Efficacy of Nilotinib versus Imatinib in Philadelphia Positive Patients with Chronic Myeloid Leukemia in Early Chronic Phase Who Have a Warning Molecular Response to Imatinib

Background and Objectives: Chronic myeloid leukemia (CML) accounts for approximately 15% of newly diagnosed cases of leukemia in adults. In this study, the efficacy of nilotinib at 400 mg BID is compared with imatinib at 400 mg BID in CML patients with suboptimal molecular response after at least 12 months of daily dose 400 mg of imatinib therapy. Patients and Methods: This study included a total number of 50 patients, divided into two groups (25 patients each). The first group (Group I): Patients received imatinib at 400 mg BID, second group (Group II): Patients had a suboptimal molecular response to imatinib and received nilotinib at 400 mg BID in early chronic phase. During the two years period of data collection, the primary end included median survival. The secondary end included response rate, type of response, duration of response and progression free survival. Also side effects were recorded. Patients were followed up every month by complete and differential blood counts, liver function test, renal function test and (PCR) every three months for two year. Results: Nilotinib group had significantly higher frequency of major molecular response (MMR) where 23 (92%) patients achieved it while only 16 (64%) patients in Imatinib group achieved MMR (P = 0.01). Nilotinib had better toxicities profile than Imatinib. Conclusion: Both Nilotinib and high dose Imatinib achieved response in CML patients with suboptimal response with rapid and deeper molecular response, better survival outcomes and less side effects in nilotinib.

Chronic myeloid leukemia-from the Philadelphia chromosome to specific target drugs:A literature review

Chronic myeloid leukemia(CML)is a myeloproliferative neoplasm and was the first neoplastic disease associated with a well-defined genotypic anomaly―the presence of the Philadelphia chromosome.The advances in cytogenetic and molecular assays are of great importance to the diagnosis,prognosis,treatment,and monitoring of CML.The discovery of the breakpoint cluster region(BCR)-Abelson murine leukemia(ABL)1 fusion oncogene has revolutionized the treatment of CML patients by allowing the development of targeted drugs that inhibit the tyrosine kinase activity of the BCR-ABL oncoprotein.Tyrosine kinase inhibitors(known as TKIs)are the standard therapy for CML and greatly increase the survival rates,despite adverse effects and the odds of residual disease after discontinuation of treatment.As therapeutic alternatives,the subsequent TKIs lead to faster and deeper molecular remissions;however,with the emergence of resistance to these drugs,immunotherapy appears as an alternative,which may have a cure potential in these patients.Against this background,this article aims at providing an overview on CML clinical management and a summary on the main targeted drugs available in that context.

A novel t(3;12)(q21;p13) translocation in a patient with accelerated chronic myeloid leukemia after imatinib and nilotinib therapy

The acquisition of secondary chromosomal aberrations in chronic myeloid leukemia (CML) patients with Philadelphia chromosome-positive (Ph+) karyotype signifies clonal evolution associated with the progression of the disease to its accelerated or blastic phase. Therefore, these aberrations have clinical and biological significance. T(3;12)(q26;p13), which is a recurrent chromosomal aberration observed in myeloid malignancies, is typically associated with dysplasia of megakaryocytes, multilineage involvement, short duration of any blastic phase, and extremely poor prognosis. We have identified a recurrent reciprocal translocation between chromosomes 3 and 12 with different breakpoint at bands 3q21 in the malignant cells from a 28-year-old man. The patient was initially diagnosed as having Ph+ CML in the chronic phase. The t(3;12)(q21;p13) translocation occurred 4 years after the patient was first diagnosed with CML while undergoing tyrosine kinase inhibitor therapy. We confirmed the t(3;12)(q21;p13) translocation via fluorescence in situ hybridization assay by using whole-chromosome paint probes for chromosomes 3 and 12. Our findings demonstrate that, similar to other recurrent translocations involving 3q26 such as t(3;3) and t(3;21), the t(3;12)(q21;p13) translocation is implicated not only in myelodysplastic syndrome and acute myeloid leukemia but also in the progression of CML. These findings extend the disease spectrum of this cytogenetic aberration.

