Bruton’s tyrosine kinase inhibitors in primary central nervous system lymphoma:New hopes on the horizon

In this editorial,we comment on the article by Wang et al.This manuscript explores the potential synergistic effects of combining zanubrutinib,a novel oral inhibitor of Bruton’s tyrosine kinase,with high-dose methotrexate(HD-MTX)as a therapeutic intervention for primary central nervous system lymphoma(PCNSL).The study involves a retrospective analysis of 19 PCNSL patients,highlighting clinicopathological characteristics,treatment outcomes,and genomic biomarkers.The results indicate the combination’s good tolerance and strong antitumor activity,with an 84.2%overall response rate.The authors emphasize the potential of zanubrutinib to modulate key genomic features of PCNSL,particularly mutations in myeloid differentiation primary response 88 and cluster of differentiation 79B.Furthermore,the study investigates the role of circulating tumor DNA in cerebrospinal fluid for disease surveillance and treatment response monitoring.In essence,the study provides valuable insights into the potential of combining zanubrutinib with HD-MTX as a frontline therapeutic regimen for PCNSL.The findings underscore the importance of exploring alternative treatment modalities and monitoring genomic and liquid biopsy markers to optimize patient outcomes.While the findings suggest promise,the study’s limitations should be considered,and further research is needed to establish the clinical relevance of this therapeutic approach for PCNSL.

Novel deletion mutation in Bruton’s tyrosine kinase results in X-linked agammaglobulinemia:A case report

BACKGROUND X-linked agammaglobulinemia is a primary immunodeficiency disease caused by gene mutations of Bruton’s tyrosine kinase(BTK).We found a new mutation point and summarized the correlation analysis and performed a literature review.CASE SUMMARY The proband was a 5-year-old boy.He was admitted to our hospital due to a recurrent cough and a fever that had persisted for a month.He had a history of multiple respiratory infections and sinusitis.There was no immunodeficiency or recurrent infection history among his family members.Agammaglobulinemia was characterized as follows:Immunoglobulin(Ig)A,90.0 mg/dL(90-450 mg/dL);IgG,20.0 mg/dL(800-1800 mg/dL);and IgM,18.0 mg/dL(60-280 mg/dL).Notably,the assessment of IgG subtypes revealed the following very low levels:Subtype 1,0.26 g/L(3.62-12.28 g/L);subtype 2,0.10 g/L(0.57-2.9 g/L);subtype 3,0.009 g/L(0.129-0.789 g/L);and subtype 4,0.003 g/L(0.013-1.446 g/L).Cellular immunological test results were as follows:CD3,74.6%(50%-84.0%);CD4,47.3%(27.0%-51.0%);and CD8,24.9%(15.0%-44.0%).A de novo hemizygous deletion in BTK was detected:c.902_c.904delAAG/p.E301del.Transcript levels of the mutant BTK were similar to those of the wild-type gene,though overexpression resulted in markedly reduced levels of mutant BTK(9.49%±1.58%),relative to the wildtype BTK(75.8%±2.98%,P<0.01).CONCLUSION This case of X-linked agammaglobulinemia was attributed to a de novo hemizygous deletion mutation in BTK(c.902_c.904delAAG/p.E301del).The mutation resulted in markedly reduced BTK protein stability in vitro.

Navigating the complex terrain of hepatitis B virus reactivation in the era of Bruton tyrosine kinase inhibitors

In this editorial,we offer a summary of the risk associated with hepatitis B reactivation(HBVr)in the setting of both solid and hematologic malignancies treated with Bruton tyrosine kinase(BTK)inhibitors,with insights derived from current studies.Furthermore,we emphasize the critical need for a framework regarding robust risk evaluation in patients undergoing such treatments.This framework is essential for identifying those at increased risk of HBVr,enabling healthcare providers to implement proactive measures to prevent reactivation and ensure the safe administration of BTK inhibitor therapy.

