依鲁替尼(Ibrutinib)合成路线图解

依鲁替尼(Ibrutinib)是一款由Pharmacyclics和Janssen Biotech公司联合研发的布鲁顿酪氨酸激酶(Bruton′s tyrosine kinase,BTK)抑制剂,也是第一个BTK靶向治疗套细胞淋巴癌(MCL)的小分子药物.本文对依鲁替尼的合成工艺进行归纳总结,以期为依鲁替尼的合成路线设计提供新思路.

Ibrutinib and atrial fibrillation:An in-depth review of clinical implications and management strategies

Ibrutinib,a targeted therapy for B-cell malignancies,has shown remarkable efficacy in treating various hematologic cancers.However,its clinical use has raised concerns regarding cardiovascular complications,notably atrial fibrillation(AF).This comprehensive review critically evaluates the association between ibrutinib and AF by examining incidence,risk factors,mechanistic links,and management strategies.Through an extensive analysis of original research articles,this review elucidates the complex interplay between ibrutinib’s therapeutic benefits and cardiovascular risks.Moreover,it highlights the need for personalized treatment approaches,vigilant monitoring,and interdisciplinary collaboration to optimize patient outcomes and safety in the context of ibrutinib therapy.The review provides a valuable resource for healthcare professionals aiming to navigate the intricacies of ibrutinib’s therapeutic landscape while prioritizing patient well-being.

Ibrutinib逆转SDF-1α/CXCR4介导的急性淋巴细胞白血病耐药机制

目的:探讨在急性淋巴细胞白血病细胞株SUP-B15中Ibrutinib对SDF-1α/CXCR4轴介导的耐药影响。方法:流式细胞术检测细胞凋亡及细胞表面CXCR4表达情况,Western blot检测CXCR4、ERK、Bcl-xL表达水平,qPCR检测CXCR4的mRNA表达水平。结果:Ibrutinib增强化疗药物阿霉素诱导SUP-B15的凋亡(17.100%±4.3%vs28.133%±3.16%);Ibrutinib抑制SDF-1α诱导的CXCR4磷酸化,呈浓度和时间依赖性(r_(24h)=-0.99659,r_(48h)=-0.99764,r=-0.99980);Ibrutinib抑制CXCR4下游信号分子ERK、BCL-xL的表达与活性。结论:Ibrutinib增强SUP-B5细胞株对化疗药物阿霉素的敏感性,逆转SDF-1α/CXCR4轴介导的耐药,其可能的作用机制是通过抑制CXCR4/ERK/BCL-xL信号通路而实现的。

Bruton酪氨酸激酶及Ibrutinib应用于B细胞肿瘤的研究进展

Bruton酪氨酸激酶(BTK)是非受体酪氨酸激酶肝脏肿瘤中表达的酪氨酸激酶家族的一员,是B细胞受体信号通路中的关键蛋白分子,在正常B淋巴细胞的成熟以及B细胞肿瘤中发挥重要的作用。Ibrutinib是BTK的小分子抑制剂,它能不可逆地与BTK结合,有效抑制包括慢性淋巴细胞白血病、非霍奇金淋巴瘤和多发性骨髓瘤等血液系统B细胞恶性肿瘤细胞的生存和发展。Ibrutinib的作用已经在体内实验以及临床试验中获得肯定。现就BTK的分子结构、作用机制,以及Ibrutinib临床前和临床研究等方面进行综述。

Ibrutinib alleviated LPS-induced neuroinflam⁃mation and synaptic defects in mouse model of depression

