Focal lymphoblastic transformation of chronic myelogenous leukemia develops into erythroid leukemia:A case report

BACKGROUND We present a case of focal lymphoblastic transformation to erythroid leukemia following acute myeloblastic transformation in a patient with chronic myelogenous leukemia(CML)and discuss its mechanism of occurrence and development.CASE SUMMARY The presence of the Philadelphia(Ph)chromosome was identified through karyotype analysis,while the BCR-ABL fusion gene was detected using quantitative real-time polymerase chain reaction of the peripheral blood sample.Fluorescence in situ hybridization was used to detect the expression of the BCRABL gene in the lymphoma.Antigen expression and gene mutations in the primitive cells were detected by flow cytometry.The analysis confirmed the presence of CML along with focal lymphoblastic transformation to erythroid leukemia.Additionally,the patient was found to have secondary erythroid leukemia,along with multiple new gene mutations and abnormalities in complex karyotypes of chromosomes.CONCLUSION Our findings suggest a possible molecular basis for the focal lymphoblastic transformation secondary to myeloblastic transformation in patients with CML.

Redistribution of Platelet Membrane Glycoprotein IV and Release of Intracellular α-granule Thrombospondin in Patients with Chronic Myelogenous Leukemia

The redistribution of platelet membrane glycoprotein IV (GPIV) and the release of intracellular Q-granule thrombospondin (TSP) were examined and the inhibition of 5-thromboglobulin (&TG) and platelet factor 4 (PF4) in patients with chronic myelogenous leukemia (CML) was observed and quantitation of β-TG and PF4 in sera was conducted. GPIV in inactive platelet from CML was 36080±17010 molecules/platelet as compared with 13190±4810 from the controls (P<0,01), No abnormality was found in the distribution of platelet membrane GPIb and GPIIb/III.(P>0. 05). The GPIV redistribution on active platelet membrane induced thrombin (1U/ml) from CML and healthy donors was 44320132310 and 228001 12700 molecules/platelet respectively (P<0. 01 ). The difference in the release of intracellular Q-granule TSP between CML and the control group was not found (P>0.05). There was no direct correlation between GPIV expression and TSP binding after platelet activation. The high leveIs of β-TG and PF4 in sera inhibited release of intracellular a-granule TSP in vitro. These results indicate that the abnormality of platelet membrane GPIV is a common marker in CML, therefore the specific increase of platelet GPIV in patients with CML may be a useful tool for the diagnosis and monitoring of the platelet dysfunction. The release of interna1 TSP pools is hindered by either β-TG or PF4 in sera.

HIM_(1) AND HIM4, TWO MONOCLONAL ANTIBODIES POTENTIALLY USEFUL FOR AUTOLOGOUS BONE MARROW TRANSPLANTATION IN CHRONIC MYELOGENOUS LEUKEMIA

We developed two complement-fixing MoAbsHIMand HIM(murine)that were specifically reac-tive with chronic myelogenous leukemia (CML) cells.They were capable of fixing human or rabbit com-plement and suitable for CML cells purging of re-mission marrow from CML patients.HIMreactedwith majority leukemic cells form 7 out of 10 CMLpatients by complement-mediated cytotoxicity(C’MC)assay(positive cells 80%—90%),HIMreacted withmajority CML cells from 4 out of 5 CML by C’MCassay(positive cells 80%—90%).Treatment withHIMor HIMand human C’was capable of lysing97% of K562,U937,HL-60 and CML cells in a 20fold excess of unrelated cells by indirect FITC+EBstain.Using limited dilution culture,incubation withHIMand C’produced 1.5 logs inhibition of growthin K562 cells,and 1.9 logs in U937 cells,and withHIMand C’produced 2.9 logs inhibition in HL-60cells and 3.0 logs in U937 cells.Both MoAbs cocktailwas shown 1.8 logs in K562 cells and 3.2 logs in U937cells.They were no suppression on the growth o

Research on Marketing Strategies of Product D—a Chronic Myelogenous Leukemia Drug for Pharmaceutical Company A

Objective To put forward some suggestions on the marketing strategies for chronic myelogenous leukemia in a pharmaceutical enterprise.Methods Based on the development status of the pharmaceutical industry and the SWOT analysis of a company’s product,the marketing strategies were formulated to provide theoretical basis for pharmaceutical enterprise to adapt to the new medical reform.Results and Conclusion Nowadays,due to fierce competition,in order to expand the new market,enterprises should implement the strategies of new products,centralized management and professional training.Meanwhile,the effective marketing strategies should be formulated and strictly carried out according to the conditions of the pharmaceutical company.

