Aquaporin-4-IgG-seropositive neuromyelitis optica spectrum disorders:progress of experimental models based on disease pathogenesis

Neuromyelitis optica spectrum disorders are neuroinflammatory demyelinating disorders that lead to permanent visual loss and motor dysfunction.To date,no effective treatment exists as the exact causative mechanism remains unknown.Therefore,experimental models of neuromyelitis optica spectrum disorders are essential for exploring its pathogenesis and in screening for therapeutic targets.Since most patients with neuromyelitis optica spectrum disorders are seropositive for IgG autoantibodies against aquaporin-4,which is highly expressed on the membrane of astrocyte endfeet,most current experimental models are based on aquaporin-4-IgG that initially targets astrocytes.These experimental models have successfully simulated many pathological features of neuromyelitis optica spectrum disorders,such as aquaporin-4 loss,astrocytopathy,granulocyte and macrophage infiltration,complement activation,demyelination,and neuronal loss;however,they do not fully capture the pathological process of human neuromyelitis optica spectrum disorders.In this review,we summarize the currently known pathogenic mechanisms and the development of associated experimental models in vitro,ex vivo,and in vivo for neuromyelitis optica spectrum disorders,suggest potential pathogenic mechanisms for further investigation,and provide guidance on experimental model choices.In addition,this review summarizes the latest information on pathologies and therapies for neuromyelitis optica spectrum disorders based on experimental models of aquaporin-4-IgG-seropositive neuromyelitis optica spectrum disorders,offering further therapeutic targets and a theoretical basis for clinical trials.

奥法妥木单抗治疗视神经脊髓炎谱系疾病疗效分析

目的探讨奥法妥木单抗治疗视神经脊髓炎谱系疾病(NMOSDs)的疗效及安全性。方法纳入2022年4月至2023年3月郑州大学第一附属医院采用奥法妥木单抗治疗方案的25例NMOSDs患者,分为定期给药组(A组,12例)及按CD19+B细胞百分比给药组(B组,13例),计算用药前和用药1年时年化复发率(ARR)、复发例数、复发次数和时间、复发症状,采用扩展残疾状态量表(EDSS)评估神经功能,记录用药期间药物不良反应。结果奥法妥木单抗治疗1年时3例(12%)复发,A组1例患者复发2次,分别为用药后1和5个月;B组2例患者复发,1例复发2次,为用药后2和6个月,1例复发1次,为用药后2个月。两组用药1年时与用药前仅ARR变化幅度差异具有统计学意义(F=29.061,P=0.000),A组用药1年时ARR较用药前下降(t=13.215,P=0.001),B组用药1年时ARR亦较用药前下降(t=19.259,P=0.000)。有8例出现注射部位疼痛、3例注射后发热、1例注射后头痛,其中1例诊断为细菌性脑膜炎;14例感染新型冠状病毒,其中1例因新型冠状病毒感染致肺炎入住重症监护病房;均无残疾、死亡等严重不良反应,EDSS评分均未增加。结论奥法妥木单抗定期给药或依据CD19+B细胞百分比给药均可减少患者复发风险,改善EDSS评分;早期与糖皮质激素联用需警惕感染风险。

干燥综合征合并视神经脊髓炎谱系疾病的临床特征分析

目的分析干燥综合征(SS)合并视神经脊髓炎谱系疾病(NMOSD)患者的临床特征、治疗及预后情况。方法检索中国学术期刊数据库(万方)、中国期刊全文数据库(中国知网)、中文科技期刊数据库(维普)、PubMed数据库,检索时间为2011年至2021年,以“干燥综合征、视神经脊髓炎谱系疾病”“干燥综合征神经系统病变”“Sjogren syndrome”“NMOSD”为关键词,分析SS合并NMOSD患者的临床表现、辅助检查及治疗预后情况。结果SS合并NMOSD女性占比较高(94.44%);临床表现常见为视力下降(61.11%),乏力(59.49%),麻木(39.24%),大小便障碍(21.51%),恶心、呕吐(16.45%);实验室检查常存在中枢神经系统水通道蛋白4(AQP4)抗体阳性(87.34%)、抗SSA抗体阳性(93.75%),脑脊液蛋白升高(50.67%);受累部位:以视神经(49.44%)及脊髓(62.01%)病变常见,还可累及脑干、大脑、脑白质。激素及免疫抑制剂治疗有效,但部分患者可能残留视力下降、乏力等症状,复发率为49.69%。结论SS合并NMOSD视力下降及麻木乏力症状多见,常出现视神经及脊髓病变,AQP4抗体对诊断意义大,早期激素和免疫抑制剂治疗可能减少复发,改善预后。

