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兰大二院下肢浅静脉炎专家

简介:

兰州大学第二医院(简称兰大二院)建于1928年,是集医疗、急救、教学、科研、预防、保健、康复、健康于一体的大型综合性三级甲等医院,“全国百姓放心示范医院”及“全国百姓放心百佳示范医院”。医院本部包括甘肃省儿童医院。除本部外,有西固医院一个分院。医院规模:医院本部占地155亩,总建筑面积约40.1万平方米,现有职工5600余人(含离退休人员)。医院开放床位3294张,2021全年门诊量213.97万人次,急诊量8.66万人次,住院人数11.86万人次,手术量6.63万台次,医院本部设有24个党政后勤职能处室、89个临床医技科室、1个直属机构、2个直属单位。兰州大学第二医院西固医院(兰州市西固区人民医院)是一所集医疗、预防、教学、科研于一体的综合性二级甲等医院,建筑面积44332平方米。新建门诊医技综合大楼建筑面积25967.14平方米,于2017年5月8日正式投入使用,医院医疗用房面积达到5万平方米,目前核定床位490张,实际开放床位550张。全院职工800人,医院现有38个专业科室。正高级职称10人,副高级60人,中级182人,助理级345人,初级139人。在岗人员中,硕士研究生17名,本科生462名。省、市医学会各专业委员会副主任委员1名,其他委员20名。兰大二院本部32名专家坐诊,有力提升了门诊服务能力和解决疑难杂症的能力。拥有2个兰州市临床重点建设专科(内分泌糖尿病科、中医科),4个甘肃省县级临床重点建设专科(妇产科、普外科、内分泌科、呼吸科)。3个区级质控中心(区护理质控中心、区合理用药质控中心、区院内感染质控中心);我院为了不断提高服务水平和能力,购置了飞利浦双板数字化DR;1.5T超导核磁共振;超声美国GE和飞利浦IU22彩超仪;奥林巴斯消化内镜;高清富士支气管镜;美国GE呼吸机。2020年6月放射能谱CT室开科,拥有顶尖美国GE先锋Revolution256排高端能谱CT;2020年7月建设PCR实验室(临床基因扩增实验室)验收成功,拥有顶尖ABI基因扩增仪。2013年被评为全国综合医院中医工作示范单位;2014年5月通过国际医疗机构评审委员会JCI认证,成为我省首家,也是唯一一家通过JCI评审的医疗机构;2015年8月获得省级文明单位称号。2015年8月在兰州大学第二医院和西固区委、区政府的友好协商、沟通下,加入兰大二院医疗集团,由兰大二院全面托管,成立兰州大学第二医院西固医院。2018年被省卫健委评为“全省优质医疗服务示范医院”;2018年获批成为国家心力衰竭医联体成员单位;2018年获得批准成立甘肃省助理全科医生培训基地。2019年获得“甘肃省健康促进医院”荣誉称号;2019年7月被中国妇幼保健协会授予“母婴友好医院”称号;2020年11月被国家卫生健康委脑卒中防治工程委员会授予“综合防治卒中中心”;2020年荣获国家级“节约型公共机构示范单位”称号;2020年获得西固区卫健局授予的区域性五大医学中心称号(影像中心、心电中心、病理中心、检验中心、消毒供应中心)。人才队伍:医院人才济济,享受国务院政府特殊津贴专家17人,卫生部突出贡献中青年专家3人,特聘专家、中国工程院院士1人,国家级人才计划1人,甘肃省拔尖人才2人、省级优秀专家9人,省级领军人才35人,获批陇原青年英才3人,兰大萃英学者获批10人,甘肃省卫生健康行业骨干人才9人,甘肃省卫生健康行业青年人才5人,省“555科技人才工程”人选17人,省“333科技人才工程”人选9人,省卫生系统领军人才21人。省级重点人才项目(省委组织部项目)获批8人、获评陇原青年创新团队6个(省委组织部项目)、陇青创新人才个人16人(省委组织部项目),兰大临床医学青年人才建设计划28人,陇原人才服务卡150人、甘肃省军民融合发展智库专家4人。学科建设:医院现拥有5个国家临床重点专科、6个国家临床医学研究中心分中心、2个甘肃省临床医学中心、29个省级医疗卫生重点学科、21个省级医疗卫生重点专业、1个甘肃高校省级重点学科、7个兰州大学临床医学研究型学科、1个院士专家工作站,下设3个院士工作基地。15个国家级培训基地、18个省级质量控制中心、34个甘肃省专科(技术)联盟、6个省级重点实验室、4个省级工程研究中心、13个省级临床医学研究中心、1个省级科技创新服务平台、5个省级国际科技合作基地、2个省级行业技术中心、1个萃英生物医学研究中心、12个院级重点实验室。获批五星高级卒中中心、甘肃省I级创伤中心、甘肃省危重孕产妇救治中心、甘肃省危重新生儿救治中心、甘肃省心理卫生中心、甘肃省听力障碍诊断中心、甘肃省眼科疾病干部保健中心、甘肃省儿童青少年健康指导中心等专科专病诊疗中心,通过中国胸痛中心、中国高血压中心、中国房颤中心认证,建成中国西部首家“内镜培训基地”以及西北地区首家直通梅奥国际会诊中心。教学状况:现有临床医学博士一级学科点和临床医学博士专业学位授权类型各1个,包含临床医学博士专业学位授权类型10个,临床医学一级学科博士包含6个学科方向。临床医学一级学科硕士点1个,包含14个学科方向;临床医学硕士专业学位授权类型1个,包含20个专业领域。具有临床医学、医学检验技术、医学影像学、麻醉学4个本科专业,形成了博士、硕士和学士的完整的人才培养体系。现有42个教研室,硕博士生导师179人(其中博士生导师56人),教授54人,副教授112人。2014年成立兰州大学第二医院住院医师规范化培训基地,是国家首批住院医师规范化培训基地之一,共拥有内科、儿科、急诊科、皮肤科、精神科、神经内科、全科、重症医学科、外科、外科(神经外科方向)、外科(胸心外科方向)、外科(泌尿外科方向)、外科(整形外科方向)、骨科、妇产科、眼科、耳鼻咽喉科、麻醉科、临床病理科、放射科、超声医学科、核医学科、口腔全科、口腔内科、口腔颌面外科、口腔修复科26个专业;2020年儿科专业基地获得全国重点专业基地;2021年急诊科专业基地获得全国重点专业基地。培训师资力量雄厚,培训设施、设备齐全,萃英临床技能教学中心占地3500余平方米,培训模拟设备种类齐全。自2015年2月开始,共计招生2596人,目前在培人员968人,累计考核合格并取得国家颁发的《住院医师规范化培训合格证》达1263人。科研成果:医院拥有6个省级重点实验室(甘肃省消化系肿瘤重点实验室、甘肃省骨关节疾病研究重点实验室、甘肃省泌尿系统疾病研究重点实验室、甘肃省血液病重点实验室、甘肃省医学影像重点实验室、甘肃省神经病学重点实验室);4个省级工程研究中心(甘肃省骨科3D打印工程研究中心、甘肃省消化内镜工程研究中心、甘肃省心脏康复工程研究中心、甘肃省智能超声医学工程研究中心);13个省级临床医学研究中心(甘肃省消化系统疾病临床医学研究中心、甘肃省骨科临床医学研究中心、甘肃省泌尿外科临床医学研究中心、甘肃省神经内科临床医学研究中心、甘肃省超声影像临床医学研究中心、甘肃省眼科临床医学研究中心、甘肃省急诊医学临床医学研究中心、甘肃省普通外科微创治疗临床医学研究中心、甘肃省血液病临床医学研究中心、甘肃省肾脏疾病临床医学研究中心、甘肃省耳鼻咽喉疾病临床医学研究中心、甘肃省风湿免疫疾病临床医学研究中心、甘肃省功能及分子影像临床医学研究中心);1个省级科技创新服务平台(甘肃省高原高发肿瘤生物样本库);5个省级国际科技合作基地(神经病学疾病精准诊疗甘肃省国际科技合作基地、脊柱疾患疼痛机制研究及治疗甘肃省国际科技合作基地、泌尿系统疾病转化医学研究与应用甘肃省国际科技合作基地、医学影像人工智能甘肃省国际科技合作基地、心血管病甘肃省国际科技合作基地);2个省级行业技术中心(甘肃省智能骨科行业技术中心、甘肃省介入超声装备应用行业技术中心);1个萃英生物医学研究中心;12个院级重点实验室(神经外科、耳鼻咽喉头颈外科、肝胆胰外科、放射影像、心血管疾病防控、消化疾病、肾病、药物基因组学、内分泌代谢、眼科、急诊医学和人源化动物模型重点实验室);近三年科研立项732项,获批科研经费21628.38万元,科研获奖35项(其中厅局级29项,省部级6项);科研论文2454篇(其中SCI906篇、CSCD612篇、统计源503篇、其他433篇),授权专利226项(其中发明专利14项、实用新型专利211项、外观设计专利1项),出版专著39部。专科联盟:2017年医院组建专科联盟,通过整合区域内优质医疗资源,健全专科医生人才培养体系,密切加强专科间学术交流与合作,有效加强专科深度建设和精准分级诊疗,提高基层医疗机构诊疗技术水平,提升解决专科重大疾病的救治能力。贯彻国家、省、市医联体建设工作,推动优质医疗资源下沉,进一步提升县级基层医疗机构的技术水平和服务能力,更好地为基层群众提供优质的医疗服务。目前,我院共计34(含护理)个学科与省各市、县区医院合作,获批省卫健委组织我院优势专科牵头的省级紧密型专科(技术)联盟34个,省内已签约成员单位分部14个地区,辐射一百余家医院。切实发挥专科优势和引领作用,带动区域专科辐射力及诊疗能力不断提升。医疗设备:医院拥有总价值达10.66亿余元的大型高精尖检测、诊断、治疗设备,包括Pet-CT,容积旋转调强(VMAT-ElektaSynergy™)医用直线加速器,飞利浦放疗专用大孔径4D-CT模拟定位机(BrillianceCTBigBore),铱-192高剂量率近距离治疗机,医科达-Monaco和飞利浦-Pinnacle3治疗计划系统,医科达肿瘤信息网络系统(Mosaiq),德国激光定位灯LAP(DORADO4)以及德国PTW三维水箱、瑞典ScandiDos公司实时剂量四维验证系统(Delta4)、二维矩阵验证系统,3.0T核磁共振、128排螺旋CT、宝石CT、移动CT、ECT、直线加速器、数字胃肠机、体外震波碎石机、3D腹腔镜、数字减影血管造影机、彩色多普勒超声检查仪、大型自动化生化仪、一体化手术间、流式细胞仪、基因测序仪、全自动质谱分析仪、全自动片剂摆药机、神经外科立体定向系统、椎间孔镜、超声内镜、数字乳腺机、准分子激光仪等国际一流医疗设备。雄厚的技术力量和先进的诊疗手段,促进医院诊疗水平。医院成绩:医院连续八年荣登艾力彼中国顶级医院百强排行榜,稳居甘肃首位。获评2022届顶级医院HIC60强,为甘肃省唯一上榜医疗机构;连续四年全国三级公立医院绩效考核结果位列A+等级,获评全国第82位。顺利通过甘肃省三级医院等级评审、国家电子病历系统应用水平五级评审。获评国家卫健委、国家中医药局“2020-2021年度公立医疗机构经济管理年活动优秀单位”;甘肃省总工会“2022年甘肃省五一劳动奖状”;新甘肃、每日甘肃网“2022新甘肃最具满意度三甲医院”。获得国家卫健委医政医管局、健康报社颁发的“2020年度改善医疗服务示范医院”荣誉称号。获得国家卫健委颁发的“2018-2020年改善医疗服务先进典型医院”“全国改善医疗服务宣传报道优秀医院”。获得国家卫健委医政医管局2020年度颁发的“对口帮扶-医院能力再提升”优秀案例优秀单位实践案例奖。获得“全国肺栓塞和深静脉血栓形成防治能力建设项目办公室血栓防治中心优秀单位”;获得兰州大学2020年新闻宣传工作先进单位。获得甘肃省精神文明建设指导委员会办公室、共青团甘肃省委、甘肃省广播电视总台失物招领公益联盟2020年度优秀合作单位。获得上海交通大学医院能源管理中心首届蓝源杯全国医院节能领跑示范单位。获得兰州市公安局交警支队城关大队2020年度“道路安全管理工作先进单位”。2019年医院荣获“2018年度脑卒中高危人群筛查和干预项目获脑防委先进集体”荣誉称号;“2018年度脑卒中高危人群筛查和干预项目先进集体”荣誉称号;获得由国家卫生健康委医政医管局、人民网共同颁发的“2019年度群众满意的医疗机构”;“2019年公立医院建设成就奖”。成为甘肃省首家通过“国家医疗健康信息互联互通标准化成熟度等级四级甲等”的医院,成为全国健康管理学科建设与科技创新中心旗舰单位、2018届三级医院健康管理(体检)机构100强,2021年度各省级质控中心试评估”得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科普文章

