Synchronous diagnosis and treatment of acute myeloid leukemia and chronic lymphocytic leukemia:Two case reports

BACKGROUND The concurrence of acute myeloid leukemia(AML)and chronic lymphocytic leukemia(CLL)is rare.Previous reports of such cases have focused mainly on clinical diagnosis and characteristics,so the mechanism remains unclear,and therapy options have been poorly explored.CASE SUMMARY Here,we report two cases of synchronous AML and CLL.Flow cytometry revealed two distinct abnormal cell populations(myeloblasts and lymphoid cells)according to scatter characteristics.CD5-positive B cell lymphoma with myeloid leukemia invasion was observed on lymph node biopsy.Chemotherapy regimens indicated for both AML and CLL were used in our patients,and our patients achieved complete response after chemotherapy.Next-generation sequencing of 88 genes was performed.CONCLUSION We conclude that early mutation and dysregulation at the hematopoietic stem cell stage and the accumulation of multiple rearrangements may cause the concurrence of CLL and AML.The treatment of infection and combination therapy aimed at the CLL component are significant in the management of patients with concurrent CLL and AML.

Prognostic Significance of Apoptosis Regulators in B-Cell Chronic Lymphocytic Leukemia

Background: High levels of MCL-1 and BCL-2 proteins have been found in Chronic Lymphocytic Leukemia (CLL), and inversely correlated with response to treatment. BCL-2/Bax ratio is the main director of apoptosis in CLL. The study aimed to clarify the prognostic role of MCL-1, BCL-2 and BCL-2/ Bax ratio in B-CLL. Patients & method: Estimation of MCL-1, BCL-2 and Bax expressions by a flow cytometry in 45 B-CLL patients and the prognostic value of these markers were correlated with other well-known established prognostic markers and treatment response. Results: MCL-1 was expressed in 60% of cases while BCL-2 was expressed in 82.2% of cases. MCL-1 expression was significantly high in male gender, short lymphocyte doubling time (LDT), and high expression of CD 38 (p β2M, CD38 expression), low ZAP-70 expression, splenomegaly and higher Rai stage were significantly increased in patients with high expression of BCL-2 (p β2M, high C-D38 expression, low ZAP-70 expression, the poor cytogenetic and splenomegaly in patients with high expression of BCL-2/ Bax ratio (p In conclusion: MCL-1, BCL-2 expressions and BCL-2/Bax ratio could be useful potential predictive and prognostic markers in B-CLL.

Stationary distribution and extinction for a stochastic two-compartment model of B-cell chronic lymphocytic leukemia

In this paper,we study the dynamical behavior of a stochastic two-compartment model of B-cell chronic lymphocytic leukemia,which is perturbed by white noise.Firstly,by constructing suitable Lyapunov functions,we establish sufficient conditions for the existence of a unique ergodic stationary distribution.Then,conditions for extinction of the disease are derived.Furthermore,numerical simulations are presented for supporting the theoretical results.Our results show that large noise intensity may contribute to extinction of the disease.

TOSO interacts with SYK and enhances BCR pathway activation in chronic lymphocytic leukemia