低剂量利妥昔单抗治疗视神经脊髓炎谱系疾病的疗效

目的探索本文研究病例采取低剂量的利妥昔单抗达到的效果。方法选择我院2019年11月—2023年12月接收的30例视神经脊髓炎谱系疾病患者为研究对象,将其按照随机数字表法分组,分为观察组(n=15,低剂量利妥昔单抗)与对照组(n=15,吗替麦考酚酯)。对比两组治疗后扩展残疾状态量表(EDSS)评分,血清B淋巴细胞活化因子(BAFF)水平,血清AQP4-IgG水平、年复发率(ARR)、不良反应发生率以及生活质量(SF-36)评分。结果治疗后,观察组的EDSS评分低于对照组(P<0.05);治疗后,观察组BAFF水平以及血清AQP4-IgG水平均低于对照组(均P<0.05);治疗后,观察组的ARR低于对照组(P<0.05);观察组不良反应发生率为6.67%,低于对照组的26.67%(P<0.05);治疗后,观察组社会领域、生理领域、心理领域、环境领域评分均相较于对照组更高(均P<0.05)。结论使用低剂量利妥昔单抗治疗视神经脊髓炎谱系疾病治疗疗效较佳,能够有效改善神经功能,降低血清BAFF水平和AQP4-IgG水平,预防病情复发,安全性较高。

视神经脊髓炎谱系疾病免疫机制的研究进展

视神经脊髓炎谱系疾病(neuromyelitis optica spectrum disorders,NMOSD)是一种自身免疫性中枢神经系统炎性脱髓鞘疾病,主要表现为反复发作的视神经炎和纵向延伸累及多节段的横贯性脊髓炎。水通道蛋白4(AQP4)抗体(AQP4-IgG)是诊断NMOSD的高度特异性生物标志物,大多数患者血清AQP4-IgG阳性。AQP4-IgG与AQP4结合引起细胞毒性反应,继而诱发免疫细胞的激活及炎症因子的释放,最终导致神经元损伤。研究发现多种免疫细胞(如B细胞、T细胞)参与了NMOSD的炎症反应过程。现就参与NMOSD发病过程的免疫细胞类型及其作用途径和NMOSD的免疫机制研究进展进行综述,期望为NMOSD的治疗提供新的研究靶点和策略。

抗水通道蛋白4抗体阳性视神经脊髓炎谱系疾病诊断与治疗进展

视神经脊髓炎谱系疾病(NMOSDs)以抗水通道蛋白4(AQP4)抗体阳性NMOSDs最为多见,主要表现为反复发作的视神经炎和脊髓炎等,严重降低患者生活质量。近年来,对该病的诊断技术、诊断标志物和免疫治疗药物不断有新的认识,本文综述抗AQP4抗体阳性NMOSDs的诊断技术和诊断标志物新进展以及新的治疗药物,以促进对该病的诊断与治疗新技术的理解和应用,探索更多可能的临床诊断与治疗方法。

肝、肾功能及免疫相关指标在视神经脊髓炎谱系疾病诊断中的应用价值

目的分析肝功能、肾功能、自身抗体指标在神经脊髓炎谱系疾病(NMOSD)患者中的分布特点及其诊断价值。方法回顾性收集2015年6月至2023年6月在首都医科大学附属北京天坛医院确诊为NMOSD、多发性硬化(MS)患者,以及性别、年龄匹配的常规体检健康者肝功能、肾功能和自身抗体检测数据。共纳入95例NMOSD患者(NMOSD组)、230例MS患者(MS组)、244例常规体检健康者(常规体检组),评估各指标对NMOSD的诊断价值。结果与MS组相比,NMOSD组丙氨酸氨基转移酶、α-羟基丁酸脱氢酶、γ-谷氨酰基转移酶水平,以及抗SS-A抗体、抗SS-B抗体、抗核糖体P蛋白抗体和Ro-52抗体阳性率等明显升高,白蛋白、间接胆红素、总胆红素水平明显降低,差异均有统计学意义(P<0.05)。NMOSD组与常规体检组差异指标与MS组相似。α-羟丁酸脱氢酶、白蛋白、球蛋白、直接胆红素、间接胆红素、总胆汁酸和尿酸碱度7项指标均可用于NMOSD诊断,联合诊断的曲线下面积为0.969,灵敏度和特异度为92.6%和92.9%。结论NMOSD患者多种肝、肾功能指标与MS和常规体检健康者存在差异,NMOSD患者部分自身抗体指标阳性率高于MS患者,临床可将肝、肾功能及自身抗体指标用于辅助诊断,并且多指标联合应用可进一步提升其诊断价值。