Overexpression of P-glycoprotein induces acquired resistance to imatinib in chronic myelogenous leukemia cells

Imatinib,a breakpoint cluster region(BCR)-Abelson murine leukemia(ABL) tyrosine kinase inhibitor(TKI),has revolutionized the treatment of chronic myelogenous leukemia(CML).However,development of multidrug resistance(MDR) limits the use of imatinib.In the present study,we aimed to investigate the mechanisms of cellular resistance to imatinib in CML.Therefore,we established an imatinib-resistant human CML cell line(K562-imatinib) through a stepwise selection process.While characterizing the phenotype of these cells,we found that K562-imatinib cells were 124.6-fold more resistant to imatinib than parental K562 cells.In addition,these cells were cross-resistant to second-and third-generation BCR-ABL TKIs.Western blot analysis and reverse transcription-polymerase chain reaction(RT-PCR) demonstrated that P-glycoprotein(P-gp) and MDR1 mRNA levels were increased in K562-imatinib cells.In addition,accumulation of [14C]6-mercaptopurine(6-MP) was decreased,whereas the ATP-dependent efflux of [14C]6-MP and [3H]methotrexate transport were increased in K562-imatinib cells.These data suggest that the overexpression of P-gp may play a crucial role in acquired resistance to imatinib in CML K562-imatinib cells.

Myeloid sarcoma presenting as a colon polyp and harbinger of chronic myelogenous leukemia

Myeloid sarcoma, also known as granulocytic sarcoma or chloroma is an unusual accumulation of malignant myeloid precursor cells in an extramedullary site, which disrupts the normal architecture of the involved tissue. It is known to occur more commonly in patients with acute myelogenous leukemia and less commonly in those with myelodysplastic syndrome and myeloproliferative neoplasm, such as chronic myelogenous leukemia. The most common sites of involvement include bone, skin and lymph nodes. However, rare cases have been reported in the gastrointestinal tract, genitourinary tract, or breast. Most commonly, a neoplastic extramedullary proliferation of myeloid precursors in a patient would have systemic involvement of a myeloid neoplasm, including in the bone marrow and peripheral blood. Infrequently, extramedullary disease may be the only site of involvement. It may also occur as a localized antecedent to more generalized disease or as a site of recurrence. Herein, we present the first case in the English literature of a patient presenting with an isolated site of myeloid sarcoma arising in the form of a colonic polyp which, after subsequent bone marrow biopsy, was found to be a harbinger of chronic myelogenous leukemia.

High expression of RbAp46 gene in patients with acute leukemia or chronic myelogenous leukemia in blast crisis

The retinoblastoma （Rb） suppressor associated protein 46 （ RbAp46 ） also named retinoblastoma binding protein 7 （RBBP7） was first identified as a protein in HeLa cells that binds to an Rb affinity column. RbAp46 has been shown to be a core component of the mSin3 histone deacetylase （HDAC） complex and NuRD （ a multi-subunit complex containing chromosome-remodeling activity）. 2 RbAp46 is also known as the histone acetyltransferase （HAT） type B subunit

Preliminary Research on the p53 Gene Rearrangements in the Evolution of Chronic Myelogenous Leukemia to Blast Crisis

DNA from 36 patients with chronic myelogenous leukemia (CML) at various clinical stages and 6 cases of acute leukemia was investigated for alterations of the p53 gene by Southern blot analysis.Rearrangements of the p53 gene were seen in 3 of 12 (25.00%) cases of blast crisis and accelerated phase (AP) of CML and in only one of 18 chronic phrase (CP),just as has been reported previously. Meanwhile,by restriction fragment length polymorphism (RFLP) analysis the Bgl II site polymorphism in the p53 gene was also found. The frequency in Chinese people detected here was 0.392,which was strikingly higher than that in some other countries(P<0. 001).These results suggested that the alterations of the p53 gene, for example,p53 rearrangements,were probably responsible for the progression of BC in some CML patients, and that the frequency of Bgl II polymorphism in the p53 gene might be related to the population distribution.