Severe hemorrhagic colitis in a patient with chronic myeloid leukemia in the blastic phase after dasatinib use

Dasatinib is a second-line tyrosine kinase inhibitor used in patients with imatinib resistant or intolerant chronic myeloid leukemia (CML) and Philadelphia chromosomepositive acute leukemia. Gastrointestinal bleeding may occur in up to 7% of patients using dasatinib, although, severe dasatinib-related acute colitis had rarely been reported. Here, we present the case of a 36-year-old female who progressed to acute myeloid leukemia after fourteen months of receiving imatinib for CML in the chronic phase and was treated with a dasatinib-containing chemotherapy regimen. On day 34 of treatment, the patient developed moderate abdominal pain and bloody diarrhea with mucous. Analyses of stool specimens were negative for parasites, Clostridium difficile , and other pathogenic bacteria. The cytomegalovirus pp65 antigen was negative in her blood leukocytes. A colonoscopy revealed acute colitis, and a mucosal biopsy showed nonspecific colitis. The patient was treated with broad-spectrum antibiotics, bowel rest and hydration, and dasatinib treatment was stopped. Her bloody diarrhea improved within 72 h. After confirming cytological remission, the patient received initial course of consolidation, and dasatinib treatment was reinstated. However, hemorrhagic colitis recurred. After discontinuing dasatinib, herhemorrhagic colitis drastically improved and did not recur following the administration of nilotinib. The characteristics of our patient suggest that dasatinib treatment can lead to hemorrhagic colitis, which typically resolves after discontinuation of the drug.

Frequency of Bcr-Abl Fusion Oncogene Splice Variants Associated with Chronic Myeloid Leukemia (CML)

BCR-ABL fusion oncogene originates from the reciprocal translocation of chromosome 9 and 22 t(9;22) (q34;q11). It translates a chimeric protein, p210, characterized by constitutive activation of its tyrosine kinase, which triggers leukemogenic pathways resulting in onset of chronic myeloid leukemia (CML). In CML, the classic fusion is b2a2 or b3a2 fusing exon 13 (b2) or exon 14 (b3) of BCR to exon 2 (a2) of ABL. The type of bcr/abl transcripts may be associated with different prognosis and hence useful in therapeutic plan. This study was conducted to calculate the frequency of these splice variants as the frequencies of different fusion oncogenes associated with leukaemia can vary in different geographical regions due to interplay of genetic variation in different ethnic populations, diverse environmental factors and living style. A very sensitive nested RT-PCR was established to detect BCR-ABL splice variants in CML. Sensitivity of RT-PCR assay was of the order of 10–6. Thirty CML patients were subjected to BCR-ABL analysis. Out of 30 Pakistani patients, 19 (64%) expressed b3a2 while 11 (36%) expressed b2a2 transcript. This shows that BCR-ABL splice variants differ in their frequencies which may have an effect on biology and implications for prognosis and management of BCR-ABL positive Leukemias.

慢性髓系白血病慢性期TKI治疗未达最佳反应或不耐受患者转换氟马替尼的有效性和安全性临床观察

目的 观察TKI未达最佳反应或不耐受的慢性髓系白血病-慢性期(chronic myelogenous leukemia-chronicphase, CML-CP)患者转换氟马替尼治疗的效果及安全性。方法 从重庆市医院及川北医学院附属医院共5家医院收集2020年2月至2022年8月对一线伊马替尼、达沙替尼、尼洛替尼未达最佳反应或不耐受,转换氟马替尼(600 mg/d)治疗的患者,观察氟马替尼的疗效及安全。统计患者治疗3、6、12个月时最佳反应率及主要分子学反应(major molecular response, MMR)率、累积完全细胞遗传学反应(complete cytogenetic response, CCyR)率、累积MMR率、累积深度分子学反应(deep molecular response, DMR)率、无进展生存(progression-free survival, PFS)、无事件生存(event-free survival, EFS)情况及不良反应情况。结果 共纳入100例CML-CP患者,中位随访时间为18(3~36)个月,3、6、12个月最佳反应率分别为92.6%(88/95)、94.4%(85/90)和92.9%(79/85),随访截止至2023年8月20日,累积CCyR、MMR率分别为98.0%(98/100)、81.9%(77/94),达CCyR和MMR的中位时间均为3个月,累积DMR率为51.0%(51/100)。随访时间内,PFS率为100.0%(100/100),1年EFS率为85.6%(75/90)。氟马替尼最常见非血液学不良反应为腹泻腹痛(7.0%),其次为肾功能损害(6.0%)、肌肉骨骼疼痛(2.0%);血液学不良反应主要有血小板减少(12.0%)、贫血(6.0%)和白细胞减少(2.0%)。结论 氟马替尼治疗TKI未达最佳反应或不耐受的CML-CP患者有较好的MMR和DMR,耐受性及安全性良好。