病症: 胃癌 恶性黑色素瘤

患者:李女士

年龄:70岁

罹患癌症,毫无疑问对每个人都是重大打击。而如果一位患者不幸同时罹患两种癌症,我们可以想象得出他的心情会是怎样的沉重。

但时至今日,癌症早已不再是什么“不治之症”,很多良好的治疗方法,可帮助患者迈过重重困境,预后得到极大提升。

不仅如此,在医疗全球化的今天,中国患者也能通过“海外二诊”服务,快速触达到国际权威专家资源,为自己的治疗保驾护航!

今天的案例主人公李女士,正是一位“海外二诊”的受益者。我们来一起看看她的故事。*为保护隐私,文中患者个人信息均已经脱敏处理。

70岁的李女士在去年年底,因脚底疼痛去医院看病,结果发现脚后跟有一个1厘米的黑色肿物。医生判断是冻疮,于是开了点外用药,李女士也就没有再放在心上。

大概4个月后,真正的噩梦降临:李女士通过影像检查,被诊断为胃癌,而且有了淋巴结转移。 她还出现了多次呕血,病情非常危急。很快,医生为她实施了全胃切除。令人意想不到的是,几天后通过检查,医生发现李女士后脚跟的肿物竟然也是癌症——恶性黑色素瘤。于是大概2个月后,医生又切除了她的足底肿瘤。 

为了降低复发风险,李女士开始了3个周期的化疗联合免疫治疗(替吉奥联合纳武单抗)。

虽然该做的都已做完,但对于李女士来说,恐惧感还远未被消除。因为癌症最令人恐惧的,是其具有“复发转移”的能力 。一旦癌症再次袭来,李女士不知道自己该如何应对。另外,两种癌症的治疗以及术后辅助药物治疗,也让李女士遭遇了一些副作用。比如腹泻、味觉障碍还有体重明显下降的问题。这些对于已经70岁的李女士来说,都很影响生活质量,所以迫切需要解决。

在本次的国际专家“海外二诊”服务中,李女士预约的是来自日本某知名综合性医院肿瘤中心的外科部长医生,他的专长领域既包括肿瘤外科,又包括各类癌症药物疗法、姑息治疗,是一位“内外兼修”的权威专家。在充分了解了李女士既往的病情和治疗经过后,医生很快通过远程会诊的方式,为患者详细解答了当前她的所有问题。

1、 未来如果转移或复发了该怎么办?  

医生:假如您未来不幸出现转移或复发,那么化疗是核心治疗手段。对于单发的孤立转移灶,可以选择手术、放疗来进行局部治疗。

具体化疗方案选择,我按使用的先后顺序列出了3类,当前面的方案失效后,可更换为后面的方案。

一类方案:化疗联合/不联合免疫方案  

  • CAPOX (卡培他滨+奥沙利铂)±O药(即免疫药物纳武单抗)
  • SOX (替吉奥+奥沙利铂)±O药
  • FOLFOX (5-FU+奥沙利铂)±O药

二类方案:化疗联合/不联合抗血管药物方案  

  • Taxane (紫杉醇/白蛋白结合型紫杉醇/多西紫杉醇)±雷莫芦单抗

三类方案:化疗方案  

  • 曲氟尿苷/盐酸替吡嘧啶
  • 伊立替康

  2、N K细胞疗法是否对我有帮助?副作用是否可控?   X医生:目前尚没有证据表明NK细胞疗法对癌症有效,因此不予推荐。

3、口服替吉奥会腹泻,是否需要调整方案?   II/III期胃癌患者术后采用辅助治疗方案,分别为:

  • 替吉奥口服 1 年(口服 4 周,停药 2 周,共 8 个疗程或口服 2 周,停药 1 周,共 16个疗程)
  • CAPOX (卡培他滨+奥沙利铂) 共半年(每 3 周一次,共 8 个疗程)
  • SOX (替吉奥+奥沙利铂) 共半年(每 3 周一次,共 8 个疗程)

这三种方案中,替吉奥方案和CAPOX方案等效,但SOX要优于替吉奥。另外,胃癌术后直接使用纳武单抗免疫治疗无意义。

替吉奥确实会出现腹泻等代表性不良反应,患者可以考虑对症治疗,比如调节肠道的药物、止泻药等缓解副作用。如果副作用太严重,那么可以考虑减少药物剂量。

替吉奥的标准用药剂量为120mg,但用量低于80mg无法达到预期效果。如果当前患者用药为100mg,那么为了降低副作用,可以减少剂量到80mg;但如果目前剂量已经是80mg,则无法进一步降低剂量,此时考虑更换方案为CAPOX方案替代。 如果不良反应严重到干扰日常生活,则患者可以选择停药,持续观察病情变化。

对于无淋巴结转移的II期B和II其C的患者,可选择使用1年帕博丽珠单抗免疫治疗。

4 、术后患者很瘦,味觉障碍,如何调理改善?   通常,手术后患者体重会减轻20%左右。这是患者消化吸收能力低下、促食欲的胃肠激素减少引起的。大约6个月到1年时间,患者可以恢复正常。

味觉障碍可能是抗癌药的副作用引起的,也可能是饮食减少导致缺乏锌等微量元素引起的。建议患者采用少食多餐的方式饮食,每天分5-6次吃饭。在日本,我们有时也会给患者用一些营养补充剂。

另外,也可以考虑采用中草药的对症治疗,改善症状,比如十全大补汤、六君子汤。 会诊结束后,李女士的心情得到了极大的平复。她对自己未来要走的路更清晰了,也对日本专家的细致指导和会诊的快速响应非常满意。

中国是消化道癌症发病数量较多的国家,根据国家癌症中心发布的《2022年中国恶性肿瘤疾病负担情况》数据,2022年我国胃癌新发病例约为35.87万例,死亡人数26.04万人。

总体来说,胃癌属于严重威胁我国国民生命健康的蕞常见癌症之一。胃癌如能在早、中期发现,还是有很大机会通过手术实现根治的,患者仍有一定机会得到临床治愈(术后5年不复发即为临床治愈)。

但在胃癌患者中,一部分人会因为【年龄较高】、伴有诸多【基础病】等问题,对手术存有疑虑,担心“下不来手术台”,甚至会放弃手术机会,选择吃药等姑息治疗。这样的选择真的正确吗?现如今的技术能否支持这类老年患者安全手术呢?接下来,我们一起看一个真实案例。