Rituximab combined with Bruton tyrosine kinase inhibitor to treat elderly diffuse large B-cell lymphoma patients: Two case reports

BACKGROUND Diffuse large B-cell lymphoma(DLBCL)is a common aggressive non-Hodgkin's lymphoma(NHL),accounting for 30%-40%of adult NHLs.This report aims to explore the efficacy and safety of rituximab combined with Bruton tyrosine kinase inhibitors(BTKis)in the treatment of elderly patients with DLBCL.CASE SUMMARY The clinical data of two elderly patients with DLBCL who received rituximab combined with BTKi in our hospital were retrospectively analyzed,and the literature was reviewed.The patients were treated with chemotherapy using the R-miniCHOP regimen for two courses.Then,they received rituximab in combination with BTKi.CONCLUSION The treatment experience in these cases demonstrates the potential efficacy of rituximab combined with BTKi to treat elderly DLBCL patients,thus providing a new treatment strategy.

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。

Risk of hepatic decompensation from hepatitis B virus reactivation in hematological malignancy treatments

In this editorial,we discussed the apparent discrepancy between the findings described by Colapietro et al,in their case report and data found in the literature.Colapietro et al reported a case of hepatitis B virus(HBV)-related hepatic decompensation in a patient with chronic myeloid leukemia and a previously resolved HBV infection who was receiving Bruton’s tyrosine kinase(BTK)inhibitor therapy.First of all,we recapitulated the main aspects of the immune system involved in the response to HBV infection in order to underline the role of the innate and adaptive response,focusing our attention on the protective role of anti-HBs.We then carefully analyzed literature data on the risk of HBV reactivation(HBVr)in patients with previous HBV infection who were treated with either tyrosine kinase inhibitors or BTK inhibitors for their hematologic malignancies.Based on literature data,we suggested that several factors may contribute to the different risks of HBVr:The type of hematologic malignancy;the type of therapy(BTK inhibitors,especially second-generation,seem to be at a higher risk of HBVr than those with tyrosine kinase inhibitors);previous exposure to an anti-CD20 as first-line therapy;and ethnicity and HBV genotype.Therefore,the warning regarding HBVr in the specific setting of patients with hematologic malignancies requires further investigation.

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.

Prevention and management of hepatitis B virus reactivation in patients with hematological malignancies in the targeted therapy era

Hepatitis due to hepatitis B virus(HBV)reactivation can be serious and potentially fatal,but is preventable.HBV reactivation is most commonly reported in patients receiving chemotherapy,especially rituximab-containing therapy for hematological malignancies and those receiving stem cell transplantation.Patients with inactive and even resolved HBV infection still have persistence of HBV genomes in the liver.The expression of these silent genomes is controlled by the immune system.Suppression or ablation of immune cells,most importantly B cells,may lead to reactivation of seemingly resolved HBV infection.Thus,all patients with hematological malignancies receiving anticancer therapy should be screened for active or resolved HBV infection by blood tests for hepatitis B surface antigen(HBsAg)and antibody to hepatitis B core antigen.Patients found to be positive for HBsAg should be given prophylactic antiviral therapy.For patients with resolved HBV infection,there are two approaches.The first is pre-emptive therapy guided by serial HBV DNA monitoring,and treatment with antiviral therapy as soon as HBV DNA becomes detectable.The second approach is prophy-lactic antiviral therapy,particularly for patients receiving high-risk therapy,especially anti-CD20 monoclonal antibody or hematopoietic stem cell transplantation.Entecavir and tenofovir are the preferred antiviral choices.Many new effective therapies for hematological malignancies have been introduced in the past decade,for example,chimeric antigen receptor(CAR)-T cell therapy,novel monoclonal antibodies,bispecific antibody drug conjugates,and small molecule inhibitors,which may be associated with HBV reactivation.Although there is limited evidence to guide the optimal preventive measures,we recommend antivi-ral prophylaxis in HBsAg-positive patients receiving novel treatments,including Bruton’s tyrosine kinase inhibitors,B-cell lymphoma 2 inhibitors,and CAR-T cell therapy.Further studies are needed to determine the risk of HBV reactivation with these agents and the best prophylactic strategy.

