珍,叶志中,蔡旭(深圳市第四人民医院香蜜湖风湿病分院,广东深圳518040)[摘要]报道英夫利昔单抗治疗类风湿关节炎患者的护理体会。
在使用该药时严格低温保存,即用即取;药物现配现用,选择小号注射器的针头溶解药液,避免药液浪费;密切观察用药不良反应,如输液反应、呼吸道感染、结核感染、白细胞减少、肝功能异常等;因为该药的给药时间是按周排列的,不是传统的集中一个时间段每天用药的规律,不需要住院,因此加强对患者用药依从性的教育,以免延时用药,影响疗效。
熟悉药物特性,如药物的作用特点、疗效标准、安全性、剂量、疗程、联合用药、每次用药前的检查等,了解患者治疗进展,及时与患者沟通,了解患者的感受,密切观察患者用药疗效,为医生及时调整治疗方案提供依据。
21例类风湿关节炎患者在第0、2、6周及以后每隔8周静脉输注英夫利昔单抗3mg/kg,采用美国风湿病学会疗效评定标准,在用药后第1天、第2周、第6周、第14周ACR20改善分别为7例(33%)、9例(43%)、15例(72%)、18例(86%)。
[关键词]类风湿关节炎;英夫利昔单抗;护理[中图分类号]R473.5;R453[文献标识码]A[文章编号]1008-9969(2008)11-0071-03The Nursing of Rheumatoid Arthritis Patients Treated with InfliximabDONG Hui-juan,HE Wei-zhen,YE Zhi-zhong,CAI Xu(Xiangmihu Hospital for Rheumatism,Shenzhen Fourth People’s Hospital,Shenzhen518040,China)Abstract:The authors report their experience in nursing rheumatoid arthritis patients treated with Infliximab.They suggest the drug should be stored rigidly at lower temperature and be dissolved with small size of needle right at preparation;the adverse reactions should be closely observed like transfusion reactions,infection of respiratory tract,tuberculosis infection,reduction of leucocytes,and abnormities in hepatic function.The patients should be educated in compliance in case they delay use of the drug and the therapeutic effect is detained.The nurses should know well about the features of the drug like the drug action,standard for therapeutic effect, safety,dosage,treating course,drugs for combination,pre-administration examinations.They also keep pace of progress in treatment and communicate with patients,know their feelings and observe the therapeutic effect so that the doctors can modulate the therapy. 21rheumatoid arthritis patients in the study received venous transfusion of Infliximab at weeks0,2and6,and then at a dosage of 3mg/kg once every eight weeks.In line with the standard of ACR,the improvement rates of ACR20at day1,weeks2,6and14were 33%(7cases),43%(9cases),72%(15cases)and86%(18cases),respectively.Key words:rheumatoid arthritis;Infliximab;nursing类风湿关节炎(rheumatoid arthritis,RA)是以对称性多关节炎为主要表现的慢性炎症性疾病,可有关节外组织器官受累,可致残并使生活质量下降。
英国皇家学会(The Royal Society)一、简介英国皇家学会,全称“伦敦皇家自然知识促进学会”,成立于1660年,是为推动自然科学和应用科学发展而设立的,由英国资助科学发展的组织。
在1662年,由英国国王查理二世授予它第一个自治的学术团体,并于1663年、1669年领到皇家的各种特许证。
英女皇是学会的保护人。
英国皇家学会是世界上历史最长而又从未中断过的科学学会,也是英国最具名望的科学学术机构,在英国起着全国科学院的作用。
其成员在尖端科学方面饶有贡献。
该学会在多方面支持不少英国的年轻顶尖科学家、工程师及科技人才,对科学政策的制定起着一定作用,而且在科学事务问题上参与公众讨论。
英国皇家学会是一个独立的、享有慈善机构特权的组织,有1300名院士及外国成员。
学会的院士都是来自英国及外籍的著名科学家、工程师和科技人员。
二、历史英国皇家学会在1660年由著名科学罗伯特·波义尔、约翰·维尔金斯、克里斯托弗·雷恩等发起成立。
在16世纪40年代中期,一些哲学家开始聚会,讨论英国思想家弗兰西斯·培根的思想,这是皇家学会这家“无形学院”的始源。
皇家学会正式奠定基础的日期是1660年11月28日,当时12名哲学家在格雷舍姆学院,天文学教授克里斯托弗·雷恩一次讲课后,召集了一个会,正式提出成立一个促进物理-数学实验知识(promoting of physical-mathematical experimental learning)的学院。
约翰·威尔金斯被推选为主席,并起草了一个“被认为愿意并适合参加这个规划”的四十一个人的名单。
不久,罗伯特·莫雷带来了国王的口谕,同意成立“学院”,莫雷就被推为这个集会的会长。
学会每星期聚会,见证实验和进行讨论科学事务。
英国皇家学会(The Royal Society)这个名字在1661年首次见于文字,在1663年第二个英皇宪章中,学会被称为“推广自然知识的伦敦皇家学会”(The Royal Society of London forImproving Natural Knowledge)。
规范化治疗——风湿病领域永恒的话题栗占国近年来,“规范化治疗”的概念已在不少学科受到关注,并促进了临床治疗水平的提高。
风湿病学作为内科领域发展最快的学科之一,规范化治疗更是不容忽视。
临床上,因不正规用药导致病情迁延不愈、出现内脏损害甚至致残的风湿病患者绝不在少数。
最近又读到几篇国外关于“规范化”或“系统性”治疗类风湿关节炎( RA )和系统性红斑狼疮( SLE )等的文章,更促使我动笔将近几年国内外的临床研究以及自己的思考写成此文,供同道们参考。
1 规范化治疗是风湿病缓解的必由之路众所周知, RA 、 SLE 及干燥综合征( SS )等风湿病的发生和致病过程均与抗原的介导、自身抗体形成、致炎性因子的产生,以及细胞免疫异常等一系列免疫和炎症过程有关。
因此,临床上仅给予对症治疗、短期使用缓解病情抗风湿药( DMARDs )或免疫抑制剂很难控制这些疾病的发展。
大量的临床研究证明,规范化的系统用药是大多数风湿病患者病情缓解的关键。
比如,在 RA 的治疗中,尽早给予 DMARDs 已成为国际共识[ 1 , 2 ]。
而且, DMARDs 的给药是否及时与 RA 患者关节破坏的程度有直接关系[ 3 ]。
Panay i 等对 1975 — 2004 年 30 年来发表的 DMARDs 治疗 RA 的所有随机对照研究( RCT )进行了荟萃分析。
其结论十分明确,即对于多数 RA 患者应及早采用 DMARDs 联合治疗的方法[ 4 ]。
尽管有少数临床研究的设计存在不足,但联合治疗对患者显示出的明显优势得到了肯定。
不仅如此, Grigor 等在《柳叶刀》杂志发表的论文甚至提倡更为积极的方案治疗 RA [ 5 ]。