The Philadelphia chromosome in leukemogenesis

The truncated chromosome 22 that results from the reciprocal translocation t(9;22)(q34;q11) is known as the Phila?delphia chromosome(Ph) and is a hallmark of chronic myeloid leukemia(CML).In leukemia cells,Ph not only impairs the physiological signaling pathways but also disrupts genomic stability.This aberrant fusion gene encodes the breakpoint cluster region?proto?oncogene tyrosine?protein kinase(BCR?ABL1) oncogenic protein with persistently enhanced tyrosine kinase activity.The kinase activity is responsible for maintaining proliferation,inhibiting differentia?tion,and conferring resistance to cell death.During the progression of CML from the chronic phase to the accelerated phase and then to the blast phase,the expression patterns of different BCR?ABL1 transcripts vary.Each BCR?ABL1 transcript is present in a distinct leukemia phenotype,which predicts both response to therapy and clinical outcome.Besides CML,the Ph is found in acute lymphoblastic leukemia,acute myeloid leukemia,and mixed?phenotype acute leukemia.Here,we provide an overview of the clinical presentation and cellular biology of different phenotypes of Ph?positive leukemia and highlight key findings regarding leukemogenesis.

A survey on tyrosine kinase inhibitor treatment in patients with chronic myeloid leukemia in China: from patients' perspective

Objective To assess tyrosine kinase inhibitor(TKI)treatment status in patients with chronic myeloid leukemia(CML)in China and analyze the response-associated factors.Methods From May to November in 2014,anonymous questionnaires were distributed to adult CML patients who were receiving TKI treatment all over China.

Patient reported outcome of tyrosine kinase inhibitor related side effects and their impact on daily life in Chinese patients with chronic myeloid leukemia in the chronic phase

Objective To explore the impact of patient reported outcome of tyrosine kinase inhibitor(TKI)related side effects on daily life in Chinese patients with chronic myceloid leukemia(CML)in the chronic phase(CP).Methods From May to November in 2014。

A comparison of efficacy and safety between Chinese generic imatinib and branded imatinib in patients with newly-diagnosed chronic myeloid leukemia in the chronic phase:a single-center prospective cohort study

Objective To compare the efficacy and safety between Chinese generic imatinib(Xinwei~,Jiansu Hansoh Pharmaceutical Group Co.,Ltd.)and branded imatinib(Glivec~,Novartis)in patients with newly-diagnosed chronic myeloid leukemia in chronic phase(CML-CP).Methods Patients with newly diagnosed CML-CP

MIC分型评价成人急-性髓系白血病中的淋系抗原表达

目的:研究成人急性髓系白血病(acute myeloid leukemia,AML)中淋系抗原的表达及其与预后的关系。方法:对275例成人AML进行细胞形态学、流式细胞免疫表型分析和染色体细胞遗传学(MIC)分型实验研究并对其中的64例M2进行临床治疗结果观察研究。结果:①AML淋系抗原阳性率31．3％,其中t(8;21)者为48．3％,无t(8;21)者为26．5％(P< 0．001)。②CD19+在t(8;21)中占38．3％,无t(8;21)中占1．9％(P<0．001);而其他淋系抗原两组比较均为P>0．05．③治疗结果(CR率):t(8;21)和无t(8;21)M2分别为66．7％和41．9％,CD19+和CD19-M2分别为76．5％和46．8％,CD19+／t(8; 21)和CD19-／无t(8;21)分别为80．0％和41．4％,以上均为P<0．05。而CD19-／t(8;21)和CD19+／无t(8;21)分别为55．6％和50．0％(P>0．05)。结论:成人AML中淋系抗原表达与核型密切相关,t(8;21)AML高表达CD19。t(8;21)和CD19都是M2预后好的标志之一。