The role of RAS effectors in BCR/ABL induced chronic myelogenous leukemia

BCR/ABL is the causative agent of chronic myelogenous leukemia(CML).Through structure/function analysis,several protein motifs have been determined to be important for the development of leukemogenesis.Tyrosine177 of BCR is a Grb2 binding site required for BCR/ABL-induced CML in mice.In the current study,we use a mouse bone marrow transduction/transplantation system to demonstrate that addition of oncogenic NRAS(NRASG12D)to a vector containing a BCR/ABL^(Y177F)mutant“rescues”the CML phenotype rapidly and efficiently.To further narrow down the pathways downstream of RAS that are responsible for this rescue effect,we utilize well-characterized RAS effector loop mutants and determine that the RAL pathway is important for rapid induction of CML.Inhibition of this pathway by a dominant negative RAL is capable of delaying disease progression.Results from the present study support the notion of RAL inhibition as a potential therapy for BCR/ABL-induced CML.

Cryptococcal Meningitis in Patient with Chronic Myeloid Leukemia

Objective: This study aimed to report the case of a female patient with chronic myeloid leukemia affected by cryptococcal meningitis. Case report: ML, white, 48 years old, female sex, previously diagnosed with chronic myeloid leukemia that has been refractive to the use of imatinib and who has recently begun using nilotinib, was admitted complaining of sudden and disabling migraine in the last 1 month associated with asthenia, adinamia, anorexia, disinterest for daily activities, dizziness, nausea, and vomiting. She evolved with ataxia, and started to stroll with help and showed decrease of muscular strength in her upper limbs. She also presented episodes of decrease of consciousness, with look fixation, no respond to sound stimulation, and short-term hearing loss. The cerebrospinal fluid showed presence of Cryptococcus sp. and, therefore, we began treatment with intravenous liposomal amphotericin B in the dose of 3 mg/kg/day, for 6 weeks. A new cerebrospinal fluid analysis, at the end of treatment, also showed rare structures that are compatible with Cryptococcus sp. As sequelae, she continued with hearing loss in her right ear and enhancement in her right auditory canal, seen in the magnetic resonance imaging. After stabilization and clinical improvement, she was discharged. After 3 weeks, she was hospitalized again with degeneration of the condition, and died due to intracranial hypertension secondary to cryptococcal infection. Final Considerations: This report reinforces the need of reflecting on fungi pathologies, especially in immunosuppressant patients, as well as the importance of early diagnosing and making a fast intervention, with the aims of providing quality of life and comfort to the patient and of minimizing neurological sequelae to the patient.

Predictive indicators of successful tyrosine kinase inhibitor discontinuation in patients with chronic myeloid leukemia

Clinical trials have demonstrated that some patients with chronic myeloid leukemia(CML)treated for several years with tyrosine kinase inhibitors(TKIs)who have maintained a molecular response can successfully discontinue treatment without relapsing.Treatment free remission(TFR)can be reached by approximately 50%of patients who discontinue.Despite having similar levels of deep molecular response and an identical duration of treatment,the factors that influence the successful discontinuation of CML patients remain to be determined.In this review we will explore the factors identified to date that can help predict whether a patient will successfully achieve TFR.We will also discuss the need for the identification of predictive biomarkers associated with a high probability of achieving TFR for the future personalized identification of patients who are suitable for the discontinuation of TKI treatment.

β-谷甾醇通过诱导ROS累积造成氧化应激抑制K562/ADR细胞增殖并促进凋亡和分化

目的:探讨β-谷甾醇抑制耐阿霉素人类髓性白血病细胞K562/ADR增殖、促进细胞凋亡与分化的效果及其可能机制。方法:使用细胞毒性试验计算β-谷甾醇对K562/ADR细胞的半数抑制率(IC50),采用CCK-8法检测细胞增殖率,采用流式细胞术检测细胞凋亡率与线粒体膜电位下降率,使用分光光度法检测细胞上清中SOD活力与MDA含量,使用荧光试剂盒检测细胞ROS强度,使用联苯胺染色检测红细胞分化程度,使用蛋白质印迹(Western blot)检测珠蛋白转录因子1(GATA-1)、β-珠蛋白(β-globin)和核因子e2相关因子2(NF-E2)蛋白表达水平。结果:β-谷甾醇对K562/ADR细胞的半数抑制浓度的IC50为163.64μmol/L。与空白组相比,3个浓度的β-谷甾醇均能抑制细胞增殖、促进细胞凋亡与红细胞分化,降低SOD活力、线粒体膜电位,增加MDA与ROS含量,升高GATA-1、β-globin和NF-E2蛋白表达水平(P<0.01)。结论:β-谷甾醇能抑制K562/ADR细胞增殖,促进细胞凋亡,并且诱导红细胞分化,其机制可能是通过促进ROS积累引起氧化应激失衡。