OBJECTIVE Previous studies have demonstrated a close association between an altered immune system and major depressive disorders,and inhibition of neuroinflammation may represent an alternative mechanism to treat depression.Recently,the anti-inflammatory activ⁃ity of ibrutinib has been reported.However,the effect of ibrutinib on neuroinflammation-induced depression and its underlying mechanism has not been comprehensively studied.Therefore,we aimed to elucidate the potential anti-depres⁃sive role and mechanism of ibrutinib against neu⁃roinflammation-induced depression and synaptic defects.METHODS AND RESULTS Ibrutinib treatment significantly reduced lipopolysaccha⁃ride(LPS)-induced depressive-like behaviors and neuroinflammation via inhibiting NF-κB acti⁃vation,decreasing proinflammatory cytokine levels,and normalizing redox signaling and its downstream components,including Nrf2,HO-1,and SOD2,as well as glial cell activation mark⁃ers,such as Iba-1 and GFAP.Further,ibrutinib treatment inhibited LPS-activated inflammasome activation by targeting NLRP3/P38/caspase-1 signaling.Interestingly,LPS reduced the number of dendritic spines and expression of BDNF,and synaptic-related markers,including PSD95,snap25,and synaptophysin,were improved by ibrutinib treatment in the hippocampal area of the mouse brain.CONCLUSION Ibrutinib can allevi⁃ate neuroinflammation and synaptic defects,sug⁃gesting it has antidepressant potential against LPS-induced neuroinflammation and depression.

Ibrutinib治疗慢性淋巴细胞白血病及其他B细胞恶性肿瘤

慢性淋巴细胞白血病和非霍奇金淋巴瘤等成熟B细胞肿瘤患者的存活和疾病进展依赖B细胞受体(BCR)提供的信号,而Bruton酪氨酸激酶(BTK)是BCR信号通路上的关键激酶。Ibrutinib是一种新型的BTK选择性抑制剂,对BTK具有不可逆的抑制作用,在B细胞肿瘤的初步临床试验显示了令人振奋的疗效。本文就其作用机制以及在B细胞肿瘤的研究现状进行综述。

Ibrutinib联合三氧化二砷对套细胞淋巴瘤细胞系的作用

目的:探讨Ibrutinib联合三氧化二砷(arsenic trioxide,ATO)对套细胞淋巴瘤细胞系的影响,初步研究其可能机制。方法:应用CCK-8法检测Ibrutinib联合ATO对套细胞淋巴瘤细胞系增殖的影响;流式细胞术检测Ibrutinib、ATO单药及两药联合对套细胞淋巴瘤细胞系凋亡、周期的影响;Western Blot检测周期及凋亡相关蛋白表达水平变化。结果:CCK-8结果显示两药联合对套细胞淋巴瘤细胞系增殖的抑制作用较单药更明显,两药之间具有协同作用,最佳协同浓度为Ibrutinib 5μmol/L和ATO 0.75μmol/L(P<0.001);Annexin V-PE/7AAD双染流式细胞术分析结果表明未加药对照组、5μmol/L Ibrutinib组、0.75μmol/L ATO组、联合用药组24 h细胞凋亡率为(3.0±0.81)%、(3.5±0.91)%、(4.9±0.04)%和(20.4±0.93)%(P<0.0001),48 h细胞凋亡率为(2.5±0.75)%、(3.6±1.82)%、(26.2±2.76)%和(76.4±9.33)%(P=0.003);流式细胞术检测显示5μmol/L Ibrutinib、0.75μmol/L ATO单药及两药联合能将套细胞淋巴瘤细胞周期阻滞于S期;5μmol/L Ibrutinib、0.75μmol/L ATO单药及两药联合使Caspase-3、PARP、CyclinD1、Bcl-2表达水平下调,而Cleaved caspase-3、Cleaved PARP表达水平上调,且两药联合较单药更明显。结论:Ibrutinib、ATO单药及两药联合能有效抑制套细胞淋巴瘤细胞系增殖、诱导其凋亡和细胞周期阻滞,且在一定浓度范围内两药联合有协同作用。