该文的研究者给 RA 患者以柳氮磺吡啶(40 mg · kg- 1· d- 1)及羟氯喹(6.5 mg · kg- 1· d- 1),并联用甲氨蝶呤(≤ 25 mg/ 周),必要时加用激素或改用来氟米特或金诺芬等三种药物联合治疗,研究者称之为“强化”( intensive )治疗方案。
Guideline (Executivesummary)British Society for Rheumatology and British Health Professionals in Rheumatology Guideline for the Management of GoutKelsey M.Jordan,J.Stewart Cameron 1,Michael Snaith 2,Weiya Zhang 3,Michael Doherty 3,Jonathan Seckl 4,Aroon Hingorani 5,Richard Jaques 6,George Nuki 7on behalf of the British Society for Rheumatology and British Health Professionals in Rheumatology Standards,Guidelines and Audit Working Group (SGAWG)K EYWORDS :Gout,Guidelines,Non-pharmacological treatment,Pharmacological treatment.Scope and purpose of the guidelineGout is a common disease both in primary care and hospital practice [1].Although drug therapy for gout has become a paradigm for the effective management and prevention of an acute and potentially chronic rheumatic disease,many of the recommendations for treat-ment are based on expert consensus rather than research evidence and audits of practice suggest that treatment is very variable.Evidence-based guidelines are needed at the present time: to provide a framework for improving standards of care.to assess the potential of new therapies such as Coxibs [2],urate oxidases [3]and novel xanthine oxidase inhibitors [4]currently in clinical development;to provide recommendations for alcohol consumption,diet and lifestyle modification in response to frequently asked questions by patients ()in the light of recent epidemiological studies linking gout with alcohol consumption [5],dietary protein intake [6]and features of the metabolic syndrome,which are assuming epidemic proportions [7];to define recommendations for treating secondary atypical gout,and small subgroups of patients with severe recurrent gout associated with renal insufficiency,organ transplantation,allopurinol hypersensitivity or primary purine overproduction.The aim has been to develop concise,patient-focussed,evidence-based recommendations for the management of gout for doctors and allied heath professionals in primary care and hospital practice in the UK,which will also provide a useful resource for patients.Recommendations for the diagnosis and investigation of gout [8]are not addressed.Guideline for the management of goutThis is a short summary of the guideline.The full guideline can be accessed at Rheumatology Online ().The management pathways proposed are summarized in the accompanying flowchart.The strength recommendations,based on levels of evidence,are graded A–C [9],and the recommenda-tions are divided into three sections:Management of acute gout(1)Affected joints should be rested (C)and analgesic,anti-inflammatory drug therapy commenced immediately,and continued for 1–2weeks (A).(2)Fast-acting oral NSAIDs at maximum doses are the drugs ofchoice when there are no contraindications (A).(3)In patients with increased risk of peptic ulcers,bleeds orperforations,co-prescription of gastro-protective agents should follow standard guidelines for the use of NSAIDs and Coxibs (A).(4)Colchicine can be an effective alternative but is slower towork than NSAIDs (A).In order to diminish the risks of adverse effects (especially diarrhoea)it should be used in doses of 500 g bd–qds (C).(5)Allopurinol should not be commenced during an acuteattack (B)but in patients already established on allopurinol,it should be continued and the acute attack should be treated conventionally (A).(6)Opiate analgesics can be used as adjuncts (C).