01七旬老人遭遇中期胃癌

一位七十多岁的“老胃病”项女士,因短时间体重骤降(8斤)前往就医。血液检测显示,她有一项指标异常升高。进一步检查发现,她的食道和胃连接的地方(贲门)以及胃的“外墙”(胃壁)都变得异常的厚,而且形状不均匀——这正是胃癌常见的表现。

医生随后通过胃镜检查和病例活检(取一小块组织观察上面的细胞),确诊了老人患有胃癌。由于还没有出现胃以外的远处其他器官的转移,也没有附近淋巴结转移,因此项女士的胃癌分期为中期。虽不是早期,但中期胃癌通常是可以手术的。为项女士提供诊疗的医生也表示,可以通过全胃切除手术实现根治。

但一来项女士已经七十多岁,二来她有20多年的糖尿病(手术伤口会更慢愈合、感染风险高、术后并发症风险高)、右肺还有一枚1.2厘米的肺结节。种种问题让老人和家人们都比较犹豫,担心扛不住治疗,最终“越治越糟”。在这样的背景下,项女士决定找一位足够权威的外科专家,来为自己进行全面评估,看看能不能兼顾好肿瘤根治以及手术的安全性。

不久后,项女士预约了来自日本癌研有明医院消化中心胃外科部长布部创也医生为自己提供指导。

02日本专家咨询内容分享

在充分了解了项女士的病情信息和全部资料后,布部创也医生给出了如下指导建议:首先,患者此前接受的是普通CT而非增强CT,胃镜也没有清晰展示食道上肿瘤具体侵犯的程度,因此很难得出精准的分期判断。

后面患者来癌研有明医院就医时,医疗团队会在治疗前为她做一套非常精细、全面的检查,此后就可以明确肿瘤情况了。届时如果发现患者的分期、肿瘤侵犯的范围确实和现在的结果相同,那么可以通过一个腹腔镜微创手术实现根治,损伤会非常小;如果届时发现肿瘤侵犯食道过多,则需要消化道联合食道外科共同进行胸腔镜手术治疗。

但无论是哪一种情况,患者都可以耐受手术,并且保留一部分胃。癌研有明医院是一家极为擅长肿瘤微创手术的知名癌症专科医院。在胃癌方面,2005年,医院开始导入腹腔镜,2019年又引入了达芬奇手术机器人,患者术后并发症更少了。如今,癌研有明医院98%的外科手术都采用微创。

受益于此,很多在别的医院需要胃全切的胃癌患者,到癌研有明后可以保留一部分胃,还能兼顾临床治愈。这对于术后患者的长期营养摄入和体重维持都很有帮助。布部创也医生所在科室的主要目标之一,正是在做到根治性切除的前提之下,将原本的胃全切术式变为次全胃切除术,尽可能为患者保留一些胃,让他们未来的生活质量得到提升。

那么项女士的糖尿病问题,会不会影响到手术呢?对此,布部创也医生认为完全不必担心,因为对于这类患者,癌研有明医院会进行详细的术前评估,并且有专业团队介入,从生活方式调整和专业治疗入手,帮助患者控制好血糖,让血糖水平达到符合手术的标准,从而降低术后愈合不良风险。

关于肺部的1.2厘米结节,布部医生认为可以暂不处理,无论它到底是良性还是恶性。因为这枚结节属于纯磨玻璃结节,即便是恶性,进展也非常缓慢,并不会快速出现转移扩散。而胃癌根治手术虽然会采用微创方式,但依然会给患者带来一定的负担,如果同时处理肺结节,会导致负担过重、患者难以承受。所以当前蕞好的处理办法,是先集中精力解决胃癌肿瘤,术后安排呼吸科专家为患者进行肺结节诊断,给出随访或手术或根治性放疗的建议。

03项女士术后,是否需要化疗来降低复发风险、争取更大治愈希望?

对此,布部创也医生表示,是否化疗现在还不能判断。因为术后患者能获得蕞精准的分期判断,有可能患者术前被认为是2期,但实际上术后成了1期(无需化疗);有时也可能患者术前是1期,但术后成了2-3期。假如是2-3期,则患者术后需要坚持1年的辅助化疗,大概可以降低10%的复发风险。

当地时间10月29日礼来宣布了Ⅲb期临床试验(TRAILBLAZER-ALZ 6)的积极结果,对于早期症状性阿尔茨海默病成人患者,用改良滴定方案接受donanemab治疗的患者在24周主要终点时,伴水肿/积液的淀粉样蛋白相关影像学异常(ARIA-E)有所减少。

donanemab这个新药在今年7月获批于美国,又在之后获日本厚生劳动省、英国药品和医疗产品监管局批准,用于轻度阿尔茨海默病、轻度认知功能障碍的治疗。donanemab在国内2023年取得突破性治疗药物认定,并纳入优先审评审批程序,目前还在审评审批过程中。

CDE官网截图

但在FDA说明书中有黑框警告,大意是应用该药时应注意淀粉样蛋白相关影像学异常(ARIA),表现为ARIA-E和ARIA伴含铁血黄素沉积(ARIA-H),通常发生在治疗早期,且无症状,很少发生严重和危及生命的事件。本次试验的积极结果和这个黑框警告相关。一起来看详情。

FDA说明书截图

给药方式有哪些改变?会不会影响效果?

TRAILBLAZER-ALZ 6是一项多中心随机双盲Ⅲb期研究,主要研究donanemab的不同给药方案对早期症状性AD患者ARIA-E和淀粉样蛋白清除率的影响,这里的早期AD指的是轻度认知障碍(MCI)和轻度痴呆疾病阶段。

给药方式和既往不同,既往标准给药方案是在前三次输注时接受2瓶(700mg)donanemab,然后再接受4瓶(1400mg);改良滴定方式是患者第一次输注1瓶(350mg),第二次输注2瓶(700mg),第三次输注3瓶(1050mg),此后每次输注4瓶(1400mg)。

研究的主要终点是第24周时患者出现ARIA-E占总参与者的比例,结果显示接受改良滴定方式的患者ARIA-E发生率为14%,而标准给药方案为24%,相对风险降低41%。载脂蛋白E(APOE)是已知的阿尔茨海默病遗传风险因素的携带者,在这些患者中,19%患者在改良滴定时患有ARIA-E,而标准给药方案中为57%,相对风险降低67%。

看到这里你或许也有疑问,虽然ARIA-E的发生风险降低了,但改良滴定方案会不会影响疗效?答案是不会。

与接受标准给药方案的患者相比,改良滴定患者淀粉样斑块和p-tau217减少。改良滴定的患者的淀粉样斑块水平较基线平均降低 67%,而标准给药组患者为69%。

参考来源

1.Modified Titration of Donanemab Demonstrated Reduction of ARIA-E in Early Symptomatic Alzheimer's Disease Patients in Phase Ⅲb study.

2.CED官网.

3.A Study of Different Donanemab (LY3002813) Dosing Regimens in Adults With Early Alzheimer's Disease (TRAILBLAZER-ALZ 6).

当地时间10月29日,阿西米尼(asciminib)获美国食品药品管理局(FDA)加速批准[1] ,用于慢性期新诊断的费城染色体阳性慢性粒细胞白血病(Ph+CML)成年患者。CML是一种骨髓和血细胞癌症,通常由费城染色体的异常染色体引起。在一线治疗中,约1/3的患者会出现下列问题:由于不良反应或者治疗无效而停止酪氨酸激酶抑制剂(TKI)治疗。

为了解决这一问题,需要开发新的药物,asciminib就是解决这一困境的新药。早在2022年8月,加拿大药物和卫生技术局(CADTH)建议[2] :“若满足条件,可通过公共药物计划报销asciminib用于治疗费城染色体阳性慢性粒细胞白血病。”

asciminib为何得到FDA的青睐?

本次获批基于一项III期多中心随机研究,研究目的是比较每日80mg的asciminib与TKI治疗的疗效。TKI治疗是接受伊马替尼、尼洛替尼、达沙替尼或博舒替尼任意一种治疗。

共有405名患者被随机分配(1:1)进两组治疗。主要疗效结局指标是48周时的主要分子反应(MMR)率。这个指标是慢性髓性白血病的关键指标,这个比例越高,说明该治疗在基因水平上对疾病的控制效果越好,能够更有效地抑制疾病相关基因的表达,进而有望更好地控制疾病的进展、改善患者的症状和预后。

研究结果显示,48周时MMR率方面,asciminib组中为68%(95% CI: 61, 74),TKI组为49%(95% CI: 42, 56),二者相差19%。细看具体的TKI,入组伊马替尼和其他TKI药物入组比例为1:1;asciminib组的MMR率为69%(95% CI: 59, 78),而伊马替尼组为40%(95% CI: 31, 50),相差近30%(95% CI: 17, 42)。

这个新药安全吗?每周需要打几次药?

根据FDA数据显示,在新诊断和既往接受过治疗的患者,应用新药最常见的不良反应(≥20%)是肌肉骨骼疼痛、皮疹、疲劳、上呼吸道感染、头痛、腹痛和腹泻。若只看新诊断的患者,最常见的实验室异常(≥40%)是淋巴细胞计数降低、白细胞计数降低、血小板计数降低、中性粒细胞计数降低等。

根据FDA已批准的asciminib说明书,用药期间还需要注意一下事项:

1.骨髓抑制 :用药期间可能因出现骨髓抑制,发生血小板减少症、中性粒细胞减少症和贫血。用药应在治疗的前3个月,需要每两周进行一次全血细胞计数,此后每月进行一次检测,从而判断患者有无骨髓抑制症状。根据严重程度,咨询医生是否需要停药。

2.胰腺毒性 :患者可能出现血清脂肪酶和淀粉酶无症状升高,每月需评估血清脂肪酶和淀粉酶水平,如果您有胰腺炎,则注意主动告知医生,需要进行频率更高的检测。

3.高血压风险 :可能出现3级或4级高血压风险,应注意检测血压。

4.超敏反应 :可能出现3级或4级超敏反应,包括皮疹、水肿和支气管痉挛。如果出现这些症状,需及时反馈医生,医生会根据超敏反应的体征和症状,开始适当的治疗。

5.心血管毒性 :如果您有心血管病史,需要告知医生;对于3级或更高级别的心血管毒性,医生会考虑暂停用药、减少剂量或永久停药。

6.胚胎/胎儿毒性 :若您在怀孕期间用药或在服用药物期间怀孕,可能对孩子有潜在风险。这个新药是口服药,需要根据不同的给药剂量(80mg或40mg)每天/或每两天用药。

近些年来,还有哪些白血病药物获批FDA?