Ibrutinib抑制弥漫大B细胞淋巴瘤细胞生存的作用研究

目的:探讨Bruton酪氨酸激酶(Bruton's tyrosine kinase,BTK)抑制剂ibrutinib抑制弥漫大B细胞淋巴瘤(diffuse large B cell lymphoma,DLBCL)细胞生存的作用及其相关机制。方法:用不同浓度的ibrutinib处理DLBCL细胞系SUDHL-10、HBL-1和患者原代细胞,以MTT法检测细胞的增殖抑制情况;以Annexin V/PI流式细胞术和DAPI染色法检测细胞的凋亡情况;应用Western blot法检测细胞表达磷酸化BTK、AKT、ERK的变化。DLBCL细胞与MSC共培养后,体外克隆形成实验和NOD/SCID肿瘤模型小鼠检测ibrutinib在肿瘤微环境里对DLBCL细胞的抑制作用。结果:2.5μmol/L及更高浓度的ibrutinib对DLBCL细胞的增殖有明显的抑制作用,且呈剂量依赖性。1.0、2.5μmol/L ibrutinib作用于SUDHL-10细胞24 h,细胞凋亡率分别为(21.73±3.64)%和(34.71±2.36)%,高于对照组(3.55±1.89)%(P<0.05)。5、10μmol/L ibrutinib处理24 h后,DLBCL细胞系均出现核皱缩(5μmol/L)、碎裂(10μmol/L)。ibrutinib处理细胞后磷酸化BTK、AKT、ERK的表达均明显降低。ibrutinib抑制共培养时DLBCL细胞的体外克隆形成(P<0.01)及DLBCL细胞在体内的增殖生长,差异均具有统计学意义(P<0.05)。结论:ibrutinib可抑制细胞系SUDHL-10和HBL-1的增殖,诱导凋亡,其机制可能通过阻断AKT、ERK信号途径而实现;在肿瘤微环境中ibrutinib同样对DLBCL细胞具有较强的抑制生存的作用,该药物有望为DLBCL的治疗带来希望。

Wells’syndrome possibly caused by hematologic malignancy,influenza vaccination or ibrutinib:A case report

BACKGROUND Wells’ syndrome(eosinophilic cellulitis) is an uncommon eosinophilic dermatosis of uncertain pathogenesis,characterized by clinical polymorphism and suggestive but nonspecific histopathologic traits.Its course is recurrent,and response to therapy is unpredictable.In a case in which the patient has a number of potential triggers for the manifestation of Wells’ syndrome skin rash,the treating physician must decide or must make an assumption in order to establish the most likely clinical scenario.This is important for the patient’s future treatment plans.CASE SUMMARY We describe the clinical case of a 46-year-old female with chronic lymphocytic leukemia who had already received treatment for several months with ibrutinib.She was diagnosed with Wells’ syndrome 10 d after an influenza vaccination containing thimerosal.Based on the literature,the patient was treated with a course of oral steroids.Resolution of clinical symptoms and rash were observed in response to the treatment.Ibrutinib was not discontinued.CONCLUSION The etiology of Wells’ syndrome remains unknown.Clinically,it resembles bacterial cellulitis.Lack of response to antibiotic treatment should lead the physician to consider a diagnosis of Wells’ syndrome.Treating the underlying condition is important and may lead to resolution of the syndrome.However,the most common and effective treatment to limit the course of the disease are systemic steroids.

Meta-Analysis of the Efficacy and Adverse Reactions of Ibrutinib in the Treatment of Refractory/Relapsed Mantle Cell Lymphoma

Objective: Therapeutic results of relapsed/refractory mantle cell lymphoma (R/R MCL) are very disappointing at present, and there is no standard effective treatment regimen. Ibrutinib has been proved to be effective for R/R MCL, however, the sample size of these individual clinical studies was relatively small. Hence, current clinical experience in its usage is still limited. It is necessary to systematically analyze the efficacy and adverse reactions of ibrutinib in the treatment of R/R MCL. Methods: The PubMed, Cochrane Library, and Embase databases were searched using English search terms, mantle cell lymphoma, MCL, and ibrutinib;the VIP, Wanfang, and China National Knowledge Infrastructure (CNKI) databases were searched using the Chinese search terms, ibrutinib and mantle cell lymphoma. The extracted data were subjected to meta-analysis using R software to deduce the effective rate and occurrence rate of serious adverse reactions. Results: A total of 12 cohort studies were included in this analysis. The results demonstrated that ibrutinib could be an efficient therapy regimen for R/R MCL patients and the effect of combination therapy was better than that of single-drug therapy. During the treatment with ibrutinib, the adverse reactions mainly included hematological toxicity, infection, atrial fibrillation, and bleeding. Discussion: Our analysis showed ibrutinib is an optimal second-line treatment for R/R MCL, and the combination therapy is more effective than monotherapy as it was well-tolerated by the patients. Therefore, the combination of other drugs for R/R MCL should be considered for patients with poor efficacy of ibrutinib alone or relapse after treatment.