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。

BTK及其相关炎症因子在AIS患者中的变化及作用探讨

目的探讨急性脑梗死(AIS)后布鲁顿酪氨酸溶酶(BTK)及其相关炎症因子的变化及作用。方法2020年10月至2022年3月在河北医科大学第二医院神经内科住院的58例AIS患者,另随机选取25例健康志愿者作为对照组,收集人口学、既往史、NIHSS评分等资料,比较两组BTK、核因子-κB(NF-κB)、白细胞介素(IL-β)、IL-6和肿瘤坏死因子(TNF-α)水平,分析BTK与NF-κB、NIHSS评分、AIS体积的相关性。结果AIS组BTK、NF-κB明显高于对照组,差异有统计学意义(P<0.01),IL-β、IL-6和TNF-α与对照组相比升高不明显(P>0.05)。BTK与NF-κB(r=0.828 P<0.01)、AIS体积(r=0.647 P<0.01)以及NIHSS(r=0.498 P<0.01)存在正相关关系。结论AIS患者BTK较健康人明显升高,且与NF-κB、NIHSS评分和AIS体积相关,BTK可能是AIS治疗潜在靶点。

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.

Bruton酪氨酸激酶Btk的生物学特性研究进展

酪氨酸激酶Btk是非受体酪氨酸家族的成员,它由PH结构域、TH结构域、SH3结构域、SH2结构域和催化结构域5部分组成.Btk参与多种信号通路,对细胞的增殖、分化和凋亡起着重要的调控作用.Btk的突变可导致X连锁无丙种球蛋白血症,一直以来都是研究热点.笔者将围绕Btk的结构、功能、X连锁无丙种球蛋白血症的临床表现等方面的内容加以综述,着重探讨Btk参与B细胞信号通路、TLR信号通路和肥大细胞脱颗粒等过程的具体机制.

布鲁顿氏酪氨酸激酶抑制剂治疗原发中枢神经系统淋巴瘤16例临床分析

目的:分析应用布鲁顿氏酪氨酸激酶(BTK)抑制剂治疗原发中枢神经系统淋巴瘤(PCNSL)患者的临床特征,探讨影响疗效的因素及疗效不佳患者的后续治疗经验。方法:回顾性分析初诊应用BTK抑制剂(包括奥布替尼、泽布替尼)联合传统化疗诱导治疗的PCNSL患者的临床资料。结果:16例PCNSL患者中,男性13例,女性3例,中位年龄62.5岁。病灶数目以多发为主,占56%;病理分型以非生发中心B细胞(non-GCB)型为主,占62%;双表达型占38%;9例患者有初诊脑脊液生化数据,脑脊液蛋白升高者占78%;7例患者有基因测序结果,MYD88突变占57%,CD79B突变占43%;16例患者中9例(56%)接受奥布替尼联合传统化疗治疗,7例(44%)接受泽布替尼联合传统化疗治疗;16例患者的总体反应率(ORR)为69%。5例疗效不佳的患者中,4例为多发病灶,4例为双表达类型,3例具有MYD88突变;2例接受造血干细胞移植序贯嵌合抗原受体T细胞治疗(auto-HSCT+CAR-T),获得完全缓解。结论:BTK抑制剂联合传统化疗治疗PCNSL患者的ORR为69%,多发病灶、双表达、MYD88突变可能是疗效差的因素。auto-HSCT+CAR-T可能是BTK抑制剂联合传统化疗治疗PCNSL疗效不佳患者可行的后续治疗方案。