根据FDA肿瘤学/血液系统恶性肿瘤批准通知,白血病相关新药整理如下表。

另外可以看出21年时asciminib已获批白血病治疗,但限定既往接受过两种或更多TKIs治疗,本次获批属于扩大适应证。

参考来源:

1.FDA grants accelerated approval to asciminib for newly diagnosed chronic myeloid leukemia. 2.Asciminib(Scemblix):CADTHReimbursementRecommendation:Indication:ForthetreatmentofadultpatientswithPhiladelphiachromosome-positivechronicmyeloidleukemia(Ph+CML)inchronicphase(CP)previouslytreatedwith2ormoretyrosinekinaseinhibitors.Ottawa(ON):CanadianAgencyforDrugsandTechnologiesinHealth;2022Aug.PMID:38713779. 3.AStudyofOralAsciminibVersusOtherTKIsinAdultPatientsWithNewlyDiagnosedPh+CML-CP. 4.Product information:SCEMBLIX-asciminibtablet,filmcoated.UpdatedAugust7,2024. 5.Oncology(Cancer)/HematologicMalignanciesApprovalNotifications.

以下内容来源于新英格兰医学杂志。

Presentation of Case

Dr. Carrie Chui (Neurology): A 79-year-old man was admitted to this hospital because of involuntary movements on the left side and transient unresponsiveness.
The patient had been in his usual state of health until 9 months before admission, when involuntary movements of the left shoulder and left side of the face developed. The movements were described by the patient as twitching, were not associated with a change in the level of consciousness, and resolved after 1 to 2 minutes. During the next 6 months, the patient had similar episodes approximately once per month, but the episodes increased in duration, lasting 5 to 6 minutes.
Three months before admission, the episodes of involuntary movements increased in frequency, and the patient was evaluated by his primary care physician. The physical examination was normal. Results of kidney-function tests were normal, as were blood levels of glucose and electrolytes, except for the sodium level, which was 129 mmol per liter (reference range, 135 to 145). There was a history of inappropriate antidiuretic hormone secretion, and the sodium level was similar to levels obtained during the past 4 years. Magnetic resonance imaging (MRI) of the head (Figure 1A), performed before and after the administration of intravenous contrast material, revealed a focus of enhancement in the right middle frontal gyrus that was thought to be a small vascular anomaly. Electroencephalography (EEG), performed with the patient in awake and drowsy states, revealed rare, brief, focal slowing in the left temporal lobe during drowsiness; no epileptiform abnormalities were present.
Figure 1
MRI of the Head and CT Angiogram of the Head and Neck.
Two months before admission, the patient was evaluated in the epilepsy clinic affiliated with this hospital. He reported that the episodes of involuntary movements had increased in both frequency and duration, occurring once or twice per day and lasting approximately 10 minutes. Episodes began with tingling and numbness in the left leg that prompted the patient to voluntarily stomp the left foot to relieve the uncomfortable sensation. Then, the patient had involuntary movements that he described as an uncontrollable invisible force moving the left leg and arm, with hyperextension of the arm backward and pronation of the wrist. There was associated numbness in the distal portions of the left third, fourth, and fifth fingers and involuntary movement of the left cheek. No prodromal symptoms occurred. The patient had awareness during the episodes, and after the episodes, he felt fatigued but had a normal level of consciousness, without confusion. The examination in the epilepsy clinic was normal. A diagnosis of seizure disorder was considered, and treatment with levetiracetam was started.
Three weeks before admission, the patient was again evaluated in the epilepsy clinic. He reported that the episodes of involuntary movements still occurred on a daily basis but had decreased in duration and involved only the left leg, without abnormal movements of the arm or face. Dizziness, headache, and weakness had developed and were attributed to the use of levetiracetam. The patient’s family had recorded a video of one of the episodes of involuntary movements. After reviewing the video, the patient’s neurologist thought that the episodes were less likely to be caused by seizures and more consistent with choreoathetoid movements. Cross-tapering of medications — with the simultaneous administration of levetiracetam in decreasing doses and clobazam in increasing doses — was initiated, and the patient was referred to the movement disorders clinic affiliated with this hospital.
On the morning of admission, an episode of involuntary movements of the left leg and left shoulder occurred and persisted for 1 hour. Several hours after the symptoms abated, the patient’s wife found the patient to be unresponsive; he was sitting in a chair. Emergency medical services were called, and when they arrived, the patient was responsive. The fingerstick blood glucose level was 180 mg per deciliter (10.0 mmol per liter) and the blood pressure 110/80 mm Hg. The patient was transported to the emergency department of this hospital for further evaluation.
In the emergency department, the patient reported dysuria and increased urinary frequency. The patient’s daughter noted that he had been more anxious during the past 3 years and occasionally had trouble with memory. Other medical history included Barrett’s esophagus, benign prostatic hypertrophy, chronic hepatitis B virus infection, eczema, gastroesophageal reflux disease, hypertension, nonischemic cardiomyopathy, and osteoporosis. There was no history of head trauma or extended loss of consciousness. Medications included aspirin, atorvastatin, doxazosin, finasteride, omeprazole, metoprolol, sacubitril, and valsartan. There were no known drug allergies. The patient was a lifelong nonsmoker and drank alcohol rarely; he did not use illicit drugs. His mother had had gastric cancer, and his sister had had esophageal cancer; there was no family history of seizures.
On examination, the temporal temperature was 36.8°C, the blood pressure 152/97 mm Hg, the pulse 65 beats per minute, the respiratory rate 16 breaths per minute, and the oxygen saturation 96% while the patient was breathing ambient air. The body-mass index (the weight in kilograms divided by the square of the height in meters) was 21.7. The blood pressure decreased to 130/63 mm Hg with standing. The patient was alert and interactive. The lower jaw was held to the left, but the nasolabial folds and smile were symmetric with activation. There were nonrhythmic, nonstereotyped, writhing movements of the left arm. Tone was normal, and strength was assessed as 5 out of 5 in the arms and legs. Results of liver-function and kidney-function tests were normal, as were blood levels of glucose and electrolytes, except for the sodium level, which was 125 mmol per liter. The lactate level was 2.1 mmol per liter (19 mg per deciliter; reference range, 0.5 to 2.0 mmol per liter [5 to 18 mg per deciliter]). The urinalysis was normal. Intravenous fluids were administered. Imaging studies were obtained.
Dr. Rajiv Gupta: Computed tomographic (CT) angiography of the head and neck (Figure 1B) revealed extensively calcified plaque with severe stenosis of the distal right common carotid artery (CCA), extending into the proximal right internal carotid artery (ICA), as well as stenosis of the right and left paraclinoid ICAs and the left vertebral artery at its origin. There was no vascular abnormality on the CT angiogram that corresponded to the abnormality in the right middle frontal gyrus seen on the previous MRI.
Dr. Chui: The patient was admitted to the hospital. On the second hospital day, the sodium level had increased to 130 mmol per liter, and the lactate level was normal. Additional imaging studies were obtained.
Dr. Gupta: MRI of the head showed no evidence of acute infarction. The focus of enhancement in the right frontal lobe that had been noted previously was not seen on the current MRI.
Dr. Chui: Blood levels of thyrotropin, cobalamin, and glycated hemoglobin and results of coagulation tests were normal. Screening tests for Lyme disease, tuberculosis, and syphilis were negative, as were tests for antibodies to cardiolipin and β2-glycoprotein. A test for antinuclear antibodies was positive, at a titer of 1:160 in a homogeneous pattern. During a physical therapy session, the patient had abnormal movements of the left leg, left arm, and left side of the face. The abnormal movements diminished when the patient used distraction techniques, such as thigh tapping, finger snapping, and walking while holding a glass of water.
The transient unresponsiveness that led to the patient’s admission was attributed to a combination of sedation from clobazam and hypovolemia. Treatment with clobazam was stopped, and hydration was encouraged. A diagnosis of functional neurologic disorder was considered; outpatient physical therapy with continued use of distraction techniques was recommended. The patient was discharged home on the third hospital day.
Episodes of involuntary movements continued to occur on a daily basis at home. Two weeks after discharge, when the patient was doing exercises while sitting in a chair and having a conversation with his wife, he suddenly stopped talking. She found him slumped in the chair with his eyes closed, no longer exercising. When she asked him questions, he repeatedly said “yes.” Emergency medical services were called, and when they arrived, the patient was alert, diaphoretic, and nonverbal. He had a facial droop on the left side and a right gaze preference. The fingerstick blood glucose level was 130 mg per deciliter (7.2 mmol per liter) and the blood pressure 120/60 mm Hg. The patient was transported to the emergency department of this hospital for further evaluation.
In the emergency department, the temporal temperature was 36.6°C, the blood pressure 143/63 mm Hg, the pulse 66 beats per minute, the respiratory rate 18 breaths per minute, and the oxygen saturation 98% while the patient was breathing ambient air. He was alert and interactive. There was a facial droop on the left side. There was no effort against gravity in the left arm. The patient was able to lift the left leg off the bed for 1 to 2 seconds. He had a right gaze deviation that could not be overcome and mild dysarthria. The remainder of the examination was normal. A diagnosis of stroke was considered, and emergency CT angiography was performed.
Dr. Gupta: CT angiography showed no evidence of acute territorial infarction and no changes in cerebrovascular disease.
Dr. Chui: On repeat physical examination performed after CT angiography, the gaze deviation and dysarthria had resolved, and strength was normal. Mild facial paralysis was present.
A diagnosis was made.