甲磺酸伊马替尼治疗慢性粒细胞白血病122例疗效评价

目的评价甲磺酸伊马替尼治疗Ph阳性慢性粒细胞白血病(CML)的有效性与安全性。方法95例Ph阳性CML慢性期(CP)患者持续口服甲磺酸伊马替尼400mg/d;15例加速期(AP)和12例急变期(BC)患者持续口服甲磺酸伊马替尼400mg/d或600mg/d。结果①CP(早CP56例,晚CP39例):中位追踪15(5.0～44.0)个月,获得的总的完全血液学缓解(CHR)率为97.8%,主要细胞遗传学缓解(MCyR)率为80.0%,完全细胞遗传学缓解(CCyR)率为73.6%。其中早CP(<12个月)缓解率分别为98.2%、91.0%、80.3%;晚CP(≥12个月)分别为97.4%、64.1%、56.4%。②进展期(AP和BC):中位追踪15(6.0～33.0)个月,获得总的CHR、MCyR、CCyR分别为55.6%、33.3%,22.2%。③治疗中Ⅲ级WBC和Plt减少总的发生率在CP分别为15.8%,24.2%。进展期总的发生率分别为26.0%,40.7%。Ⅲ～Ⅳ级非血液学不良反应很少发生。结论①甲磺酸伊马替尼对经干扰素(IFN-α)治疗失败的CML-CP有较高的血液学及遗传学缓解率,且早CP较晚CP疗效更好。②伊马替尼对AP、BC患者也有一定的近期疗效,但与CP相比较差。远期疗效有待进一步观察。

甲磺酸伊马替尼治疗3例Ph阳性慢性髓性白血病达细胞遗传学缓解后的疾病转化

目的观察Ph阳性慢性髓性白血病(Philadelphia chromosome-positive chronic myelogenous leukemia,Ph+CML)患者在甲磺酸伊马替尼治疗达细胞遗传学缓解后的疾病进展。方法对3例伊马替尼单药治疗有效的Ph+CML患者,包括第1次慢性期(例1)、第2次慢性期(例2)和加速期(例3)各1例,在治疗前及持续治疗后定期监测其血液学和细胞遗传学(G显带方法)变化。结果例1、例2和例3分别在伊马替尼治疗4个月、3个月和6个月时获得完全细胞遗传学缓解(complete cytogenetic remission,CCyR),但在随后的12个月、6个月和0个月(即服药的第16个月、9个月和6个月)时,分别发生了急性淋巴细胞白血病、急性髓性白血病和皮肤软组织髓外急变,同期骨髓染色体检查显示例1和例3未检出Ph+细胞,呈完全正常核型,例2Ph+细胞仅占20%。结论伊马替尼治疗Ph+CML获得CCyR后,患者仍可发生Ph阴性(Philadelphia chromosome-negative,Ph-)或Ph-为主的急性白血病或髓外急变。

Ph染色体阳性慢性粒细胞白血病的细胞遗传学研究

目的 研究Ph染色体阳性慢性粒细胞白血病即Ph (+ )CML患者的核型状况与病程变化、预后的关系 .方法 采用直接法和短期培养法制备骨髓细胞染色体 ,通过G显带对 198例Ph (+ )CML患者进行染色体核型分析 .结果 ⑴Ph(+ )CML患者中 193例为典型Ph易位 ,占 97.5 %,5例为变异Ph易位 ,占 2 .5 %;⑵急变期超二倍体发生率 (10 .8%)较慢性期 (4.2 %)有显著性差异 (P <0 .0 5 ) ;⑶ 4 1例慢性期患者 (32 .3%)合并额外染色体异常 ,主要异常核型有 19种 ,以 + 8、2个Ph ,-Y较为多见 ;⑷ 2 6例急性期患者 (78.8%)出现额外染色体改变 ,主要异常核型有 2 1种 ,以 2个Ph ,+ 8,i(17q) ,+ 19较多见 ;⑸急变后只有Ph染色体者和同时具有Ph及额外染色体异常者的中位生存期分别为 5 .5月、3.6月 ,二者有显著性差异 (P <0 .0 5 ) .结论 额外染色体畸变的有无及程度与Ph (+ )CML病程进展、预后密切相关 .

伊马替尼治疗慢性粒细胞性白血病疗效观察

目的观察伊马替尼(Imatinib)治疗慢性粒细胞性白血病(CML)的近期疗效和安全性。方法28例CML患者均予伊马替尼400或600 mg/d一次性餐后顿服,常规体检,用药后血液学取得完全缓解后择期复查骨髓、Ph染色体和/或BCR-ABL基因。结果随访结束时,血液学完全缓解率61%(17/28),部分缓解率11%,总有效率71%,绝大多数为轻度不良反应,多可耐受。结论伊马替尼治疗CML有效、安全,但远期疗效需进一步观察。