Background:TOSO,also named Fas inhibitory molecule 3(FAIM3),has recently been identified as an immunoglobulin M(IgM)Fc receptor(FcμR).Previous studies have shown that TOSO is specifically over-expressed in chronic lymphocytic leukemia(CLL).However,the functions of TOSO in CLL remain unknown.The B-cell receptor(BCR)signaling pathway has been reported to be constitutively activated in CLL.Here,we aimed to investigate the functions of TOSO in the BCR signaling pathway and the pathogenesis of CLL.Methods:We over-expressed TOSO in B-cell lymphoma cell lines(Granta-519 and Z138)by lentiviral transduction and knocked down TOSO by siRNA in primary CLL cells.The over-expression and knockdown of TOSO were confirmed at the RNA level by polymerase chain reaction and protein level by Western blotting.Co-immunoprecipitation with TOSO antibody followed by liquid chromatography coupled with tandem mass spectrometry(IP/LCMS)was used to identify TOSO interacting proteins.Western blotting was performed to detect the activation status of BCR signaling pathways as well as B-cell lymphoma 2(BCL-2).Flow cytometry was used to examine the apoptosis of TOSO-over-expressing B lymphoma cell lines and TOSO-down-regulated CLL cells via the staining of Annexin V and 7-AAD.One-way analyses of variance were used for intergroup comparisons,while independent samples t tests were used for two-sample comparisons.Results:From IP/LCMS,we identified spleen tyrosine kinase(SYK)as a crucial candidate of TOSO-interacting protein and confirmed it by co-immunoprecipitation.After stimulation with anti-IgM,TOSO over-expression increased the phosphorylation of SYK,and subsequently activated the BCR signaling pathway,which could be reversed by a SYK inhibitor.TOSO knockdown in primary CLL cells resulted in reduced SYK phosphorylation as well as attenuated BCR signaling pathway.The apoptosis rates of the Granta-519 and Z138 cells expressing TOSO were(8.46±2.90)%and(4.20±1.21)%,respectively,significantly lower than the rates of the control groups,which were(25.20±4.60)%and(19.72±1.10)%,respectively(P<0.05 for both).The apoptosis rate was reduced after knocking down TOSO in the primary CLL cells.In addition,we also found that TOSO down-regulation in primary cells from CLL patients led to decreased expression of BCL-2 as well as lower apoptosis,and vice versa in the cell line.Conclusions:TOSO might be involved in the pathogenesis of CLL by interacting with SYK,enhancing the BCR signaling pathway,and inducing apoptosis resistance.

Promises and pitfalls of targeted agents in chronic lymphocytic leukemia

Targeted agents have significantly improved outcomes for patients with chronic lymphocytic leukemia,particularly high-risk subgroups for whom chemoimmunotherapy previously offered limited efficacy.Two classes of agent in particular,the Bruton tyrosine kinase inhibitors(e.g.,ibrutinib)and the B-cell lymphoma 2 inhibitor,venetoclax,induce high response rates and durable remissions in the relapsed/refractory and frontline settings.However,maturing clinical data have revealed promises and pitfalls for both agents.These drugs induce remissions and disease control in the majority of patients,often in situations where modest efficacy would be expected with traditional chemoimmunotherapy approaches.Unfortunately,in the relapsed and refractory setting,both agents appear to be associated with an inevitable risk of disease relapse and progression.Emerging patterns of resistance are being described for both agents but a common theme appears to be multiple sub-clonal drivers of disease progression.Understanding these mechanisms and developing effective and safe methods to circumvent the emergence of resistance will determine the longer-term utility of these agents to improve patients’quality and length of life.Rational drug combinations,optimised scheduling and sequencing of therapy will likely hold the key to achieving these important goals.

Modulation of B-cell receptor and microenvironment signaling by a guanine exchange factor in B-cell malignancies

Objective： Chronic lymphocytic leukemia （CLL） and mantle cell lymphoma （MCL） cells over-express a guanine exchange factor （GEF）, Rasgrf-1. This GEF increases active Ras as it catalyzes the removal of GDP from Ras so that GTP can bind and activate Ras. This study aims to study the mechanism of action of Rasgrf-1 in B-cell malignancies. Methods： N-terminus truncated Rasgrf-1 variants have a higher GEF activity as compared to the full-length transcript therefore a MCL cell line with stable over-expression of truncated Rasgrf-1 was established. The B-cell receptor （BCR） and chemokine signaling pathways were compared in the Rasgrf-I over-expressing and a control transfected cell line. Results： Cells over-expressing truncated form of Rasgrf-1 have a higher proliferative rate as compared to control transfected cells. BCR was activated by lower concentrations of anti-IgM antibody in Rasgrf-1 over-expressing cells as compared to control cells indicating that these cells are more sensitive to BCR signaling. BCR signaling also phosphorylates Rasgrf-1 that further increases its GEF function and amplifies BCR signaling. This activation of Rasgrf-1 in over-expressing cells resulted in a higher expression of phospho-ERK, AKT, BTK and PKC-alpha as compared to control cells. Besides BCR, Rasgrf-1 over-expressing cells were also more sensitive to microenvironment stimuli as determined by resistance to apoptosis, chemotaxis and ERK pathway activation. Conclusions： This GEF protein sensitizes B-cells to BCR and chemokine mediated signaling and also upregulates a number of other signaling pathways which promotes growth and survival of these cells.