Differential Diagnosis

Dr. Albert Y. Hung: This 79-year-old man initially presented with involuntary movements of the left shoulder and face without associated loss of consciousness. Diagnosis of an unusual movement disorder, especially one that is present episodically, can be challenging. Videos brought in by the patient can be very useful. 1 Most movement disorders result from abnormal functioning of extrapyramidal circuits involving the basal ganglia, rather than a specific neuroanatomical lesion, and the first step toward diagnosis is to identify the type of abnormal movements. 2
Four salient aspects of this patient’s involuntary movements can help in characterizing the movement disorder before generating a differential diagnosis. First, the movements were paroxysmal, lasting for short periods of time with resolution between episodes. Second, the movements were nonstereotyped, appearing randomly and variably. Third, the movements were restricted to the left side of his body throughout the course, localizing the disease process to the right cerebral hemisphere. Finally, the symptoms were progressive, increasing in both duration and frequency.

Movement Disorders

This patient had abnormal involuntary movements, symptoms indicative of a hyperkinetic movement disorder. Tremor, the most common hyperkinetic disorder, is unlikely because the patient did not have rhythmic movements. Dystonia is also unlikely, because he did not have sustained muscle contractions that were causing twisting or abnormal postures of the legs, arms, head, neck, or face. Although the patient initially described the movements as twitching, his later descriptions are not suggestive of myoclonus or tics, which manifest as sudden, rapid, recurrent movements.
This patient’s neurologist described the involuntary movements as “choreoathetoid” after reviewing a video of an episode. Chorea, athetosis, and ballism make up a spectrum of involuntary movements that often occur in combination. Chorea refers to involuntary movements that are “dancelike” — irregular, random, unintended, and flowing from one body part to another. When these movements are slow and writhing (with a lower amplitude) and involve the distal limbs, the term athetosis is used. The presence of both chorea and athetosis in the same patient is referred to as choreoathetosis. When the movements are fast and flinging (with a higher amplitude) and involve the proximal limbs, the term ballism is used. Although the description of this patient’s movements was not clearly suggestive of ballism, hemichorea and hemiballismus often occur together.
The term dyskinesia can refer to any abnormal movements and is often used to describe hyperkinetic disorders that are induced by specific drugs, such as tardive dyskinesia induced by dopamine antagonists or dyskinesia induced by levodopa in patients with Parkinson’s disease. Often, dyskinesia manifests as chorea or choreoathetoid movements, but chorea and dyskinesia are not synonymous. This patient appears to have involuntary dyskinesia with choreoathetosis as the primary phenomenology. Before constructing a differential diagnosis for dyskinesia in this patient, I will consider two conditions that mimic dyskinesia: seizures and functional movement disorder.

Seizures

Various movement disorders may be mistaken for seizures, although these movement disorders are not associated with EEG abnormalities during the episode. Patients with some forms of epilepsy may present with abnormal movements without other features that are typically associated with seizures, such as aura, change in responsiveness, incontinence, or a postictal state. 3,4 Seizures were initially suspected in this patient, and he was referred to the epilepsy clinic. Recurrent focal seizures were probably suspected because of the transient nature of the episodes. Initial MRI had shown a small abnormality in the right middle frontal gyrus, but this finding was not seen on follow-up imaging, which makes it unlikely to be related to the overall presentation. Baseline EEG had shown only brief left temporal slowing, without epileptiform abnormalities. The EEG was an interictal study, so the findings do not rule out seizures. However, the slowing was ipsilateral to the abnormal movements, so it is unlikely to be related to the episodes. In addition, the patient’s involuntary movements were nonstereotyped and nonrhythmic, which makes his presentation unlikely to be due to a seizure disorder.

Functional Movement Disorder

Because this patient’s movements diminished with the use of distraction techniques, a diagnosis of functional movement disorder was considered. Most cases of functional movement disorder begin abruptly after a trigger, such as a mild physical injury or illness; a psychological stressor can be present but is not required for diagnosis. Symptoms are typically most severe around the time of onset and may wax and wane over time. Although distractibility is a finding associated with functional disorders, abnormal movements that occur with nonfunctional syndromes can sometimes be suppressed by action or incorporated into voluntary movements in a manner that may appear distractible. Several clinical features in this patient make a diagnosis of functional disorder unlikely. Functional movement disorder is more common in women than in men, and the average age at onset is 40 years. 5 In addition, tremor is the most common clinical phenotype seen in patients with functional movement disorder; chorea or choreoathetosis, which was seen in this patient, is very unusual in patients with functional movement disorder. Overall, functional movement disorder is unlikely to explain this patient’s presentation.

Dyskinesia

Primary paroxysmal dyskinesia refers to a group of heterogeneous syndromes characterized by recurrent involuntary movements that occur episodically and abruptly, without loss of consciousness. 6 These disorders usually begin in childhood or young adulthood. Both the age of this patient and the described phenomenology make a diagnosis of primary paroxysmal dyskinesia unlikely.
The differential diagnosis in this case is therefore focused on causes of secondary dyskinesia, of which there are many. 7 MRI ruled out the presence of a mass lesion suggestive of cancer. The patient had no history of acute illness suggestive of a viral or other infectious encephalitis, and there was no history of trauma or exposure to drugs or other toxins. Although his daughter mentioned trouble with memory, there was no compelling history suggestive of a neurodegenerative disease.
A common metabolic cause of secondary dyskinesia is diabetic striatopathy, a syndrome involving the acute-to-subacute onset of chorea and ballism in the context of hyperglycemia. 8 This syndrome can occur as the initial manifestation of type 2 diabetes mellitus or as a complication of poorly controlled diabetes. Diabetic striatopathy is more likely to develop in women than in men, and the average age at onset is 70 years. Most patients present with hemichorea and hemiballismus, rather than bilateral symptoms. CT shows hyperdensity, and T1-weighted MRI shows hyperintensity, in the contralateral basal ganglia. However, this patient had no history of diabetes and had a normal blood glycated hemoglobin level, features that rule out a diagnosis of diabetic striatopathy.
Choreiform movements can also be a manifestation of autoimmune conditions. 9 This patient’s initial presentation with unilateral shoulder and face movements would have suggested the possibility of faciobrachial dystonic seizures associated with anti–leucine-rich, glioma-inactivated 1 (anti-LGI1) encephalitis. 10 This condition is often associated with hyponatremia, which was present in this patient. However, as the case evolved, leg involvement and sensory changes developed that would be atypical for anti-LGI1 encephalitis.
One key clue in this case is that the patient did not have an isolated movement disorder. In addition to motor symptoms, he had a variety of sensory symptoms involving both the left arm and the left leg. His first hospital admission was precipitated by an episode of unresponsiveness. The clinical event that led to his second presentation to the emergency department was distinctly different: an acute onset of speech difficulty accompanied by left hemiparesis and right gaze deviation that was worrisome for an acute right middle cerebral artery (MCA) syndrome. The symptoms resolved without intervention, which indicates that he may have had an acute transient ischemic attack (TIA). The most relevant imaging finding was severe cerebrovascular disease, including severe stenosis of the distal right CCA and proximal right ICA. Could this patient’s movement disorder be explained by a vascular lesion?

Limb-Shaking TIAs

Limb-shaking TIAs were first described by C. Miller Fisher in 1962. 11 In most case reports, these episodes are associated with high-grade stenosis of the ICA, which was seen in this patient. 12,13 The mechanism is thought to be cerebral hypoperfusion, and changes in posture or head position that decrease cerebral blood flow can precipitate these episodes. In this patient, the first episode of unresponsiveness that led to hospital admission occurred when he was sitting. He then had an acute episode involving right gaze preference that was provoked by exercise and was very suggestive of a TIA in the right MCA territory. These findings are highly suggestive of a diagnosis of limb-shaking TIAs, and I would refer this patient for emergency carotid endarterectomy.

Clinical Impression and Initial Management

Dr. Scott B. Silverman: When I evaluated this patient, his transient right gaze preference and left hemiparesis were consistent with a right MCA syndrome due to a TIA from symptomatic severe stenosis of the right ICA. The mechanism of this event was either artery-to-artery embolism or hypoperfusion. His previous, recurrent episodes of transient choreoathetosis on the left side that had occurred mainly while he was sitting, standing, or exercising were consistent with limb-shaking TIAs from hypoperfusion or low flow.
The pathogenesis of a low-flow state related to severe carotid stenosis resulting in limb-shaking TIAs is described in a small case series. 14 In six out of eight patients, the transient, stereotyped, involuntary movements were eliminated with carotid artery revascularization. Positional cerebral ischemia in patients without orthostatic hypotension has been described. 15
Treatment with atorvastatin was continued, the dose of aspirin was increased to 325 mg per day, and an intravenous heparin infusion was started. The strategy of permissive hypertension was used, with high blood pressure allowed to a maximum systolic blood pressure of 180 mm Hg. The patient was admitted to the stroke service, and carotid artery duplex ultrasonography was performed.
Dr. Gupta: Doppler ultrasonography of the carotid arteries (Figure 2) revealed markedly elevated Doppler flow velocities within the proximal right ICA. There was a parvus et tardus waveform in the distal right ICA, a finding indicative of low flow related to the more proximal high-grade stenosis. The Doppler waveform contours had poststenotic turbulence.
Figure 2
Doppler Ultrasound Image.
Dr. Silverman: The vascular surgery service was consulted, and the patient underwent right carotid endarterectomy.