慢性淋巴细胞白血病BTKi治疗后免疫功能重建研究

目的:分析慢性淋巴细胞白血病(CLL)经布鲁顿酪氨酸激酶抑制剂(BTKi)治疗后的免疫功能重建情况。方法:收集2017年1月至2022年3月在福建医科大学附属协和医院血液科就诊的59例CLL患者的病历信息,对其诊断、治疗和实验室检查资料进行回顾性分析研究。结果:59例CLL患者中位年龄为60.5(36-78)岁;BTKi治疗1年后,51例(86.4%)的CLL肿瘤克隆(CD5+/CD19+)明显缩小,治疗前后分别为(46±6.1)×10^(9)/L和(2.3±0.4)×10^(9)/L(P=0.0013),而非肿瘤克隆(CD19+减去CD5+/CD19+)无明显变化;免疫球蛋白IgA明显升高,治疗前后分别为(0.75±0.09)g/L和(1.31±0.1)g/L(P<0.001),但IgG和IgM下降,分别为(8.1±0.2)g/L和(7.1±0.1)g/L(P<0.001)、(0.52±0.6)g/L和(0.47±0.1)g/L(P=0.002)。BTKi治疗前后CLL患者的T细胞亚群出现明显变化,表现为总T细胞数从(2.1±0.1)×10^(9)/L减少至(1.6±0.4)×10^(9)/L(P=0.042),CD4+细胞数从(0.15±6.1)×10^(9)/L增加至(0.19±0.4)×10^(9)/L(P<0.001),CD8+细胞数从(0.27±0.01)×10^(9)/L增加至(0.41±0.08)×10^(9)/L(P<0.001),NK/T细胞数从(0.11±0.1)×10^(9)/L下降至(0.07±0.01)×10^(9)/L(P=0.038);白细胞介素(IL)-2表达上调、IL-4和干扰素γ表达下降,但IL-6、IL-10、肿瘤坏死因子α表达变化不大;TCR和BCR组库多样性都得到恢复,完全缓解患者比部分缓解患者恢复更明显,完全缓解患者BTKi治疗前后TCR组库香农指数分别为0.02±0.008和0.14±0.01(P<0.001),部分缓解患者分别为0.01±0.03和0.05±0.02(P>0.05),而BCR组库香农指数分别是0.19±0.003和0.33±0.15(P<0.001)、0.15±0.009和0.23±0.18(P<0.05)。结论:BTKi治疗可以缩小CLL克隆,促进IgA表达,增加功能性T细胞数量,调节IL-2、IL-4、干扰素γ等分泌,改善肿瘤微环境的免疫调节状态;BTKi治疗还能促进TCR和BCR免疫组库多样性的恢复。BTKi治疗有助于CLL患者的免疫功能重建。

Bruton酪氨酸激酶在对乙酰氨基酚诱导的小鼠肝损伤中变化及意义

目的观察对乙酰氨基酚(APAP)诱导的小鼠急性肝损伤中Bruton酪氨酸激酶(Btk)、磷酸化Btk(p-Btk)、核因子κB(NF-κB)、核苷酸结合寡聚域样受体蛋白3(NLRP3)、白细胞介素1β(IL-1β)、肿瘤坏死因子-α(TNF-α)的动态变化,初步探讨Btk在APAP诱导的急性肝损伤中的作用。方法随机将54只小鼠分为9组,分别为对照组、APAP 0.5 h组、APAP 1 h组、APAP 3 h组、APAP 6 h组、APAP 12 h组、APAP 24 h组、APAP 36 h组、APAP 48 h组,每组6只。禁食12 h后,单次腹腔注射APAP(300 mg/kg)0.5、1、3、6、12、24、36、48 h后处死相应组别的小鼠。测定各组血清丙氨酸氨基转移酶(ALT)、天门冬氨酸氨基转移酶(AST);观察各组肝脏病理变化;ELSIA测定各组肝组织匀浆中IL-1β和TNF-α;Western blot测定肝组织中Btk、p-Btk、NF-κB及NLRP3表达。结果与对照组比较,APAP干预后的各组血清ALT(F=100.968,P=0.000)、AST(F=73.539,P=0.000)、肝脏坏死程度(F=29.845,P=0.000)、肝脏Btk(F=441.280,P=0.000)、p-Btk(F=1323.022,P=0.000)、NF-κB(F=133.125,P=0.000)及NLRP3水平(F=820.095,P=0.000)、IL-1β(F=8.643,P=0.000)、TNF-α(F=20.545,P=0.000)含量均有变化,其中24 h的各种指标最高。结论单次腹腔注射APAP诱导的小鼠肝损伤呈现动态变化,其病理机制可能与其激活Btk,导致NLRP3形成、NF-κB激活及炎症因子升高有关。