淋巴样增强结合因子1在B细胞慢性淋巴增殖性疾病中的表达

目的研究淋巴样增强结合因子1(lymphoid enhancer-binding factor 1,LEF1)在B细胞慢性淋巴增殖性疾病(B cell chronic lymphoproliferative disorders,B-CLPD)中的表达情况,探讨在B-CLPD亚型诊断中的价值。方法回顾性分析58例B-CLPD患者骨髓或淋巴结标本和20例对照组标本,采用免疫组化的方法,检测LEF1的表达情况。结果慢性淋巴细胞白血病(chronic lymphocytic leukemia,CLL)20例,LEF1阳性16例,阳性率为80%;套细胞淋巴瘤阳性为1/12;滤泡性淋巴瘤为1/5;边缘区淋巴瘤为0/11;淋巴浆细胞淋巴瘤为0/8;毛细胞白血病0/2;20例非恶性血液病患者未见LEF1表达;LEF1表达在CLL组差异有统计学意义(P=0.000);LEF1的表达和CD200、CLL积分等CLL的相关指标具有相关性(P<0.05)。4例LEF1阴性的CLL患者中,2例+12染色体异常,检出率高于LEF1阳性组(P>0.05)。结论LEF1在慢性淋巴细胞白血病患者的诊断和鉴别诊断中,有较好的灵敏性和特异性,是B-CLPD鉴别诊断的良好指标。

弥漫大B细胞型Richter综合征2例并文献复习

Richter综合征(Richter syndrome,RS)指在慢性淋巴细胞白血病(chronic lymphocytic leukemia,CLL)或小淋巴细胞淋巴瘤(small lymphocytic lymphoma,SLL)的背景下,疾病向侵袭性淋巴瘤进展转化的临床过程。RS转化是恶性血液病进展的一种临床表现,患者在出现RS转变时提示预后差。目前,全球范围内还未形成统一的RS治疗标准。本文回顾性分析2例从CLL向弥漫大B细胞淋巴瘤(diffuse large B-cell lymphoma,DLBCL)转化的RS患者的治疗方案及预后,探讨化疗后采用造血干细胞移植或嵌合抗原受体T细胞(chimeric antigen receptor T cell,CAR-T)免疫治疗等策略治疗RS的可能性,以为临床实践提供参考与借鉴。

骨髓形态联合免疫分型检测对慢性淋巴细胞白血病诊断及预后价值研究

目的:探讨慢性淋巴细胞白血病(CLL)患者骨髓形态、免疫表型特征,以及它们之间的关系。方法;采用流式细胞术对89例CLL患者骨髓或外周血标本进行免疫表型检测,依据细胞形态学分析将CLL患者分为典型CLL和混合型CLL两组,比较两组之间各抗原表达差异,并分析其对预后的影响。结果:89例CLL患者抗原表达阳性率由高至低依次为CD_(19)(98.9%)、HLA-DR(97.8%)、CD_5(88.8%)、CD_(20)(85.4%)、CD_(22)(71.9%)、CD_(23)(61.8%)、CD_(38)(39.3%)、FMC-7(11.2%)、CD_3(2.2%)。细胞形态学分型89例CLL中,典型CLL72例(80.9%),混合型CLL17例(19.1%)。CD_(38)在典型CLL及混合型CLL组间的阳性表达存在显著的统计学差异,CD_5、CD_(19)、CD_(20)、CD_(22)、CD_(23)、HLA-DR、FMC-7各抗原在两组间表达差异无统计学意义.预后分析显示混合型CLL生存期较典型CLL短(P<0.01),死亡患者与存活患者之间CD_(38)表达差异有明显的统计学意义。结论:细胞形态学结合免疫表型分析不仅是CLL诊断、鉴别诊断的主要手段,而且对预后判断具有重要价值。