Biomarkers for neuromyelitis optica:a visual analysis of emerging research trends

Neuromyelitis optica is an inflammatory demyelinating disease of the central nervous system that differs from multiple sclerosis.Over the past 20 years,the search for biomarke rs for neuromyelitis optica has been ongoing.Here,we used a bibliometric approach to analyze the main research focus in the field of biomarkers for neuromyelitis optica.Research in this area is consistently increasing,with China and the United States leading the way on the number of studies conducted.The Mayo Clinic is a highly reputable institution in the United States,and was identified as the most authoritative institution in this field.Furthermore,Professor Wingerchuk from the Mayo Clinic was the most authoritative expe rt in this field.Keyword analysis revealed that the terms "neuro myelitis optica"(261 times), "multiple sclerosis"(220 times), "neuromyelitis optica spectrum disorder"(132 times), "aquaporin4"(99 times),and "optical neuritis"(87 times) were the most frequently used keywords in literature related to this field.Comprehensive analysis of the classical literature showed that the majority of publications provide conclusive research evidence supporting the use of aquaporin-4-IgG and neuromyelitis optica-IgG to effectively diagnose and differentiate neuromyelitis optica from multiple sclerosis.Furthermore,aquaporin-4-IgG has emerged as a highly specific diagnostic biomarker for neuromyelitis optica spectrum disorder.Myelin oligodendrocyte glycoprotein-IgG is a diagnostic biomarke r for myelin oligodendrocyte glycoprotein antibody-associated disease.Recent biomarkers for neuromyelitis optica in clude cerebrospinal fluid immunological biomarkers such as glial fibrillary acidic protein,serum astrocyte damage biomarkers like FAM19A5,serum albumin,and gammaaminobutyric acid.The latest prospective clinical trials are exploring the potential of these biomarkers.Preliminary results indicate that glial fibrillary acidic protein is emerging as a promising candidate biomarker for neuromyelitis optica spectrum disorder.The ultimate goal of future research is to identify non-invasive biomarkers with high sensitivity,specificity,and safety for the accurate diagnosis of neuro myelitis optica.

视神经脊髓炎谱系疾病患者睡眠质量的研究进展

视神经脊髓炎谱系疾病是一种罕见的自身免疫性疾病,会导致中枢神经系统严重炎症,主要影响视神经和脊髓,不仅会造成身体功能的损害,也会带来心理、疲劳等一系列问题。睡眠障碍在视神经脊髓炎谱系疾病患者中普遍存在,与其他临床症状共同出现,相互影响,严重影响患者的预后及身心健康。越来越多的学者进行了相关的研究。本文对视神经脊髓炎谱系疾病患者睡眠障碍的评估工具、影响因素等进行综述,以期为早期识别视神经脊髓炎谱系疾病患者睡眠障碍并开展相关干预提供参考。