Clinical Diagnosis

Limb-shaking transient ischemic attacks.

Dr. Albert Y. Hung’s Diagnosis

Limb-shaking transient ischemic attacks due to severe carotid stenosis, with secondary paroxysmal dyskinesia.

Pathological Discussion

Dr. Caroline F. Hilburn: The endarterectomy specimen included the carotid bifurcation and was notable for firm arterial walls, a finding consistent with calcification. On gross examination (Figure 3A), a large plaque was centered at the carotid bifurcation and protruded into the lumen, resulting in a maximal luminal stenosis of 80%. The plaque had an irregular and focally friable surface. On microscopic examination (Figure 3B), the plaque was characterized by extensive calcification. Some regions of the plaque had a smooth, healed fibrous cap, whereas other regions had an irregular surface suggestive of ulceration, which indicated potential sites of plaque rupture. Multiple smaller calcified plaques were present, affecting both branches of the artery.
Figure 3
Endarterectomy Specimen.

Pathological Diagnosis

Complex atherosclerotic plaque with portions of attached media.

Additional Management

Dr. Silverman: After the procedure, the patient had an uneventful recovery and was discharged home on the fifth hospital day. He was seen 1 month after discharge in the stroke prevention clinic. There had been no further episodes of involuntary movements or choreoathetosis and no stroke or TIA. The patient continues to take aspirin, atorvastatin, and antihypertensive medications.

Final Diagnosis

Limb-shaking transient ischemic attacks.

以下内容来源于新英格兰医学杂志。

Presentation of Case

Dr. Christine M. Parsons (Medicine): A 75-year-old woman was evaluated at this hospital because of arthritis, abdominal pain, edema, malaise, and fever.

Three weeks before the current admission, the patient noticed waxing and waning “throbbing” pain in the right upper abdomen, which she rated at 9 (on a scale of 0 to 10, with 10 indicating the most severe pain) at its maximal intensity. The pain was associated with nausea and fever with a temperature of up to 39.0°C. Pain worsened after food consumption and was relieved with acetaminophen. During the 3 weeks before the current admission, edema developed in both legs; it had started at the ankles and gradually progressed upward to the hips. When the edema began to affect her ambulation, she presented to the emergency department of this hospital.

A review of systems that was obtained from the patient and her family was notable for intermittent fever, abdominal bloating, anorexia, and fatigue that had progressed during the previous 3 weeks. The patient reported new orthopnea and nonproductive cough. Approximately 4 weeks earlier, she had had diarrhea for several days. During the 6 weeks before the current admission, the patient had lost 9 kg unintentionally; she also had had pain in the wrists and hands, 3 days of burning and dryness of the eyes, and diffuse myalgias. She had not had night sweats, dry mouth, jaw claudication, vision changes, urinary symptoms, or oral, nasal, or genital ulcers.

The patient’s medical history was notable for multiple myeloma (for which treatment with thalidomide and melphalan had been initiated 2 years earlier and was stopped approximately 1 year before the current admission); hypothyroidism; chikungunya virus infection (diagnosed 7 years earlier); seropositive erosive rheumatoid arthritis affecting the hands, wrists, elbows, and shoulders (diagnosed 3 years earlier); vitiligo; and osteoarthritis of the right hip, for which she had undergone arthroplasty. Evidence of gastritis was reportedly seen on endoscopy that had been performed 6 months earlier. Medications included daily treatment with levothyroxine and acetaminophen and pipazethate hydrochloride as needed for cough. The patient consumed chamomile and horsetail herbal teas. She had no known allergies to medications, but she had been advised not to take nonsteroidal antiinflammatory drugs after her diagnosis of multiple myeloma.

Approximately 5 months before the current admission, the patient had emigrated from Central America. She lived with her daughter and grandchildren in an urban area of New England. She had previously worked in health care. She had no history of alcohol, tobacco, or other substance use. There was no family history of cancer or autoimmune, renal, gastrointestinal, pulmonary, or cardiac disease.

On examination, the temporal temperature was 37.1°C, the heart rate 106 beats per minute, the blood pressure 152/67 mm Hg, and the oxygen saturation 100% while the patient was breathing ambient air. She had a frail appearance and bitemporal cachexia. The weight was 41 kg and the body-mass index (the weight in kilograms divided by the square of the height in meters) 15.2. Her dentition was poor; most of the teeth were missing, caries were present in the remaining teeth, and the mucous membranes were dry. She had abdominal tenderness on the right side and mild abdominal distention, without organomegaly or guarding. Bilateral axillary lymphadenopathy was palpable. Infrequent inspiratory wheezing was noted.

The patient had swan-neck deformity, boutonnière deformity, ulnar deviation, and distal hyperextensibility of the thumbs (Fig. 1). Subcutaneous nodules were observed on the proximal interphalangeal joints of the second and third fingers of the right hand and on the proximal interphalangeal joint of the fourth finger of the left hand. Synovial thickening of the metacarpophalangeal joints of the second fingers was noted. There was mild swelling and tenderness of the wrists. She had pain with flexion of the shoulders and right hip, and there was subtle swelling of the shoulders and right knee. Pitting edema (3+) and vitiligo were noted on the legs. No sclerodactyly, digital pitting, telangiectasias, appreciable calcinosis, nodules, nail changes (including pitting), or tophi were present. The remainder of the examination was normal.

Figure 1

Photograph of the Hands.

The blood levels of glucose, alanine aminotransferase, aspartate aminotransferase, bilirubin, globulin, lactate, lipase, magnesium, and phosphorus were normal, as were the prothrombin time and international normalized ratio; other laboratory test results are shown in Table 1. Urinalysis showed 3+ protein and 3+ blood, and microscopic examination of the sediment revealed 5 to 10 red cells per high-power field and granular casts. Urine and blood were obtained for culture. An electrocardiogram met (at a borderline level) the voltage criteria for left ventricular hypertrophy.

Table 1
Laboratory Data.

Dr. Rene Balza Romero: Computed tomography (CT) of the chest, abdomen, and pelvis, performed after the intravenous administration of contrast material, revealed scattered subcentimeter pulmonary nodules (including clusters in the right middle lobe and patchy and ground-glass opacities in the left upper lobe), trace pleural effusion in the left lung, coronary and valvular calcifications, and trace pericardial effusion, ascites, and anasarca. The scans also showed slight enlargement of the axillary lymph nodes (up to 11 mm in the short axis) bilaterally and a chronic-appearing compression fracture involving the T12 vertebral body.

Dr. Parsons: Morphine and lactated Ringer’s solution were administered intravenously. On the second day in the emergency department (also referred to as hospital day 2), the blood levels of haptoglobin, folate, and vitamin B12 were normal; other laboratory test results are shown in Table 1. A rapid antigen test for malaria was positive. Wright–Giemsa staining of thick and thin peripheral-blood smears was negative for parasites; the smears also showed Döhle bodies and basophilic stippling. Antigliadin antibodies and anti–tissue transglutaminase antibodies were not detected. Tests for hepatitis A IgG and hepatitis C antibodies were positive. Tests for hepatitis B core and surface antibodies were negative. A test for human immunodeficiency virus type 1 (HIV-1) and type 2 (HIV-2) was negative.

Findings on abdominal ultrasound imaging performed on the second day (Fig. 2A and 2B) were notable for a small volume of ascites and kidneys with echogenic parenchyma. Ultrasonography of the legs showed no deep venous thrombosis. An echocardiogram showed normal ventricular size and function, aortic sclerosis with mild aortic insufficiency, moderate tricuspid regurgitation, a right ventricular systolic pressure of 39 mm Hg, and a small circumferential pericardial effusion. Intravenous hydromorphone was administered, and the patient was admitted to the hospital.

Figure 2

Imaging Studies of the Abdomen and Hands.

On the third day (also referred to as hospital day 3), nucleic acid testing for cytomegalovirus, Epstein–Barr virus, and hepatitis C virus was negative, and a stool antigen test for Helicobacter pylori was negative. An interferon-γ release assay for Mycobacterium tuberculosis was also negative. Oral acetaminophen and ivermectin and intravenous hydromorphone and furosemide were administered.

Dr. Balza Romero: Radiographs of the hands (Fig. 2C through 2F) showed joint-space narrowing of both radiocarpal joints and proximal interphalangeal erosions involving both hands. Radiographs of the shoulders showed arthritis of the glenohumeral joint and alignment suggestive of a tear of the right rotator cuff. A radiograph of the pelvis showed diffuse joint-space narrowing of the left hip, without osteophytosis, and an intact right hip prosthesis.

Dr. Parsons: Diagnostic tests were performed, and management decisions were made.

Differential Diagnosis

Dr. Beth L. Jonas: This patient is a 75-year-old woman who recently emigrated from Central America. She presented to this hospital with a multisystem disease involving the respiratory, gastrointestinal, renal, and musculoskeletal systems. Her medical history is notable for seropositive erosive rheumatoid arthritis and multiple myeloma, which had been treated with melphalan and thalidomide. Relevant clinical features on presentation include unintended weight loss and cachexia, axillary lymphadenopathy, serositis, cytopenia in two cell lines, hypocomplementemia, and elevated serum free kappa and lambda light-chain levels (with a normal free light-chain ratio) with no monoclonal spike. The white-cell count was elevated, but she had no eosinophilia. CT images of the chest showed scattered subcentimeter pulmonary nodules. With respect to the patient’s anemia, no schistocytes were present, the haptoglobin level was normal, and the iron studies were unremarkable. These findings, in combination with the elevated ferritin level, indicate anemia of chronic inflammation. The renal findings are most salient in the context of the patient’s hypertension, anasarca, elevated cystatin C level, active urinary sediment with proteinuria in the nephrotic range, and small, echogenic kidneys on ultrasonography.
In constructing a differential diagnosis, I will consider medication use, cancer, infectious disease, and autoimmune disease. Medications can be eliminated as the cause of this patient’s illness, since she was taking only levothyroxine, acetaminophen, and the antitussive agent pipazethate.