慢性淋巴细胞白血病免疫表型特征分析及其临床意义

目的 :探讨慢性淋巴细胞白血病 (CLL)的免疫表型特点 ,并结合 β2 MG和LDH水平 ,对CLL患者的预后进行评价。方法 :采用间接免疫荧光法检测 15例CLL患者、12例急性粒细胞白血病 (AML)患者、11例急性淋巴细胞白血病 (ALL)患者和 1例滤泡细胞淋巴瘤 (FCL)患者的免疫表型 ;采用速率散射比浊法测定 13例CLL患者的血清 β2 MG和LDH水平。结果 :本组CLL患者的平均发病年龄为 6 2 .9岁 ,男女性别之比为 4∶1。免疫学标志CD5 ,CD19,CD2 0 ,全部阳性 ,12例CD2 3阳性 ;15例CLLCD38全部阳性 ;1例FCL患者CD10 ,CD19,CD2 0阳性 ,CD5 ,CD2 3阴性。 9例BinetC期CLL患者血清 β2 MG和LDH水平均较 3例BinetA期CLL患者明显增高 (均P <0 .0 5 )。结论 :CD19,CD2 0 ,CD5是B细胞型CLL特异的免疫表型 ,有助于CLL的诊断 ;CD2 3阴性的CLL患者临床分期属于BinetC期 ,提示预后不良 ;CD38阳性作为CLL的预后指标缺乏特异性 ;血清LDH和 β2

慢性B淋巴细胞白血病免疫表型的诊断研究

目的探讨慢性B淋巴细胞白血病(B-CLL)免疫表型的诊断情况。方法选择2014年1月至2015年2月潜江市江汉油田总医院初诊的50例B-CLL患者为观察组,再选择同期50例急性B淋巴细胞白血病(B-ALL)患者作为对照组。分别测定两组患者免疫细胞分型,并对比两组患者T细胞和自然杀伤细胞等免疫表型情况。结果 50例观察组患者中CD5、CD19以及CD20的表达较为常见,其阳性率分别为88.0%(44/50)、98.0%(49/50)、94.0%(47/50),CD22的表达阳性率较低,为78.0%(39/50),CD38最低,为36.0%(18/50)。观察组CD+3CD+4、CD+3CD+8、CD+4CD+8、CD+3、CD3-CD16+CD56+均高于对照组[(4.35±0.23)%比(3.21±0.45)%,(4.15±0.22)%比(3.02±0.32)%,(1.51±0.23)%比(1.10±0.11)%,(9.53±1.95)%比(6.46±1.54)%,(6.12±0.64)%比(4.35±0.12)%],差异有统计学意义(P<0.05或P<0.01)。结论 B-CLL的表型特征是CD19、CD23以及CD5的共同表达;CD10,CD5可以作为成熟型B-ALL和B-CLL鉴别诊断时特异性的指标。

慢性淋巴细胞白血病伴中枢神经系统浸润1例并文献复习

目的：探讨慢性淋巴细胞白血病（chronic lymphocytic leukemia，CLL）伴中枢神经系统（central nervous system，CNS）浸润的发病率、诊治方法及预后。方法：报道1例以头晕、复视、肢体无力为首发表现的CLL患者诊治经过并结合文献复习。结果：尸解研究显示CLL浸润CNS的发生率为8％-71％，而患者生前出现有症状CNS浸润的发生率较低约1％，发生原因与临床分期、年龄、性别及疾病变异无明确相关性，临床表现不特异，诊断主要依靠脑脊液细胞形态学结合流式细胞分析，鞘内化疗及放疗可使多数患者CNS症状及脑脊液改善，未治疗的患者均迅速恶化死亡。结论：CLL有症状的CNS浸润较少见，一旦发生预后差，及时诊断和积极治疗是获得长期缓解的关键。