塞利尼索联合伊马替尼对K562/G01细胞的增殖及凋亡的影响

目的观察塞利尼索(selinexor,SEL)联合伊马替尼(imatinib,IM)对人慢性髓原白血病细胞耐伊马替尼(K562/G01,KG)细胞株的增殖及凋亡的影响,探索其可能的作用机制。方法分别用IM、SEL单独或联合处理人慢性髓系白血病(K562)细胞株及KG细胞株,采用MTT法检测细胞活力,流式细胞术检测细胞凋亡率,RT-PCR法检测细胞的BCR-ABL mRNA表达,Western blotting法检测细胞的XPO1蛋白表达。结果IM、SEL均可抑制K562细胞和KG细胞的增殖,作用48 h的半数抑制浓度IC50分别为IM(0.16μmol/L vs.6.48μmol/L),SEL(132.0 nmol/L vs.275.9 nmol/L);SEL联合IM作用于KG细胞,与单用相比,可明显抑制KG细胞的增殖(P<0.05),促进KG细胞的凋亡(P<0.05),降低KG细胞BCR-ABL mRNA(P<0.05),抑制KG细胞XPO1的表达(P<0.05)。结论SEL联合IM可协同抑制KG细胞的增殖并诱导其凋亡,进而抑制BCR-ABL mRNA和XPO1蛋白的表达,发挥抗白血病作用。

糖酵解参与调控楝酰胺抑制慢性粒细胞白血病细胞增殖的研究

本研究旨在探讨糖酵解参与楝酰胺的抗慢性粒细胞白血病细胞活性及机制。研究发现,楝酰胺以时间和浓度依赖性抑制K562细胞的生长增殖,其作用于K562细胞3 d的IC 50为21.70±5.68 nmol/L。楝酰胺阻滞K562细胞于G2/M期,诱导出现凋亡。楝酰胺降低了K562细胞的葡萄糖消耗量和乳酸生成水平,抑制c-Myc和己糖激酶2(hexokinase 2,HK2)的蛋白表达。K562细胞在进行去葡萄糖处理后生长减慢,乳酸生成水平降低,c-Myc蛋白表达下调。楝酰胺在无葡萄糖培养下K562细胞上的抑制率明显低于含葡萄糖培养下K562细胞上的抑制率。以上结果说明楝酰胺具有抗慢性粒细胞白血病细胞活性,其作用机制可能是抑制c-Myc和HK2介导的糖酵解。

miR-103a-3p对慢性粒细胞白血病细胞增殖和凋亡影响

目的检测miR-103a-3p在慢性粒细胞白血病(CML)病人骨髓组织中的表达,探讨miR-103a-3p对CML细胞增殖、凋亡的影响。方法收集32例CML病人和20例健康供者的骨髓标本,采用实时荧光定量PCR(RT-qPCR)检测miR-103a-3p表达。采用CCK8法和流式细胞术检测CML细胞系K562细胞增殖及凋亡的变化;采用免疫印迹法(Western blot)检测K562细胞中凋亡相关蛋白Bcl-2相关X蛋白(Bax)和B淋巴细胞瘤-2基因(Bcl-2)表达;小鼠皮下注射K562细胞,通过苏木精-伊红(HE)染色观察组织病理变化。结果与健康供者相比,miR-103a-3p在CML病人的骨髓单个核细胞中的表达量显著降低(t=3.317,P<0.01);K562细胞中的miR-103a-3p表达水平也显著低于正常人骨髓基质细胞HS-5(t=21.430,P<0.001)。体外实验显示,转染agomiR-103a-3p后,K562细胞的增殖受到抑制(t=4.949~12.170,P<0.01),凋亡增强(t=3.181,P<0.05)。成瘤实验显示,Lv-miR-up组小鼠的肿瘤质量较Lv-miR-NC组低(t=4.518,P<0.01),肿瘤体积较Lv-miR-NC组小(t=15.670~36.290,P<0.001)。结论miR-103a-3p可抑制CML细胞K562的增殖,促进其凋亡。