Cancer

The patient has a history of multiple myeloma, which may manifest with a multisystem disease involving the kidneys, but serum protein electrophoresis showed no monoclonal protein. Given the presence of nephrotic syndrome in the context of multiple myeloma, systemic immunoglobulin light-chain amyloidosis would be highest on the differential diagnosis with respect to cancer; however, the patient’s normal light-chain ratio makes this diagnosis unlikely. The development of myeloid neoplasms, such as acute myeloid leukemia, myelodysplastic syndromes, and myeloproliferative neoplasms, is important to consider in the context of previous treatment with alkylating agents, 1 which this patient had received. However, the peripheral-blood smear showed no findings that would indicate a hematologic cancer, and such a diagnosis would not explain the patient’s acute kidney injury with nephrotic-range proteinuria.

Infectious Disease

Several features of this patient’s case warrant special consideration, including her history of immunosuppression due to rheumatoid arthritis and to previously treated myeloma, along with the fact that she had emigrated from Central America, where certain infections may be prevalent. Infection with hepatitis A virus, hepatitis B virus, hepatitis C virus, HIV-1 and HIV-2, cytomegalovirus, Epstein–Barr virus, H. pylori, and M. tuberculosis can be ruled out on the basis of laboratory studies. A rapid antigen test for plasmodium species was reported to be positive, but this assay has a known cross-reactivity with rheumatoid factor. 2 Moreover, the thick and thin peripheral-blood smears were negative. Thus, malaria would be an unlikely diagnosis.
The patient has a history of infection with chikungunya virus, an arbovirus transmitted by a mosquito vector that has been responsible for large epidemics in the Americas since 2013. 3 Acute symptoms include fever, rash, arthralgia, and myalgia. The development of a chronic arthritis that may meet the classification criteria for rheumatoid arthritis, as defined by the American College of Rheumatology and the European Alliance of Associations for Rheumatology, has been reported in up to 60% of patients infected with chikungunya virus. 4,5 In the context of this discussion, I considered whether chikungunya virus infection could be the cause of this patient’s symptoms, since this infection occurred before the diagnosis of rheumatoid arthritis. However, the degree of erosion and loss of joint space that was visible on radiographs would be most unusual for arthritis associated with chikungunya virus infection and would not explain the renal manifestations.
Strongyloidiasis is a helminth infection (caused by Strongyloides stercoralis) that is widespread in developing countries. Infection usually occurs through contact with soil, and most affected persons are asymptomatic. However, in immunosuppressed persons, strongyloides hyperinfection syndrome or a disseminated infection can develop as a consequence of accelerated autoinfection. 6 The clinical presentation of strongyloides hyperinfection syndrome can include gastrointestinal symptoms (diarrhea, constipation, nausea, or vomiting), respiratory symptoms (cough, dyspnea, or wheezing), and rash due to migration of larvae through the subcutaneous tissues. Of note, only a minority of patients present with eosinophilia. Several case reports describe the development of nephrotic-range proteinuria, thrombotic microangiopathy, and IgA vasculitis in patients with strongyloides hyperinfection syndrome. 7-9 However, strongyloidiasis would not explain this patient’s cytopenias and hypocomplementemia.

Autoimmune Disease

The patient has a 3-year history of rheumatoid arthritis, although her clinical features of swan-neck deformity, boutonnière deformity, and joint instability suggest a longer duration of disease. We do not know whether she had received previous treatment with disease-modifying antirheumatic drugs or biologic agents, but the possible use of such treatments may be a consideration with respect to her progression of disease and overall degree of immunosuppression. The blood levels of rheumatoid factor and anti–cyclic citrullinated peptide antibodies were elevated, and radiographs of the hands showed erosive disease, although there was a relative paucity of metacarpophalangeal findings. A review of systems was negative for dry mouth, but her physical examination showed poor dentition and dry mouth — findings that make secondary Sjögren’s syndrome a consideration.
Renal disease can occur in patients with Sjögren’s syndrome. The two most typical presentations are tubulointerstitial nephritis and, less commonly, nephritic syndrome (membranoproliferative glomerulonephritis related to cryoglobulinemia). Tubulointerstitial nephritis may manifest with renal disease of varying severity, usually with a bland urinary sediment and often with abnormalities of tubular function such as distal renal tubular acidosis. Membranoproliferative glomerulonephritis caused by cryoglobulinemia is the most common glomerular disease associated with Sjögren’s syndrome. Although nephrotic-range proteinuria can occur with Sjögren’s syndrome, it is relatively uncommon. 10 Renal disease is uncommon in patients with rheumatoid arthritis and is usually related to coexisting cardiovascular conditions. Medications used in the treatment of autoimmune disease — mainly nonsteroidal antiinflammatory drugs — may be associated with renal disease, but I would not expect the presence of an active urinary sediment, as was seen in this patient.
Amyloid A (AA) amyloidosis, a condition that is rare in the era of aggressive management of rheumatoid arthritis, has been described in patients with severe, long-standing seropositive erosive rheumatoid arthritis. Serum amyloid A (SAA) is a protein that is produced in the liver in response to chronic inflammation associated with interleukin-1, interleukin-6, and tumor necrosis factor α (TNF-α) in the context of chronic infections, autoimmune disease (classically rheumatoid arthritis), autoinflammatory disease, and cancers including renal cell carcinoma and non-Hodgkin’s lymphoma. 11 Signs and symptoms of AA amyloidosis are related to the deposition of the protein in organs, and patients often present with multisystem signs and symptoms. The kidney is the organ that is most often affected, but deposition can occur in the heart, gastrointestinal tract, nervous system, musculoskeletal system, and lungs. Proteinuria is the first clinical manifestation in almost 95% of patients with AA amyloidosis, and 50% of affected patients present with nephrotic syndrome. 12 The urinary sediment is generally bland, and complement levels in the blood are normal. AA amyloidosis remains on the differential diagnosis in this patient, but it would not completely explain her renal disease.

Hypocomplementemia

The key to this case is understanding the cause of this patient’s hypocomplementemia. Hypocomplementemia can be due to decreased complement production in the context of liver disease, congenital complement deficiency, or increased complement consumption resulting from activation of the innate immune system. This patient has no history of chronic liver disease and her laboratory test results indicated good hepatic synthetic function. Classical complement deficiency (including C4 deficiency) that begins early in life is associated with autoimmune disease, and early C3 deficiency is characterized by severe pyogenic infections. It would be unusual for a patient of this age to be deficient in both C3 and C4 without earlier clinical consequences. I therefore concluded that the hypocomplementemia in this case was related to complement consumption.
Rheumatic diseases that may be associated with prominent renal manifestations include antineutrophil cytoplasmic antibody–associated vasculitis, systemic sclerosis with renal crisis, cryoglobulinemic vasculitis, antiglomerular basement membrane disease, and systemic lupus erythematosus (SLE). Of those conditions, SLE would be the most likely to be manifested by an active urinary sediment and nephrotic-range proteinuria with consumption of both C3 and C4 in the context of fever, thrombocytopenia, and serositis. This patient’s fever, thrombocytopenia, and serositis also fit with this diagnosis. 13
Because the patient has long-standing seropositive erosive rheumatoid arthritis, a diagnosis of AA amyloidosis is strongly suspected. Moreover, given the presence of thrombocytopenia, hypocomplementemia, and an active urinary sediment, I would recommend a kidney biopsy to evaluate for lupus nephritis and AA amyloidosis.

Dr. Beth L. Jonas’s Diagnosis

Overlap syndrome of rheumatoid arthritis and systemic lupus erythematosus with amyloid A amyloidosis.

Pathological Discussion

Dr. Claire Trivin-Avillach: Testing for autoimmune antibodies was performed. A test for antinuclear antibodies was positive at a titer of 1:5120 with a homogeneous pattern, and a test for anti–double-stranded DNA antibodies was positive at a titer of 1:2560.
The diagnostic procedure in this case was a core-needle biopsy of the kidney. Examination of the specimen with light microscopy revealed 20 glomeruli, 45% of which were globally sclerosed, along with fibrosis involving approximately 60% of the interstitium and tubular atrophy. Diffusely enlarged glomeruli with thickened capillary walls and an expanded mesangium were weakly positive on periodic acid–Schiff staining; the glomeruli stained pale blue on Masson’s trichrome staining. Congo red staining revealed metachromatic salmon-colored deposition involving the glomeruli, the blood-vessel walls, and the interstitium, which was associated with apple-green birefringence when viewed under polarized light (Fig. 3A). In addition, mesangial and endocapillary hypercellularity was identified in approximately 30% of the nonsclerosed glomeruli and was associated with karyorrhexis (Fig. 3B). One cellular crescent was also detected. These features are characteristic of active proliferative glomerulonephritis.
Figure 3
Biopsy Specimen of the Kidney.
Immunofluorescence microscopy revealed prominent granular staining for IgG (4+), IgM (4+), C3 (3+), C1q (3+), IgA (1+), kappa (3+), and lambda (3+) along the glomerular basement membranes and within the mesangium, as well as focal granular deposits of IgG and C3 along the tubular basement membrane (Fig. 3C and 3D). Additional immunofluorescence studies showed strong positivity (4+) for SAA within the glomeruli, the blood-vessel walls, and the interstitium (Fig. 3E), whereas staining for beta2-microglobulin, transthyretin, and apolipoprotein A1 was faint.
Electron microscopy revealed the presence of subendothelial and mesangial electron-dense deposits (with no substructure identified) adjacent to randomly arranged fibrils (measuring 8.2 to 10.6 nm in diameter) within the glomerular basement membranes and the mesangium (Fig. 3F). Glomerular endothelial cells appeared reactive and contained tubuloreticular inclusions, features that were suggestive of interferon-mediated activation.
The findings on Congo red staining were characteristic of amyloidosis with typical birefringent material. The strong positivity of SAA within the deposits as compared with the faint staining of other reactants identified the type of amyloid as SAA, which is consistent with the patient’s history of rheumatoid arthritis. The biopsy also showed an immune complex–mediated proliferative glomerulonephritis with a “full house” pattern (defined as positivity for the three immunoglobulin classes IgG, IgM, and IgA and the two complement components C3 and C1q, in reference to the “full house” hand in a poker game). Immune complex–mediated proliferative glomerulonephritis has been reported in patients with rheumatoid arthritis who were receiving anti–TNF-α therapy, 14 which was not the case in this patient. The positive test for hepatitis C antibodies prompted consideration of hepatitis C–related membranoproliferative glomerulonephritis. However, taken together, the negative nucleic acid test for hepatitis C virus, the full house pattern on immunofluorescence, the tubular basement membrane deposits, and the positive test for anti–double-stranded DNA antibodies favor a diagnosis of lupus nephritis of at least class III (defined as focal proliferative glomerulonephritis), according to the criteria of the International Society of Nephrology and the Renal Pathology Society, superimposed on AA amyloidosis.