Ph染色体和bcr-abl融合基因的动态监测在慢性粒细胞白血病治疗中的临床意义

目的评价Ph染色体和bcr-abl融合基因检测在慢性粒细胞白血病诊断、治疗及微小残余病变监测中的临床意义。方法应用常规染色体显带技术、半定量反转录PCR(RT-PCR)技术和实时荧光定量PCR(RQ-PCR)技术对20例患者Ph染色体及bcr-abl融合基因进行动态监测,随诊3年。结果 20例慢性粒细胞白血病患者,19例患者Ph染色体阳性,20例均有bcr-abl融合基因阳性,其中11例应用伊马替尼治疗患者中9例患者Ph染色体和bcr-abl融合基因消失,提示遗传学缓解率为81.8%。9例应用常规化疗的患者随诊3年,Ph染色体和bcr-abl融合基因均未转阴。结论 Ph染色体和bcr-abl融合基因动态监测对慢性粒细胞白血病患者诊断、治疗、病情监测及预后判断有重要临床意义。

CML患者在TKI治疗过程中的细胞遗传学变化与病程演进的关系分析

目的:分析慢性髓系白血病(CML)患者在酪氨酸激酶抑制剂(TKI)治疗过程中的细胞遗传学变化与病程演进的关系。方法:对本院收治的150例初诊CML患者,通过骨髓细胞24 h短期培养法或直接法,行染色体G显带技术核型分析;经ABL激酶区点突变检测,分析细胞遗传学变化与其病程演进的相关性。结果:间接荧光原位杂交技术检测结果发现,150例患者BCR-ABL融合基因均为阳性,其中费城(Ph)染色体阳性142例(94.67%),阴性8例(5.33%);142例Ph染色体阳性患者中,初诊Ph阳性且伴有额外染色体异常14例(9.86%),变异易位4例(2.82%),标准易位t(9;22)(q34;q11)124例(87.32%)。14例伴有额外染色体异常的患者中,"主要路径"异常8例,-Y异常2例,"次要路径"异常4例。在TKI治疗期间,46例标准易位患者出现额外染色体异常,以染色体数目异常为主,此类患者疾病进展和出现点突变的比例较高(P<0.05)。与标准易位患者比较,初诊CML慢性期伴有额外染色体异常患者无病生存率明显降低(P<0.05),而与总生存率的比较,并无明显差异(P>0.05)。与无额外染色体异常患者比较,CML慢性期TKI治疗期间出现额外染色体异常者无病生存率及总生存率明显下降(P<0.05)。结论:部分CML患者在疾病发生和发展过程中可出现额外染色体异常,此类患者发生疾病进展的风险性较高。

伊马替尼治疗儿童慢性髓细胞性白血病效果分析

目的回顾性分析伊马替尼对儿童慢性髓细胞性白血病的疗效及不良反应。方法收集2012年1月-2013年1月经MICM分型标准确诊为慢性髓细胞性白血病伴费城染色体阳性且接受伊马替尼治疗患儿的临床资料。5例患儿中，男2例，女3例；中位年龄为9岁（6—11岁）；均予以伊马替尼口服[340mg／（m^2·d）]；中位随访时间为25个月（15～30个月），定期观察患儿临床表现及外周血象、骨髓细胞学和分子生物学指标的变化，同时监测生长发育和骨骼代谢情况。结果经伊马替尼规范治疗后，患儿分别在3个月和12个月内获得完全血液学缓解和细胞遗传学缓解。1例患儿伊马替尼治疗25个月后血清骨钙素水平超出正常值上限1倍多，其余患儿未见生长发育相关指标明显异常。结论伊马替尼对慢性髓细胞性白血病患儿的疗效显著且安全，其不良反应尚有待长期随访跟踪。

362例慢性髓系白血病的细胞遗传学分析

为探讨慢性髓系白血病(CML)的细胞遗传学特点及临床意义,对362例CML患者采用24小时短期培养法制备骨髓染色体,用R显带技术进行染色体核型分析。将患者分为慢性期和急变期两组。结果表明:附加染色体异常、变异易位、Ph(-)bcr/ab l(+)并伴有染色体异常者在两组中的比例分别为:70/268(26.1%)、19/268(7.1%)、4/268(1.5%);50/94(53.2%)、8/94(8.5%)、4/94、(4.3%)。362例标本中检出Ph阳性标本324例(89.5%),其中典型t(9;22)(q34;q11)易位297例(91.7%),变异易位27例(8.3%)。在27例变异易位中单纯变异易位13例,复杂变异易位13例,隐匿Ph 1例。362例标本中共发现120例特殊核型异常。对上述异常分析显示,出现频率较高的数目异常有:+Ph:26例(21.7%);+8:12例(10.0%);+21:12例(10.0%);+19:9例(7.5%)。结构异常中以i(17q)最多,有16例(13.3%)。结论:与慢性期相比,急变期附加染色体、变异易位等异常率均明显增加,染色体核型分析有助于疾病进展的判断。