OCT及OCTA评估水通道蛋白-4抗体阳性NMOSD视网膜结构和血管密度及其与临床特征的关系

目的应用光学相干断层扫描(optical coherence tomography,OCT)及血管成像(optical coherence tomography angiography,OCTA)评价视神经脊髓炎谱系疾病(neuromyelitis optica spectrum disorders,NMOSD)视网膜结构和血管密度改变及其与临床疾病特征的相关性。方法共纳入水通道蛋白-4抗体阳性的NMOSD患者42例(84只眼),健康对照(对照组)45名(90只眼)。根据视神经炎(optic neuritis,ON)病史,NMOSD组进一步分为两组:有ON病史的NMOSD+ON组和无ON病史的NMOSD-ON组。通过OCT和OCTA测量神经节细胞复合体(ganglion cell complex,GCC)厚度、视网膜神经纤维层(retinal nerve fiber layer,RNFL)厚度、黄斑区浅层毛细血管丛(superficial capillary plexus,SCP)、深层毛细血管丛(deep capillary plexus,DCP)和视盘区血管的血管密度。记录患者NMOSD病程和发作次数、最佳矫正视力(best corrected visual acuity,BCVA)和扩展残疾状态量表(expanded disability status scale,EDSS)评分,分析上述指标与OCT和OCTA观察指标之间的相关性。结果黄斑和视盘的结构改变:与对照组比较,NMOSD+ON组总体及颞区(TEM)、上区(SUP)、鼻区(NAS)、下区(INF)各区的RNFL厚度均明显降低(P<0.05);NMOSD-ON组总体和SUP区的RNFL厚度明显降低(P<0.05)。与NMOSD-ON组比较,NMOSD+ON组总体及TEM、SUP、NAS、INF各区的RNFL厚度均明显降低(P<0.05)。与对照组比较,NMOSD+ON组总体、SUP及INF区的GCC厚度明显降低(P<0.05);NMOSD-ON组总体及SUP区的GCC厚度明显降低(P<0.05)。与NMOSD-ON组比较,NMOSD+ON组总体GCC厚度及SUP、INF区的GCC厚度明显降低(P<0.05)。黄斑区血管密度:与对照组比较,NMOSD+ON组SCP总体、中心凹、中心凹旁及中心凹周围TEM、SUP、NAS、INF各区血管密度均明显降低(P<0.05)。与对照组比较,NMOSD-ON组DCP总体血管密度、中心凹旁及中心凹周围TEM、SUP、NAS、INF各区血管密度均明显降低(P<0.05)。与NMOSD-ON组比较,NMOSD+ON组SCP总体血管密度以及中心凹旁TEM区、SUP区、INF区和中心凹周围TEM、SUP、NAS、INF各区血管密度均明显降低(P<0.05),DCP中心凹、中心凹旁NAS区、中心凹周围TEM区血管密度明显升高(P<0.05)。与对照组比较,NMOSD+ON组视盘区总体血管密度,视盘内血管密度以及和视盘旁鼻上区(NS)、鼻下区(NI)、下鼻区(IN)、下颞区(IT)、颞下区(TI)、颞上区(TS)、上颞区(ST)、上鼻区(SN)各区血管密度均明显降低(P<0.05)。与NMOSD-ON组比较,NMOSD+ON组除视盘内血管密度差异无统计意义(P=0.268)外,视盘区总体血管密度和视盘旁各区血管密度均明显降低(P<0.05)。NMOSD组病程与GCC厚度、RNFL厚度、SCP血管密度、放射状周围毛细血管(RPC)血管密度均呈负相关(分别r=-0.436,P<0.001;r=-0.337,P=0.002;r=-0.325,P=0.003;r=-0.239,P=0.028),发病次数与RNFL厚度、RPC血管密度呈负相关(分别r=-0.360,P=0.001;r=-0.315,P=0.004),BCVA与GCC厚度呈负相关(r=-0.303,P=0.005)。结论NMOSD患者发生和不发生ON的眼,均存在视网膜结构和视网膜血管的损伤,且NMOSD病程越长、发病次数越多,损伤越明显。与没有ON的眼相比,ON患眼SCP血管密度减低。

小剂量利妥昔单抗治疗视神经脊髓炎谱系疾病发生感染的影响因素

目的:对小剂量利妥昔单抗(RTX)治疗视神经脊髓炎谱系疾病(NMOSD)发生感染的相关因素进行分析,为预防病人感染提供依据。方法:选择2014年1月—2022年6月就诊于山西医科大学第一医院使用小剂量RTX治疗NMOSD的65例病人作为研究对象。收集病人的临床特征及实验室指标,通过门诊、电话随访了解病人有无感染发生,分为感染组与非感染组,对相关因素进行统计学分析。结果:65例病人中,有20例发生感染,感染率为31%,年龄、高血压、糖尿病、使用过免疫抑制剂、行走功能障碍、睡眠障碍及排尿障碍(P<0.05)为感染发生的危险因素。多因素Cox回归分析显示,睡眠障碍[HR=6.527,95%CI(1.955,21.798),P=0.005]、排尿障碍[HR=19.441,95%CI(1.365,12.950),P=0.015]是小剂量RTX治疗NMOSD发生感染的危险因素。结论:小剂量RTX治疗NMOSD病人发生感染与睡眠障碍、排尿障碍密切相关。