(7)Intra-articular corticosteroids are highly effective in acutegouty monoarthritis (B)and i.a,oral,i.m or i.vRheumatology Department,Princess Royal Hospital,Brighton and Sussex University Hospitals Trust,1Renal Department,Guy’s,King’s &St Thomas’School of Medicine,London,2Rheumatology Department,Derbyshire Royal Infirmary and Derbyshire County Primary Care Trust,3Academic Rheumatology Unit,University of Nottingham,4The Queen’s Medical Research Institute and Endocrinology Unit,University of Edinburgh,5Centre for Clinical Pharmacology and Therapeutics,University College Hospital,London,6UK Gout Society,and 7The Queen’s Medical Research Institute and Rheumatic Diseases Unit,University of Edinburgh,UK.Submitted 13October 2006;revised version accepted 8February 2007.Correspondence to:Prof.George Nuki,Emeritus Professor of Rheumatology,University of Edinburgh Osteoarticular Research Group,The Queen’s Medical Research Institute,47Little France Crescent,Edinburgh EH164TJ,UK.E-mail:g.nuki@Rheumatology 2007;46:1372–1374doi:10.1093/rheumatology/kem056aAdvance Access publication 23May 20071372ßThe Author 2007.Published by Oxford University Press on behalf of the British Society for Rheumatology.All rights reserved.For Permissions,please email:journals.permissions@at Sichuan University on October 9, 2010 Downloaded fromGOUT: MANAGEMENT PATHWAYContinuing acute attacksTreat acute attack and when resolved go toSummary Guideline for the Management of Gout1373at Sichuan University on October 9, 2010 Downloaded fromcorticosteroids can be effective in patients unable to tolerate NSAIDs,and in patients refractory to other treatments (A).(8)If diuretc drugs are being used to treat hypertension,analternative antihypertensive agent should be considered,but in patients with heart failure,diuretic therapy should not be discontinued (C).Recommendations for diet,lifestyle modification and non-pharmacological modalities of therapy(1)In overweight patients dietary modification to achieve idealbody weight should be attempted (B),but ‘crash dieting’(B)and high protein/low carbohydrate (Atkins-type)diets (C)should be avoided.(2)Inclusion of skimmed milk and/or low fat yoghurt,soy beansand vegetable sources of protein and cherries,in the diet should be encouraged (B).(3)Intake of high purine foods and red meat should be restricted(B).Liver,kidneys,shellfish and yeast extracts should be avoided (B),and overall protein intake should be restricted (C).(4)Patients with gout and a history of urolithiasis should beencouraged to drink >2l of water daily (B)and avoid dehydration (C).Alkalinization of the urine with potassium citrate (60mEq/day)should be considered in recurrent stone formers (B).(5)Alcohol consumption should be restricted to <21units/week(men)and 14units/week (women)(B),and patients should be encouraged to have at least 3alcohol-free days per week (C).Beer,stout,port and similar fortified wines are best avoided (C).(6)Patients should be discouraged from undertaking trials ofherbal remedies without medical consultation (C).(7)Affected joints should be elevated and exposed in a coolenvironment (C).‘Bed cages’(C)and ice packs (B)can be effective adjuncts to therapy.(8)Trauma to joints (B)and intense physical exercise (B)shouldbe avoided but moderate physical exercise encouraged (B).Management of recurrent,intercritical and chronic gout(1)The plasma urate should be maintained below,300 mol/l (C).(2)In uncomplicated gout uric acid lowering drug therapyshould be started if a second attack,or further attacks occur within 1yr (B).(3)Uric acid lowering drug therapy should also be offered topatients with tophi (C),patients with renal insufficiency (B)patients with uric acid stones and gout (B)and to patients who need to continue treatment with diuretics (B).(4)Commencement of uric acid-lowering drug therapy should bedelayed until 1–2weeks after inflammation has settled (C).