B细胞慢性淋巴增殖性疾病诊断及治疗研究进展

最新的世界卫生组织(WHO)关于B细胞慢性淋巴增殖性疾病分类包括慢性淋巴细胞白血病(CLL)、B-幼淋巴细胞白血病(B-PLL)、毛细胞白血病(HCL)、边缘区淋巴瘤(MZL)、滤泡淋巴瘤(FL)、套细胞淋巴瘤(MCL)、淋巴浆细胞淋巴瘤/华氏巨球蛋白血症(LPL/WM)。它们在细胞形态、免疫表型及分子遗传学等方面有部分相似,但在治疗和预后上有明显差异。此外,许多新的作用于细胞周期和凋亡通路的药物,如蛋白酶体抑制剂、免疫调节剂、组蛋白去乙酰化酶抑制剂取得了令人鼓舞的疗效,为B细胞慢性淋巴增殖性疾病患者带来新的希望。现就近年国际上对B细胞慢性淋巴增殖性疾病的诊断和治疗最新研究进展作一综述。

复旦大学附属中山医院慢性淋巴细胞白血病/小淋巴细胞淋巴瘤诊疗规范(v1.2018)

慢性淋巴细胞白血病(chronic lymphocytic leukemia,CLL)是欧美国家最常见的成人白血病类型,文献报道中国和日本CLL的发病率仅为欧美国家的10%。近年来,随着我国经济发展水平的迅速提升和国民生活方式的日益西化,特别是随着对该病认识和诊断水平的提高,CLL的发病率(检出率)有不断升高的趋势,严重威胁国人的生命健康。与欧美国家患者相比,中国CLL患者的发病机制、临床表现及治疗转归存在一定的独特性。因此,制定适合中国患者的CLL诊疗规范,积极应对疾病谱系变迁,实现疾病治疗的个体化、精准化正当其时。本文参考国内外文献结合复旦大学附属中山医院血液科的宝贵经验,向读者展示了内容前沿准确、风格简洁明快、中心特色鲜明的单中心中国CLL诊疗规范,为同行提供参考,以期提升中国CLL治疗水平,救治更多的CLL患者。

Safety and efficacy of obinutuzumab in Chinese patients with B-cell lymphomas: a secondary analysis of the GERSHWIN trial

Background:Patients with relapsed/refractory B-cell lymphomas have limited treatment options.GERSHWIN is an open-label,single-arm,phase Ib study of obinutuzumab monotherapy in Chinese patients with histologically docu-mented CD20+relapsed/refractory chronic lymphocytic leukemia(CLL),diffuse large B-cell lymphoma(DLBCL),or follicular lymphoma(FL).The primary outcome measure of pharmacokinetics has been previously reported.We now present data on the secondary endpoint measures(e.g.,safety,and efficacy and pharmacodynamics).Methods:Patients received 1000 mg obinutuzumab intravenously on days 1,8,and 15 of cycle 1(CLL patients;first dose split over 2 days),and on day 1 of cycles 2-8.Each cycle lasted for 21 days;the treatment period was 24 weeks.All subjects receiving at least one dose of obinutuzumab were included in the analysis of safety,efficacy,as well as pharmacodynamics.Results:A total of 48 patients(>18 years of age)were enrolled(CLL:12;DLBCL:23;FL:13).The subjects received a median of two lines of anticancer treatment prior to the enrollment.Thirty-five patients(72.9%)had at least one adverse event(AE).The most frequent AE was infusion-related reactions(15 patients;31.3%),followed by pyrexia(11 patients;22.9%).Treatment-related AEs were reported in 28 patients(58.3%),and included one death(interstitial lung disease).End-of-treatment(EoT)response rate was 33.3%.Best overall response rate was 47.9%.Most CLL patients achieved a partial response at EoT(58.3%).CD19+depletion occurred in 75.0%of the patients with CLL,and all patients with FL and DLBCL.Conclusions:The safety and efficacy of obinutuzumab monotherapy in Chinese patients with B-cell lymphomas were similar to that observed in previous studies in non-Chinese patients;no new safety signals were observed.