Bruton's酪氨酸激酶抑制剂Ibrutinib与B细胞肿瘤

酪氨酸激酶的过度激活导致其下游信号途径的激活,最终导致细胞的转化、增殖和抵抗细胞凋亡,促进细胞生存。因此,许多学者致力于研究一些与肿瘤细胞分化增殖相关的细胞信号传导通路的关键酶作为药物筛选靶点,证实选择性作用于特定靶点的高效新型抗癌药物Bruton's酪氨酸激酶抑制剂Ibrutinib在初步抗B细胞肿瘤临床试验中具有非常好的疗效。

Developing potent BTK^(C481S)PROTACs for ibrutinib-resistant malignant lymphoma

Ibrutinib is a first-line treatment drug for B-cell malignancies.However,resistance to ibrutinib has been reported due to BTKC481Smutation.Although PROTAC strategy is expected to overcome this clinical resistance,it has limitations such as large molecular weight and moderate bioactivity,which restrict its potential clinical application.Herein,we report a new type of potent BTKC481S-targeting PROTAC degrader.Through design,computer-assisted optimization and SAR studies,we have developed a representative BTKC481Sdegrader L6 with a much smaller molecular weight and improved solubility.Notably,L6 demonstrates better BTK degrading activity and lower IC50value in ibrutinib-resistant cell line than the first-generation BTK degrader P13I.Optimization strategy of L6 provides a general approach in the development of PROTACs targeting BTK and other proteins for future study.

伊布替尼联合维奈托克方案治疗复发难治性弥漫大B细胞淋巴瘤的临床研究

目的:探讨伊布替尼联合维奈托克治疗复发难治性弥漫大B细胞淋巴瘤(R/R DLBCL)的临床疗效,并分析影响疗效及预后的因素。方法:回顾性分析2017年8月至2022年7月本院收治的62例R/R DLBCL患者的临床资料,患者均接受伊布替尼联合维奈托克治疗,评估临床疗效及药物安全性,观察患者的临床特征对化疗近期疗效、总生存期(OS)的影响。结果:62例患者的客观缓解率(ORR)为48.39%。病变部位在结外、NCCN-IPI中高危/高危、IPI中高危/高危、进展或复发时间<12个月是影响R/R DLBCL患者化疗近期疗效的危险因素(均P<0.05)。最常见的毒副作用为中性粒细胞减少(75.19%),其中Ⅲ-Ⅳ级中性粒细胞减少的发生率高达52.71%。62例患者1年和2年OS率分别为48.51%和31.56%,中位OS时间为12个月。多因素分析结果显示,化疗后客观缓解[HR=0.080(95%CI:0.028-0.235)]是R/R DLBCL患者OS的保护性因素,NCCN-IPI中高危/高危[HR=4.828(95%CI:1.546-15.080)]是影响R/R DLBCL患者预后的独立危险因素。结论:伊布替尼联合维奈托克可作为R/R DLBCL的有效治疗方案,NCCNIPI可作为预后的评价指标,化疗后客观缓解能使患者获得更好的OS。