氟马替尼在一、二线治疗失败的慢性髓系白血病患者中的疗效及安全性分析

目的:分析我国自主研发的第二代酪氨酸激酶抑制剂(TKI)氟马替尼对一、二线治疗失败的慢性髓系白血病慢性期(CML-CP)患者的疗效及安全性。方法:回顾性收集2020年1月至2022年9月连云港市第一人民医院采用氟马替尼治疗的30例CML-CP患者的临床资料,其中15例曾接受伊马替尼一线治疗且治疗失败的患者作为二线组,另外15例采用尼洛替尼或达沙替尼二线治疗失败的患者作为三线组;统计分析两组患者治疗3、6和12个月时的血液学、分子学反应,以及至随访终点患者的无事件生存(EFS)和不良反应发生情况。结果:二线组治疗3、6和12个月时获得主要分子学反应(MMR)分别有10、11、12例患者,均高于三线组的3、4、5例患者(P=0.010,P=0.011,P=0.010)。二线组患者治疗3个月时获完全血液学反应(CHR)、早期分子学反应(EMR)分别有12、13例,高于三线组患者的9、13例,但两组差异无统计学意义(P=0.232,P=1.000);治疗6和12个月时二线组获得MR4.5的患者分别有6、7例,高于三线组的3、2例,但差异无统计学意义(P=0.427,P=0.713)。二线组患者治疗期间出现的血液学不良反应主要为1-2级血小板减少和贫血,未出现3-4级不良反应;三线组中1-2级血小板减少2例,1-2级贫血及白细胞减少各3例,3-4级贫血1例、中性粒细胞减少2例。二线组非血液学不良反应为皮疹(2例)、头痛(1例)、腹泻(1例)、疲乏(1例)、四肢疼痛(1例),三线组腹泻、恶心、水肿各1例。两组患者在血液学不良反应及非血液学不良反应方面均无统计学意义(P>0.05)。截止随访时,二线组患者的EFS率高于三线组(100%vs 93.3%,P=0.317)。结论:我国自主研发的二代TKI氟马替尼对一、二线治疗失败的CML-CP患者具有良好的疗效及安全性。

慢性粒细胞白血病患者减量至停用酪氨酸激酶抑制剂的临床分析

目的观察分析采用酪氨酸激酶抑制剂(TKI)治疗的慢性粒细胞白血病(CML)患者达到停药标准后停药的临床表现及转归情况。方法回顾性分析2015年1月1日至2017年12月31日在华中科技大学协和深圳医院血液科治疗并长期随访的达标的44例CML患者停用TKI的临床资料,观察这些患者停药后获得无治疗缓解的情况及其影响因素。结果44例患者累积接受TKI治疗的中位时间为59.5(37,102)个月;其中40例患者有减量史;所有患者停药前均获得主要分子学缓释(MMR)及以上的疗效。停药后中位随访15(5,30)个月,34例(77.27%)患者获得长期无治疗缓释状态(TFR);10例(22.73%)患者失去MMR。10例失去MMR的患者再启动药物治疗,其中8例重启后已获得MMR以上疗效。采用Kaplan-Meier法对44例患者停药前的临床特征进行单因素分析,34例患者最终获得TFR,10例停药后出现复发情况,复发率为29.41%。单因素分析结果显示,两组患者性别、年龄、获得MMR时间、Sokal评分等因素比较,差异均无统计学意义(P>0.05);停药前MMR维持时间<24个月患者的复发率与停药前MMR维持时间≥24个月患者的复发率比较,差异有统计学意义(P<0.05)。logistic回归模型进行多因素分析结果显示,停药前MMR维持时间<24个月(β=0.519,OR=2.951,95%CI=1.187~7.526)是CML患者分子学复发的独立危险因素(P<0.05)。结论CML患者需要达到停药标准后才能够保证停用TKI,且停药前的MMR维持时间越长,患者在停药后的复发率越低。

慢性粒细胞白血病患者的妊娠管理

随着慢性粒细胞白血病患者生存率的显著提高,越来越多的人要求解决与生活密切相关的生育问题,这也为慢性粒细胞白血病患者的妊娠管理提出挑战。尽管酪氨酸激酶抑制剂应用于慢性粒细胞白血病患者的临床治疗中,其安全性和有效性是毋庸置疑的,但该药对生育的影响和致畸作用限制了该药在妊娠中的应用,白细胞分离、干扰素和羟基脲等治疗方式成为妊娠期间慢性粒细胞白血病患者的另一个选择。在选择最佳的妊娠时机时,应该遵循个体化和多学科合作的原则,充分评估继续治疗对胎儿的危害和治疗中断对母亲的风险。通过本文综述,旨在为慢性粒细胞白血病患者的妊娠管理提供建议。