28例慢性淋巴细胞白血病的诊断、变异和治疗

本文分析２８例慢性淋巴细胞白血病，提出诊断标准、变异特点及治疗指征。２６例接受联合化疗，完全缓解９例（３５％），部分缓解４例（１５％），病情稳定１３例（５０％）。缓解期＞３０～４６８７天，生存期＞５０～４８３７天。有４例变异，转化为幼稚淋巴细胞白血病３例，Ｒｉｃｈｔｅｒ综合征１例，变异后预后不良。

中国慢性淋巴细胞白血病/小淋巴细胞淋巴瘤诊疗现状:一项多中心问卷调查研究

目的了解慢性淋巴细胞白血病(CLL)/小淋巴细胞淋巴瘤(SLL)在中国各级医疗机构血液科、肿瘤科与淋巴瘤科的诊疗现状。方法2021年3月至2021年7月期间国内多家医疗单位开展了一项多中心问卷调查,共纳入1000名符合研究条件的医生,采用面对面和线上问卷调查相结合的方式,利用标准化问卷对其所诊疗的CLL/SLL患者的疾病诊断、预后评估、治疗方案选择、布鲁顿酪氨酸激酶(BTK)抑制剂使用等方面进行调查。结果①受访医生接诊的CLL/SLL患者男性比例高于女性(62.0%对38.0%),年龄主要集中在61~70岁(占37.7%);②在患者诊断上,除血常规外,受访医生大多进行了骨髓穿刺涂片、活检、免疫组化等检测;③仅13.7%的受访医生完全掌握了现有指南推荐的起始治疗指征;④在预后高危因素认知方面,受访医生对伴免疫球蛋白重链可变区(IGHV)未突变、11q-的掌握远不如TP53突变和复杂核型这两个预后高危因素,且仅有17.1%的受访医生完全掌握了CLL国际预后指数(CLL-IPI)评分系统;⑤在一线治疗方案中,BTK抑制剂是不同类型患者的一线治疗方案,且医生对伴高危因素和老年患者需优先使用BTK抑制剂已形成一定认知,但不同类型患者实际使用BTK抑制剂比例不高(31.6%~46.0%);⑥69.0%的受访医生曾减量使用过BTK抑制剂,66.8%的医生曾中断BTK抑制剂超过12 d。导致减量或中断BTK抑制剂使用的主要原因为不良反应(房颤、重度骨髓抑制、出血、肺部感染等)、经济因素以及病情得到控制;⑦血液科医生和肿瘤科医生在CLL/SLL预后评估、治疗方案选择、BTK抑制剂应用等方面均存在一定差异。结论目前中国各级医院血液科、肿瘤科与淋巴瘤科医生在CLL/SLL的诊断、治疗指征判定、预后评估、伴随疾病评估、治疗方案选择以及BTK抑制剂使用上仍有很多不足,由不良反应导致减量或中断/终止治疗的患者占比较高。

受体酪氨酸激酶样孤儿受体1在慢性淋巴细胞白血病中的诊断价值及预后意义

目的探讨受体酪氨酸激酶样孤儿受体1(ROR1)在慢性淋巴细胞白血病(CLL)中的表达及其在临床诊断中的价值,以及ROR1表达与患者遗传学和分子生物学异常的相关性。方法回顾性收集2020年11月至2021年11月于南京医科大学第一附属医院(江苏省人民医院)收治的初诊B细胞慢性淋巴增殖性疾病(B-CLPD)患者209例,其中典型免疫表型CLL 70例,不典型免疫表型CLL 16例,MCL 14例,其他类型B-CLPD 109例。应用多参数流式细胞术(FCM)检测209例患者肿瘤细胞中ROR1表达水平,采用χ^(2)检验、四格表诊断性试验分析ROR1在CLL中的诊断价值以及与患者遗传学和分子生物学异常的相关性。结果CLL患者中ROR1阳性表达率高于非CLL(78%>11%,P<0.001);典型免疫表型CLL与不典型免疫表型CLL中ROR1阳性表达率差异无统计学意义(81%>63%,P>0.05);不典型免疫表型CLL中ROR1阳性表达率高于MCL(63%>21%,P<0.05)。ROR1^(+)CLL组与ROR1-CLL组染色体核型异常检出率差异有统计学意义,ROR1^(+)CLL组复杂核型的检出率高于ROR1-CLL组(34%>14%,P<0.05)。60岁以上CLL患者ROR1阳性率更高(P<0.05)。结论ROR1可以作为CLL的辅助诊断标记物,尤其对不典型免疫表型CLL、MCL及其他类型B-CLPD的诊断及鉴别诊断有重要价值,ROR1阳性患者年龄偏高,更易检出染色体复杂核型。