达沙替尼体外抑制慢性淋巴细胞白血病增殖及BTKC481S功能

目的探讨达沙替尼(BMS-354825)体外对慢性淋巴细胞白血病(chronic lymphocytic leukemia,CLL)细胞系增殖及野生型/耐药突变型布鲁顿激酶(BTK)活化及功能的影响。方法观察不同浓度的达沙替尼对CLL细胞系的增殖抑制作用。采用不同浓度的达沙替尼及伊布替尼处理外源性表达野生型BTK及常见突变子BTKC481S、BTKT474F及BTKT474I/C481S的细胞系,Western blot检测BTK及其下游靶点PLCγ2的磷酸化水平。结果达沙替尼能显著抑制CLL细胞系MEC-1及JVM3细胞的增殖,且呈剂量依赖性,IC50分别为3.54μmol/L及0.65μmol/L;0.5μmol/L的伊布替尼及0.2μmol/L的达沙替尼可抑制野生型BTK及PLCγ2的磷酸化活化。当BCR信号激活后,BTKC481S、BTKT474F及BTKT474I/C481S均可功能性激活并磷酸化活化下游PLCγ2,这些突变子均对生理浓度的伊布替尼耐药。0.5μmol/L的达沙替尼体外可抑制BTKC481S活化并进而抑制PLCγ2活化,但不能抑制BTKT474F及BTKT474I/C481S的活化,提示沙替尼体可克服BTKC481S导致的耐药而对“守门员”位点突变无效。结论达沙替尼可抑制野生型BTK及BTKC481S激酶活化及功能并抑制CLL细胞增殖,有望解决BTKC481S引发的伊布替尼耐药。

依鲁替尼纳米晶的制备工艺研究

为改善依鲁替尼(IBR)的水溶性和溶出度,采用湿法介质研磨法制备了依鲁替尼纳米晶(IBR-NC),采用单因素实验优化了IBR-NC的制备工艺,并通过粒径分析、扫描电镜(SEM)、X-射线粉末衍射(XRPD)分析、差示扫描量热(DSC)分析及溶出度实验对IBR-NC的质量进行了评价。结果表明,以PVP-K30-SDS为稳定剂,在物料比(IBR、PVP-K30、SDS的质量比)为10∶4∶1、IBR用量为120 mg、氧化锆珠规格为0.3 mm、氧化锆珠用量为40 g、研磨转速为150 r·min^(-1)、研磨时间为2.0 h的最优条件下,制备的IBR-NC的粒径为(224.7±5.7)nm、PDI为0.151±0.017,累积溶出率在10 min能达到99.49%,溶出效果良好,且放置90 d后依然具有良好的溶出性质。

伊布替尼治疗慢性淋巴细胞白血病引起急性肾损伤不良反应1例

目的探讨伊布替尼致急性肾损伤的临床特征和处置措施。方法以1例伊布替尼治疗慢性淋巴细胞白血病引起急性肾损伤不良反应为切入点,检索FAERS数据库和查阅文献,分析其临床特征和处置措施。结果数据显示,伊布替尼引起急性肾损伤的发生率很低,表现为血清肌酐水平升高,可合并蛋白尿、血尿,肾活检显示为急性间质性肾炎或急性肾小管坏死。及时停药、经糖皮质激素等免疫抑制治疗后,部分患者血清肌酐水平可有所恢复。结论临床医生应权衡利弊,密切监测患者血肌酐,保障患者用药安全。

苯丁酸氮芥联合伊布替尼对套细胞淋巴瘤Jeko-1细胞株的作用及相关机制

目的:探讨苯丁酸氮芥联合伊布替尼对套细胞淋巴瘤Jeko-1细胞株的抑制作用及相关机制。方法:分别将不同浓度的苯丁酸氮芥、伊布替尼单药及两药联合作用于Jeko-1细胞株,采用CCK-8检测细胞增殖情况,同时采用Western blot检测细胞中BCL-2、caspase-3、PI3K、AKT、P-AKT蛋白表达的变化。结果:分别用苯丁酸氮芥(3.125、6.25、12.5、25、50μmol/L)及伊布替尼(3.125、6.25、12.5、25、50μmol/L)单药处理Jeko-1细胞株24、48和72 h后,细胞增殖均受到抑制,且抑制作用呈时间及剂量依赖性,两药联合时抑制作用更明显(均P<0.05)。与对照组相比,苯丁酸氮芥(3.125、6.25、12.5、25、50μmol/L)及伊布替尼(3.125、6.25、12.5、25、50μmol/L)单药组细胞凋亡率增加,呈剂量依赖性;与相应剂量(3.125、6.25、12.5μmol/L)单药组比较,两药联合应用组Jeko-1细胞株的凋亡率明显增加(均P<0.05)。与单药组相比,两药联合时可产生协同作用,Jeko-1细胞的caspase-3表达明显增强,BCL-2、PI3K、p-AKT/AKT表达明显减弱(均P<0.05)。结论:苯丁酸氮芥及伊布替尼能够促进套细胞淋巴瘤Jeko-1细胞株的凋亡,两药联合应用可以产生协同作用,其主要是通过AKT相关信号通路发挥作用。