木犀草素对白血病K562/ADR细胞多药耐药的逆转作用及机制研究

目的 探究木犀草素(Lut)对慢性髓系白血病K562/ADR细胞多药耐药性的逆转作用及其机制。方法K562和K562/ADR细胞经不同浓度阿霉素(ADR)处理24 h后,采用CCK-8实验检测K562/ADR细胞耐药倍数。Lut单独或联合ADR作用K562/ADR细胞24 h后,采用CCK-8实验检测Lut的细胞毒性及对ADR的增敏作用。取对数生长期K562/ADR细胞分为0μmol/L Lut组、2μmol/L Lut组、4μmol/L Lut组,采用流式细胞术检测细胞内ADR蓄积量的变化;RT-PCR法和Western blot法分别检测核因子E2相关因子2(Nrf2)、多药耐药相关蛋白1(MRP1)、P-糖蛋白(P-gp)、谷胱甘肽-S-转移酶pi(GST-pi)mRNA和蛋白的表达;谷胱甘肽(GSH)试剂盒检测细胞内GSH的含量。结果 与K562细胞相比,K562/ADR细胞株对ADR具有明显的耐药性,耐药倍数为53.69倍。与0μmol/L Lut相比,不同浓度Lut作用于K562/ADR细胞后,细胞生长均受到不同程度的抑制(P<0.05),其中2、4μmol/L Lut对K562/ADR细胞的增殖抑制率<10%,为无毒性的Lut浓度。与0μmol/L Lut组相比,2、4μmol/L Lut组可明显增强ADR对K562/ADR的细胞增殖抑制率,增加细胞内ADR蓄积量,提高逆转耐药倍数,降低细胞内GSH含量,下调细胞中MRP1、P-gp、GST-pi、Nrf2 mRNA及蛋白的表达(P<0.05);且4μmol/L Lut作用效果较2μmol/L Lut更显著。结论Lut可抑制K562/ADR细胞增殖,逆转其对ADR的耐药性,其机制可能与Lut下调Nrf2、MRP1、P-gp、GST-pi表达,进而增加细胞内ADR蓄积量有关。

Circ_0013745靶向调控miR-126-5p对慢性髓系白血病细胞K562的迁移、侵袭和增殖的影响

目的探讨circ_0013745靶向调控miR-126-5p对慢性髓系白血病(CML)细胞K562增殖和侵袭的影响。方法收集2019年7月—2021年1月在合肥市第一人民医院诊断治疗的CML患者与健康捐赠者外周血样本30对,利用实时荧光定量PCR(RT-qPCR)检测CML患者中circ_0013745表达量。通过平板克隆实验和细胞计数试剂盒8(Cell counting kit-8,CCK-8)检测circ_0013745对K562细胞增殖能力的影响。Transwell实验检测K562细胞的迁移和侵袭能力。Starbase数据库预测与circ_0013745结合的miRNA,通过双荧光素酶报告系统验证circ_0013745是否与miR-126-5p结合,并分为mimic NC与circ_0013745-WT/circ_0013745-MUT共转染组、miR-126-5p mimic与circ_0013745-WT/circ_0013745-MUT共转染组。通过挽救实验对细胞增殖能力进行检测。结果RT-qPCR检测结果显示,CML患者的外周血中circ_0013745的表达量显著高于健康人表达量(t=7.369,P<0.001)。平板克隆实验结果显示,si-circ_0013745组的K562细胞克隆个数较si-NC组的细胞克隆个数显著降低(P<0.001)。CCK-8增殖实验结果显示,si-circ_0013745组细胞增殖能力较si-NC组细胞增殖能力显著降低(t=8.413,P<0.01)。Transwell迁移实验结果显示,si-circ_0013745组细胞迁移能力低于si-NC组迁移能力(t=7.739,P<0.01)。Transwell侵袭实验结果显示,si-circ_0013745组的侵袭细胞个数较si-NC组显著降低(t=4.679,P<0.01)。Starbase数据库分析结果显示,miR-126与circ_00137453’UTR结合。双荧光素酶报告基因实验显示,与NC组比较,miR-126-5p mimic与circ_0013745-WT共转染组的荧光素酶活性显著降低(t=11.130,P<0.001),而miR-126-5p mimic与circ_0013745-Mut共转染组的荧光素酶活性无明显变化(t=0.316,P>0.05)。敲除circ_0013745后,miR-126-5p的表达量显著上升(P<0.001)。挽救实验结果显示,与si-circ_0013745组细胞增殖率比较,si-circ_0013745+miR-126-5p inhibitor组细胞增殖率增高(t=7.175,P<0.01)。结论Circ_0013745靶向调控miR-126-5p促进CML细胞K562的迁移、侵袭和增殖能力。