复发/难治DLBCL患者继发CNS侵犯的临床特征及泽布替尼联合化疗方案的疗效

目的分析4例继发中枢神经系统(CNS)侵犯的复发/难治弥漫大B细胞淋巴瘤(DLBCL)患者的临床特征,并观察泽布替尼联合化疗方案的疗效。方法选择4例DLBCL继发CNS侵犯患者,分析其初诊及复发时的临床特征;并进行相应泽布替尼联合化疗方案治疗,其中,2例采用泽布替尼+甲氨蝶呤(Z-MTX)方案治疗,1例采用泽布替尼+利妥昔单抗+吉西他滨+顺铂+地塞米松(Z-R-GDP)方案治疗,1例采用泽布替尼+利妥昔单抗+甲氨蝶呤(ZR-MTX)方案治疗,评价治疗方案的疗效及毒性反应。结果4例患者中,3例CNS复发仅侵犯脑实质,另1例同时侵犯脑、眼;3例具有淋巴瘤中枢侵袭的高危中枢神经系统国际预后指数(CNS-IPI)评分(4~6分),另1例CNS-IPI评分1分。3例患者为非生发中心(non-GCB)来源,其中MCD亚型2例、非MCD亚型1例;1例未进行相关分子生物学检查。化疗后完全缓解3例,部分缓解1例;随访4~5个月,至末次随访,3例完全缓解患者疗效持续缓解无复发,1例部分缓解患者复发。主要毒性反应为血液学毒性,未发生肿瘤溶解、心房颤动或高血压等其他3级及以上布鲁顿氏酪氨酸激酶选择性抑制剂相关的毒性反应。结论复发/难治DLBCL继发CNS侵犯多为non-GCB来源及MCD亚型,主要侵犯脑实质;泽布替尼联合化疗方案有显著、持续的疗效和生存优势,其主要毒性反应可控。

新型布鲁顿氏酪氨酸激酶蛋白水解靶向嵌合体(BTK PROTAC)的设计合成及活性评价

目的 设计合成新型布鲁顿氏酪氨酸激酶蛋白水解靶向嵌合体(BTK PROTAC),并在体外评估这些分子对BTK蛋白的降解活性。方法 以Nurix Therapeutics公司临床化合物NX-5948为先导化合物,分析其与靶蛋白的相互作用,通过引入并环代替吡嗪胺的骨架跃迁思路对其进行结构改造,成功合成了一系列新型BTK PROTACs,通过时间分辨荧光共振能量转移技术(TR-FRET)、MTS法和蛋白质免疫印迹法分别测定目标化合物的激酶活性、细胞增殖抑制活性和BTK蛋白降解活性。结果 共合成6个目标化合物(化合物B~G),活性测试结果显示,大部分化合物都具有优异的细胞增殖抑制活性和BTK降解活性,其中化合物B表现出较优的BTK蛋白降解能力,其半数最大降解浓度(DC_(50))值约为0.1 nmol·L^(-1)。结论 基于NX-5948,通过骨架跃迁的方法设计合成了一类新颖的BTK PROTAC化合物,进行了构效关系的初步探索,可为BTK PROTAC降解剂的进一步研究提供参考。