视神经脊髓炎相关视神经炎合并中心性浆液性脉络膜视网膜病变1例

40岁男性,因“左眼突发视力下降1周”入院。患者3个月前因“左视神经脊髓炎相关视神经炎”行激素冲击及序贯减量治疗,1周前感染新型冠状病毒后自觉左眼视力下降。体格检查:左眼最佳矫正视力为FC/5cm,前节未见明显异常,左眼相对性瞳孔传入障碍(RAPD)(+),眼底见视盘边界清晰,杯盘比(C/D)约0.5,A:V约2:3,视网膜平伏、色泽正常;右眼未见异常。入院后光学相干层析成像(OCT)检查提示左眼颞下血管弓位置一约2 PD直径的视网膜神经上皮层脱离区域。完善感染相关检查、血清脱髓鞘抗体检测、眼眶磁共振成像(MRI)平扫+增强后,患者确诊:①左眼复发性抗体双阴性视神经脊髓炎相关视神经炎;②双眼中心性浆液性脉络膜视网膜病变(CSC)。仍予以激素冲击及序贯减量治疗视神经炎,随访观察CSC。治疗6个月后,患者右眼BCVA为0.6,双眼CSC病变消退。讨论体会:视神经脊髓炎相关视神经炎合并未累及中心凹的CSC,仍应该给予规范性的激素冲击治疗及序贯减量。

补体调节因子与视神经脊髓炎谱系疾病的研究进展

视神经脊髓炎谱系疾病(NMOSD)是一种获得性、异质性神经眼科交叉性罕见免疫性疾病,特异性高发于视神经和脊髓等中枢神经系统部位,有严重的致残致盲性。虽然补体在NMOSD发病中的重要性已被证实,但膜补体调节因子在NMOSD发病机制中的关键调控作用尚不完全清楚,论述其在NMOSD发病中的生理和病理作用,可能成为解释NMOSD中枢发病的重要原因之一。本文重点回顾近些年来与NMOSD发病相关的补体调节因子CD46、CD55和CD59的研究进展,试图分析、综述补体调节因子在NMOSD发病机制中的作用现状及未来发展前景。

早发型与晚发型视神经脊髓炎谱系疾病患者的临床特点分析

目的:分析早发型(EO-NMOSDs)与晚发型视神经脊髓炎谱系疾病患者(LO-NMOSDs)不同的临床特征。方法:纳入2015年1月至2022年12月海南医学院第一附属医院收治的51例首次在我院确诊的视神经脊髓炎谱系疾病患者,根据发病年龄是否≥50岁分为EO-NMOSDs组22例和LO-NMOSDs组29例。统计分析两组患者的基本资料、扩展残疾状态量表(EDSS)评分、血和脑脊液化验指标。结果:两组间在人口学特征、临床特征及血清AQP-4抗体阳性率方面均无统计学意义(均P>0.05),在甘油三酯、低密度脂蛋白、载脂蛋白A、载脂蛋白B和脂蛋白a上有统计学差异(分别为P=0.010、P=0.048、P=0.014、P=0.061、P=0.001),以及脑脊液乳酸脱氢酶、微量蛋白定量和EDSS评分有统计学差异(分别为P=0.018、P=0.034、P=0.025),其中LO-NMOSDs脑脊液微量蛋白定量的水平与患者残疾程度有一定的相关性(r=0.52,P<0.03)。结论:LO-NMOSDs与EO-NMOSDs组患者具有相似的人口统计学特征、血清AQP-4抗体阳性率及临床特征,但与EO-NMOSDs相比,LO-NMOSDs组患者易患有脂质代谢异常,脑脊液中有较高的微量蛋白以及更易致残,并且在LO-NMOSDs中,脑脊液微量蛋白越高,患者的致残状况越重。

视神经脊髓炎谱系疾病的疾病修饰治疗进展

视神经脊髓炎谱系疾病(NMOSD)是一种严重的炎症性脱髓鞘疾病,其治疗主要包括急性期治疗和缓解期预防发作治疗。NMOSD缓解期的疾病修饰治疗(DMT)可有效减少疾病复发,延缓残疾程度的进展。目前国内外常用于DMT的药物包括经典免疫抑制、B细胞表面抗原单克隆抗体、补体靶向单克隆抗体、白细胞介素-6受体靶向单克隆抗体等,本文就NMOSD的DMT药物有效性、安全性及在中国上市情况进行综述。

视神经脊髓炎谱系疾病生物靶向治疗研究进展

视神经脊髓炎谱系疾病(neuromyelitis optica spectrum disorder,NMOSD)是一种自身免疫性中枢神经系统炎性脱髓鞘疾病,主要侵犯视神经和脊髓,具有高复发、高致残的特点,严重影响了患者的生活质量。在NMOSD的病程管理中,序贯治疗尤为重要。近年来,生物靶向制剂治疗NMOSD较传统免疫抑制剂显示出更好的疗效。本文就目前全球已获批用于治疗NMOSD的3类生物靶向制剂做一评述,包括补体抑制剂、IL-6受体阻断剂和B淋巴细胞耗竭剂,以期为NMOSD的生物靶向制剂治疗提供借鉴与参考。