以肾病综合征为初始表现的慢性淋巴细胞白血病1例并文献复习

目的探讨慢性淋巴细胞白血病患者肾脏受累的临床表现、诊断和治疗。方法回顾性分析2020年10月福建省人民医院收治的1例以肾病综合征为初始表现的慢性淋巴细胞白血病患者的临床资料,并复习相关文献。结果患者为68岁男性,以反复全身水肿、泡沫尿为初始表现,就诊肾内科诊断为肾病综合征,治疗后未见明显改善并逐渐出现淋巴细胞增高,就诊血液科确诊为慢性淋巴细胞白血病。应用伊布替尼单药治疗后淋巴细胞计数和尿蛋白逐渐降至正常,随访结束患者临床疗效评价为完全缓解。结论以肾病综合征为初始表现的慢性淋巴细胞白血病较为罕见,临床异质性较大,尽早诊断是治疗成功的保障,一线Bruton酪氨酸激酶抑制剂单药治疗的效果和安全性较好。

白细胞分化抗原160对慢性淋巴细胞白血病的诊断及预后意义

目的探讨CD160抗原在慢性淋巴细胞白血病(CLL)中的表达及在临床诊断中的价值,以及CD160抗原表达与患者的遗传学异常的相关性.方法回顾性研究.收集2015年1月至2017年12月南京医科大学第一附属医院(江苏省人民医院)收治的初诊的成熟小B细胞淋巴瘤336例.依据2008年第4版《造血和淋巴组织肿瘤的WHO分类》诊断200例CLL患者,根据英国马斯登皇家医院免疫标志积分系统又分为典型CLL122例,其中男80例,女42例,年龄45~82岁(中位年龄65岁);不典型CLL78例,其中男48例,女30例,年龄43~76岁(中位年龄60岁);49例套细胞淋巴瘤(MCL)患者,其中男39例,女10例,年龄27~70岁(中位年龄56岁);以及87例CD5-的小B细胞淋巴瘤(SBL)患者,其中男60例,女27例,年龄38~80岁(中位年龄63岁).应用多参数流式细胞术(FCM)检测336例患者肿瘤细胞CD160的表达率和平均荧光强度(MFI),同时采用荧光原位杂交(FISH)技术检测145例CLL患者P53缺失、107例CLL患者13q14缺失、110例CLL患者ATM缺失、104例CLL患者6q23缺失、104例CLL患者+12,以及138例CLL患者IGH重排,比较CD160+CLL患者与CD160-CLL患者遗传学和分子生物学特点.结果122例典型CLL患者中CD160阳性表达率为59.8%(73/122),MFI范围为14.9~173.9,78例不典型CLL患者中CD160阳性表达率为64.1%(50/78),MFI为范围为29.6~193.7,而MCL患者中CD160均为阴性.CD160在典型及不典型CLL中的阳性率均明显高于MCL,差异有统计学意义(χ2分别为51.16,51.81,P<0.01);在CD5-的SBL中CD160+阳性率为1.1%(1/87),CD160在典型及非典型CLL中的阳性率均明显高于CD5-的SBL,差异有统计学意义(χ2分别为80.00,80.02,P<0.01).51例CD160-的CLL中IGH重排率为31.6%(18/51),87例CD160+CLL患者的IGH重排率为62.1%(54/87),CD160+CLL患者的IGH重排率高于CD160-CLL患者,差异有统计学意义(χ2=9.24,P<0.05).结论CD160+对于辅助诊断CLL有重要价值,尤其有助于不典型CLL和MCL以及其他类型SBL的诊断和鉴别诊断.