Bruton酪氨酸蛋白激酶在创伤性休克诱发的全身炎症反应中研究与思考

Bruton酪氨酸蛋白激酶（Bruton tyrosine kinase,Btk）是非受体酪氨酸蛋白激酶Tec家族成员之一,是Toll样受体（Toll-like receptors,TLRs）信号通路的一个重要信号分子,但其在体内炎症反应中的作用仍知之甚少。由于TLRs信号通路在创伤后全身炎症反应综合征（systemic inflammatory response syndrome,SIRS）和多器官功能障碍综合征的发生发展过程中具有重要作用。

布鲁顿酪氨酸激酶抑制剂治疗套细胞淋巴瘤有效性及安全性的meta分析

目的 系统分析布鲁顿酪氨酸激酶抑制剂(Bruton’s tyrosine kinase inhibitor, BTKi)治疗套细胞淋巴瘤(mantle cell lymphoma, MCL)的有效性及安全性。方法 选取建库至2023年5月21日PubMed、Embase、The Cochrane Library、Clinical Trials.gov和Web of Science等数据库公开发表的BTKi治疗MCL的英文文献,由2位研究者独立筛选文献、提取资料并评价纳入研究的偏倚风险后,以总反应率(overall response rate, ORR)及治疗相关不良反应(adverse events, AEs)发生率作为结局指标,分析BTKi治疗MCL的有效性及安全性。结果 共检索文献4 818篇,最终纳入15篇,其中随机对照研究2篇,单臂研究13篇,共16项研究,涉及1 029例患者。Meta分析结果显示,BTKi治疗MCL的ORR为83.7%(95%CI:76.7%~89.8%)。亚组分析各因素合并反应率:低龄组(<65岁)为91.4%(95%CI:70.6%~100.0%),高龄组为(≥65岁)80.7%(95%CI:76.0%~85.0%);初治组为94.5%(95%CI:81.0%~100.0%),复发/难治组为79.0%(95%CI:75.3%~82.5%);BTKi联合治疗组为86.5%(95%CI:74.7%~95.3%),BTKi单药治疗组为79.0%(95%CI:74.4%~83.3%);第一代BTKi组为74.9%(95%CI:65.7%~83.2%),第二代BTKi组为81.7%(95%CI:77.4%~85.7%);IR方案(伊布替尼+利妥昔单抗)组为93.2%(95%CI:80.0%~99.9%),非IR方案组为77.4%(95%CI:69.6%~84.4%)。安全性方面共分析了8种不良反应,血液系统不良反应中血小板减少症(29.8%,95%CI:18.9%~42.0%)的发生率较高,非血液系统中疲劳(53.6%,95%CI:35.4%~71.4%)和腹泻(48.1%,95%CI:35.1%~61.2%)的发生率较高。结论 BTKi治疗MCL具有较好的有效性及安全性,年龄<65岁、疾病状态为初治、BTKi联合治疗、第二代BTKi单药治疗、联合治疗IR方案均有较高的反应率。

8例非Bruton酪氨酸激酶基因突变无丙种球蛋白血症患儿临床特征和基因突变/多态性分析

目的分析8例非Bruton酪氨酸激酶(BTK)基因突变无丙种球蛋白血症患儿的临床特征和基因突变/多态性特点。方法以2005年1月至2010年12月于上海交通大学医学院附属上海儿童医学中心诊断为无丙种球蛋白血症但BTK基因未检测出突变的患儿为研究对象,分析其临床资料和实验室结果。Sanger法检测其常见致病基因,包括IGHM、IGLL1、CD79a和CD79b。结果共纳入8例患儿,男女比例为3:1,平均发病年龄(3.7±2.4)岁。所有患儿均有反复感染史,其中最为常见的是肺炎和上呼吸道感染。1例患儿检测出IGLL1基因突变,其他致病基因未明。结论非BTK基因突变无丙种球蛋白血症患儿常见呼吸系统感染,可通过基因分析进行确诊。