1例误诊为脑梗死的视神经脊髓炎谱系疾病回顾分析并文献复习

本文回顾性分析1例误诊为脑梗死、以脑桥被盖下部综合征为主要特征的视神经脊髓炎谱系疾病患者的临床特点及诊疗经过,并结合国内外文献复习和总结视神经脊髓炎谱系疾病的诊断及诊疗原则。患者为53岁男性,急性起病,以面部麻木、闭目乏力、眼睑闭合不全、口角歪斜等面神经炎为首发表现,伴有肢体乏力、共济失调等症状,血清AQP4-IgG阳性,影像学提示桥臂病变,予糖皮质激素冲击、免疫抑制剂治疗症状好转。在临床工作中,以严重的视神经炎、急性脊髓炎为首发症状的视神经脊髓炎谱系病不难诊断,但表现为脑桥被盖下部综合征的视神经脊髓炎谱系病临床少见,易误诊,早期诊断并采用激素及免疫抑制剂治疗可有效阻止病程进展,改善预后,减少复发。

Comparison of inebilizumab or rituximab in addition to glucocorticoid therapy for neuromyelitis optica spectrum disorders

AIM:To investigate the short-term efficacy and safety of inebilizumab for neuromyelitis optica spectrum disorders(NMOSD).METHODS:A total of 33 patients with NMOSD treated with inebilizumab(Group INB,n=15)or rituximab(Group RTX,n=18)in addition to high-dose glucocorticoids were included.Both groups underwent hormone shock therapy during the acute phase.Subsequently,Group INB received inebilizumab injections during the remission phase,while Group RTX received rituximab injections.A comparison of aquaporins 4(AQP4)titer values,peripheral blood B lymphocyte counts,and visual function recovery was conducted before and 8wk after treatment.Additionally,adverse reactions and patient tolerability were analyzed after using inebilizumab treatment regimes.RESULTS:Following inebilizumab treatment,there was a significantly improvement in the visual acuity of NMOSD patients(P<0.05),accompanied by a notable decrease in AQP4 titer values and B lymphocyte ratio(P<0.05).Moreover,inebilizumab treatment showed a partial effect in preventing optic nerve atrophy(P<0.05).However,there were no significant differences in other therapeutic effects compared to rituximab,which has previously demonstrated substantial therapeutic efficacy(P>0.05).Furthermore,inebilizumab exhibited higher safety levels than that of rituximab injections.CONCLUSION:The combination of inebilizumab and high-dose glucocorticoids proves to be effective.In comparison to rituximab injections,inebilizumab displays better tolerance and safety.Moreover,it demonstrates a partial effect in preventing optic nerve atrophy.Thus,it stands as an effective method to reduce the disability rates and improve the daily living ability of patients with NMOSD.

Strengthening pharmacotherapy research for COVID-19-induced pulmonary fibrosis

The global spread of severe acute respiratory syndrome coronavirus 2 has resulted in a significant number of individuals developing pulmonary fibrosis(PF),an irreversible lung injury.This condition can manifest within a short inter-val following the onset of pneumonia symptoms,sometimes even within a few days.While lung transplantation is a potentially lifesaving procedure,its limited availability,high costs,intricate surgeries,and risk of immunological rejection present significant drawbacks.The optimal timing of medication administration for coronavirus disease 2019(COVID-19)-induced PF remains controversial.Despite this,it is crucial to explore pharmacotherapy interventions,involving early and preventative treatment as well as pharmacotherapy options for advanced-stage PF.Additionally,studies have demonstrated disparities in anti-fibrotic treatment based on race and gender factors.Genetic mutations may also impact therapeutic efficacy.Enhancing research efforts on pharmacotherapy interventions,while considering relevant pharmacological factors and optimizing the timing and dosage of medication administration,will lead to enhanced,personalized,and fair treatment for individuals impacted by COVID-19-related PF.These measures are crucial in lessening the burden of the disease on healthcare systems and improving patients'quality of life.

Statistical evaluation of cluster formation of relapse in neuromyelitis optica spectrum disorder

Evaluating the cluster formation of clinical attacks in chronic relapsing diseases is an important statistical issue because the presence of attack clusters may influence therapeutic strategies for relapse prevention.We recently reported the occurrence of unevenly clustered attacks in patients with anti-aquaporin-4(AQP4)antibody-positive neuromyelitis optica spectrum disorder(NMOSD)(Akaishi et al.,2020a).