(5)Initial long-term treatment of recurrent uncomplicated goutnormally should be with allopurinol starting in a dose of 50–100mg/day and increasing by 50–100mg increments every few weeks,adjusted if necessary for renal function,until the therapeutic target (SUA <300 mol/l)is reached (maximum dose 900mg)(B).(6)Uricosuric agents can be used as second-line drugs inpatients who are under-excretors of uric acid and in thoseresistant to,or intolerant of,allopurinol (B).The preferred drugs are sulphinpyrazone (200–800mg/day)in patients with normal renal function or benzbromarone (50–200mg/day)in patients with mild/moderate renal insufficiency (B).(7)Colchicine 0.5mg bd should be co-prescribed followinginitiation of treatment with allopurinol or uricosuric drugs,and continued for up to 6months (A).In patients who cannot tolerate colchicine,an NSAID or Coxib can be substituted provided that there are no contraindications,but the duration of NSAID or Coxib cover should be limited to 6weeks (C).(8)Aspirin in low doses (75–150mg/day)has insignificant effectson the plasma urate,and should be used as required for cardiovascular prophylaxis (B).However,aspirin in analge-sic doses (600–2400mg/day)interferes with uric acid excre-tion and should be avoided (B).The full guideline also contains recommendations for the use of uricolytic agents and combined therapy with allopurinol and uricosuric drugs;as well as for the management of special groups of patients with chronic gout.The guideline has been developed as a National Guideline,acceptable for use throughout the NHS in the UK.If followed and implemented,these guidelines will provide an opportunity to improve the quality of care for patients with gout in both hospital and community settings.Recommendations for auditAssess the impact of the guideline on:(1)The frequency and duration of gout flares.(2)The achievement of target reduction in plasma urate levels.(3)Lifestyle modification (weight reduction,alcohol intake anddietary adjustment).(4)The assessment and treatment of co-morbid disorders(diabetes mellitus,hypertension,and cardiovascular risk factors).(5)The time to accurate diagnosis and treatment of gout inprimary and hospital care settings.(6)Documentation of all of the above.References1Mikuls TR,Farrar JT,Bilker WB,Fernandes S,Schumacher HR Jr,Saag KG.Gout epidemiology:results from the UK general practice research database,1990-1999.Ann Rheum Dis 2005;64:267–72.2Schumacher HR Jr,Boice JA,Daikh DI et al.Randomised double blind trial of etoricoxib and indometacin in treatment of acute gouty arthritis.Brit Med J 2002;324:1488–92.3Vogt B.Urate oxidase (rasburicase)for treatment of severe tophaceous gout.Nephrol Dial Transplant 2005;20:431–3.4Becker MA,Schumacher HR Jr,Wortmann RL et al.Febuxostat,a novel nonpurine selective inhibitor of xanthine oxidase:a twenty-eight-day,multicenter,phase II,randomized,double-blind,placebo-controlled,dose-response clinical trial examining safety and efficacy in patients with gout.Arthritis Rheum 2005;52:916–23.5Choi HK,Atkinson K,Karlson EW,Willett W,Curhan G.Alcohol intake and risk of incident gout in men:a prospective ncet 2004;363:1277–81.6Choi HK,Atkinson K,Karlson EW,Willett W,Curhan G.Purine-rich foods,dairy and protein intake,and the risk of gout in men.N Eng J Med 2004;350:1093–103.7Rigby NJ,Kumanyika S,James WP.Confronting the epidemic:the need for global solutions.J Public Health Policy 2004;25:418–34.8Zhang W,Doherty M,Pascual-Gomez E et al.EULAR evidence-based recommen-dations for gout.Part 1:Diagnosis.Ann Rheum Dis 2006;65:1301–11.9/college/ceeu/conciseGuidelineDevelopmentNotes.pdf1374K.M.Jordan et al .at Sichuan 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