新型2,4-二羟基蝶啶类衍生物的合成及其抗肿瘤活性

蝶啶类化合物的抗肿瘤活性是研究最多,也是最具有治疗潜力的一类化合物。以Ibrutinib为先导化合物,以4-氨基-2,6-二羟基嘧啶为原料出发,经过多步首次合成了新型2,4-二羟基蝶啶类衍生物,并对其进行了^(1)H NMR、^(13)C NMR和MS(ESI)的表征。选用A549细胞做了抗肿瘤实验,结果表明:化合物5h,5j和6o在低浓度下表现出小于10%的抑制率,在高浓度下均有大于20%的抑制率,说明5h,5j和6o对A549细胞有一定的抑制效果。

中医药治疗慢性淋巴细胞白血病及伊布替尼不良反应个案报道

回顾性分析北京中医药大学东直门医院收治的1例伊布替尼治疗慢性淋巴细胞白血病致肺部感染患者的临床资料,并复习相关文献。该患者在服用伊布替尼治疗时并发肺部感染,遂停药,结合中医药治疗后感染症状得到控制,后继续坚持口服中药治疗,慢性淋巴细胞白血病的相关症状得到改善,且未再发生感染。针对长时间应用伊布替尼治疗慢性淋巴细胞白血病的患者,需警惕肺部真菌感染的发生。中医药在治疗慢性淋巴细胞白血病中,能够防止各类感染的发生,提高机体耐受力,延长患者生存期。

BTK抑制剂治疗不同类型B细胞淋巴瘤疗效的回顾分析

目的比较不同Bruton酪氨酸激酶(BTK)抑制剂对各类B细胞淋巴瘤的疗效,为优化治疗方案提供参考。方法收集B细胞淋巴瘤患者的PET/CT、肿瘤标志物检测、不良反应、用药方案等临床资料,按淋巴瘤类别和不同用药方案分组,比较使用伊布替尼、泽布替尼和奥布替尼对慢性淋巴细胞白血病/小淋巴细胞淋巴瘤(CLL/SLL)、弥漫大B细胞淋巴瘤(DLBCL)、套细胞淋巴瘤(MCL)的疗效和各种不良反应的发生率。结果治疗CLL/SLL,奥布替尼客观缓解率(ORR)为70.59%,泽布替尼ORR为64.52%,伊布替尼ORR为45.00%;对于DLBCL,纳入研究的治疗方案为BTK抑制剂联合R+CHOP方案,奥布替尼ORR为54.55%、泽布替尼ORR为47.62%、伊布替尼ORR为41.67%;对于MCL,泽布替尼ORR高达81.82%,奥布替尼ORR为71.43%,伊布替尼ORR为62.50%。3种BTK抑制剂均可降低β2微球蛋白(β2-MG)的水平,其中奥布替尼可显著降低CLL/SLL、DLBCL、MCL患者血清中β2-MG的含量(P<0.05)。在不良反应方面,使用奥布替尼治疗CLL/SLL、DLBCL、MCL患者腹泻、呼吸道感染、肌肉酸痛发生率均为最低。其中MCL患者中奥布替尼腹泻发生率最低且经比较,差异有统计学意义(P<0.05)。三种BTK抑制剂中性粒细胞减少、血小板减少和贫血的发生率在同病种组内比较,差异均无统计学意义(P>0.05)。结论奥布替尼治疗CLL/SLL疗效最高,泽布替尼治疗MCL疗效最高,3种BTK抑制剂联合R+CHOP方案治疗DLBCL疗效相近,其中奥布替尼略高。综合比较各项不良反应发生率,奥布替尼安全性最好。