Pathological Diagnosis

Proliferative lupus nephritis of International Society of Nephrology and Renal Pathology Society class III, superimposed on amyloid A amyloidosis.

Discussion of Management

Dr. Pui W. Cheung: On the basis of the finding of echogenic kidneys on ultrasonography and the findings of extensive interstitial fibrosis and tubular atrophy on kidney biopsy, we know that this patient has advanced chronic kidney disease that is unlikely to be reversible. The patient is also noted to have a markedly lower glomerular filtration rate (GFR) than that predicted by the blood creatinine level owing to the presence of cachexia, and this is substantiated by the cystatin C–based GFR and a 24-hour creatinine clearance of 22 ml per minute per 1.73 m2 of body-surface area. The typical induction therapy for stage III or IV lupus nephritis consists of high-dose glucocorticoids and either mycophenolate mofetil or cyclophosphamide. Other reasonable alternatives for initial therapy include mycophenolate mofetil in combination with either a calcineurin inhibitor or belimumab, or cyclophosphamide in combination with belimumab. 15 Hydroxychloroquine is also recommended as part of the therapy, since it has shown benefits in improving the response to treatment and reducing disease flare. 16 Mycophenolate mofetil and cyclophosphamide have similar efficacy with respect to clinical response, which includes a reduction in proteinuria and either an improvement in renal function or stabilization of renal function; the risks of infections and adverse events associated with these medications are also similar. 17,18
Given the severity of the lupus nephritis with overlying AA amyloidosis from active rheumatoid arthritis, the treatment options proposed were high-dose glucocorticoids and rituximab with either mycophenolate mofetil or cyclophosphamide. 19 After discussions with multidisciplinary consultants from rheumatology, infectious diseases, and nephrology, lingering concerns were raised about infection and patient frailty; ultimately, the decision was made to initiate high-dose glucocorticoid therapy in combination with mycophenolate mofetil, rituximab, and hydroxychloroquine.
The patient’s mycophenolate mofetil dose regimen was inconsistent owing to gastrointestinal side effects, and the treatment was eventually withheld because of pancytopenia and fever. Unfortunately, her kidney function worsened, and renal replacement therapy was initiated within 3 weeks after the start of the induction therapy. The cause of her renal failure was thought to be disease progression, compounded by hemodynamically mediated tubular injury in the context of infection. While the administration of mycophenolate mofetil was stopped, treatment with rituximab was continued, with slow tapering of the glucocorticoid dose at the direction of the rheumatologist. She remained dependent on dialysis and was deemed to have end-stage kidney disease after 3 months of dialysis.
Dr. Lisa G. Criscione-Schreiber: The patient has SLE with nephritis, seropositive erosive rheumatoid arthritis, and systemic AA amyloidosis. AA amyloidosis is rare owing to the availability of effective therapies for rheumatoid arthritis and is managed through aggressive treatment of inflammation due to rheumatoid arthritis. Reports addressing the management of rheumatoid arthritis–induced AA amyloidosis generally cite stability of end-organ damage caused by AA amyloid as evidence of effective management of the condition (through treatment of the inflammation of rheumatoid arthritis). Methotrexate, the cornerstone of treatment for rheumatoid arthritis, is contraindicated in this case owing to the presence of kidney disease. The alkylating agent cyclophosphamide has been reported to be effective for the treatment of AA amyloidosis from rheumatoid arthritis 20 and has known efficacy in patients with lupus nephritis, both of which make it a viable treatment option. Rituximab has also been reported to be effective for managing rheumatoid arthritis–induced AA amyloidosis, 21 is approved for the treatment of rheumatoid arthritis, and is used for manifestations of SLE, including thrombocytopenia and nephritis. Although anti–TNF-α agents, abatacept, and Janus kinase inhibitors are reported to be effective for the treatment of AA amyloidosis in patients with rheumatoid arthritis, 22 recent publications have coalesced on the ability of anti–interleukin-6 therapy to block interleukin-6–induced hepatic production of SAA. 23-25
The overlap of seropositive erosive rheumatoid arthritis and SLE (sometimes termed “rhupus”) usually resembles rheumatoid arthritis more than SLE; manifestations include thrombocytosis, leukocytosis, an elevated erythrocyte sedimentation rate, an elevated blood level of C-reactive protein, and the presence of marginal erosions on radiographs. 26 In contrast, SLE without seropositive erosive rheumatoid arthritis characteristically manifests with thrombocytopenia, leukopenia, and an elevated erythrocyte sedimentation rate but usually not an elevated C-reactive protein level; in addition, nonerosive inflammatory arthritis with reversible deformities is commonly observed. This patient had a mixed laboratory profile, on the basis of the results of antinuclear antibody and anti–double-stranded DNA antibody tests. The challenge of treating an overlap syndrome of rheumatoid arthritis and SLE is choosing disease-modifying antirheumatic drugs that are effective and safe in both conditions. This patient’s most severe disease manifestation is lupus nephritis; therefore, the treatment regimen must target nephritis along with the AA amyloidosis and inflammatory arthritis.
As noted earlier, current induction therapy for lupus nephritis includes either mycophenolate mofetil or cyclophosphamide. Mycophenolate mofetil may provide inadequate treatment of the rheumatoid arthritis and amyloidosis, whereas cyclophosphamide would treat the lupus nephritis, has possible efficacy for treatment of the AA amyloidosis, and would treat the rheumatoid arthritis. Rituximab could be added to cyclophosphamide or mycophenolate mofetil to treat the rheumatoid arthritis and resultant AA amyloidosis and could also possibly help treat the lupus nephritis. The addition of anti–interleukin-6 therapy to mycophenolate mofetil or cyclophosphamide is an intriguing option that may effectively treat the rheumatoid arthritis and subsequent AA amyloidosis. The addition of belimumab to mycophenolate mofetil or cyclophosphamide has been reported to improve renal response in patients with lupus nephritis, 27 as has the addition of voclosporin to mycophenolate mofetil. 28 However, belimumab is ineffective for the treatment of rheumatoid arthritis, and voclosporin has not been studied in patients with rheumatoid arthritis or in those with a GFR of 45 milliliters per minute or less. The high-dose glucocorticoids that are used in induction therapy for lupus nephritis will effectively manage this patient’s inflammatory arthritis and probably also the subsequent AA amyloidosis. Finally, it is important that every patient with lupus nephritis receive hydroxychloroquine, which improves the treatment response to induction therapy. 29

Follow-up

Dr. Parsons: The patient’s hospital course was further complicated by suspected immune-mediated thrombocytopenia, for which she received intravenous immune globulin. Her pancytopenia and arthritis ultimately abated. Unfortunately, she did not have renal recovery and continues to receive hemodialysis. After a prolonged hospital course, she was discharged home.

Final Diagnosis

Overlap syndrome of rheumatoid arthritis and systemic lupus erythematosus complicated by proliferative lupus nephritis, superimposed on amyloid A amyloidosis.

以下内容来源于PubMed。

Abstract

Sacituzumab govitecan (SG) significantly improved progression-free survival (PFS) and overall survival (OS) versus chemotherapy in hormone receptor-positive human epidermal growth factor receptor 2-negative (HR+HER2-) metastatic breast cancer (mBC) in the global TROPiCS-02 study. TROPiCS-02 enrolled few Asian patients. Here we report results of SG in Asian patients with HR+HER2- mBC from the EVER-132-002 study. Patients were randomized to SG (n = 166) or chemotherapy (n = 165). The primary endpoint was met: PFS was improved with SG versus chemotherapy (hazard ratio of 0.67, 95% confidence interval 0.52-0.87; P = 0.0028; median 4.3 versus 4.2 months). OS also improved with SG versus chemotherapy (hazard ratio of 0.64, 95% confidence interval 0.47-0.88; P = 0.0061; median 21.0 versus 15.3 months). The most common grade ≥3 treatment-emergent adverse events were neutropenia, leukopenia and anemia. SG demonstrated significant and clinically meaningful improvement in PFS and OS versus chemotherapy, with a manageable safety profile consistent with prior studies. SG represents a promising treatment option for Asian patients with HR+HER2- mBC (ClinicalTrials.gov identifier no. NCT04639986 ).

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