A Construction of Object Detection Model for Acute Myeloid Leukemia

The evolution of bone marrow morphology is necessary in Acute Mye-loid Leukemia(AML)prediction.It takes an enormous number of times to ana-lyze with the standardization and inter-observer variability.Here,we proposed a novel AML detection model using a Deep Convolutional Neural Network(D-CNN).The proposed Faster R-CNN(Faster Region-Based CNN)models are trained with Morphological Dataset.The proposed Faster R-CNN model is trained using the augmented dataset.For overcoming the Imbalanced Data problem,data augmentation techniques are imposed.The Faster R-CNN performance was com-pared with existing transfer learning techniques.The results show that the Faster R-CNN performance was significant than other techniques.The number of images in each class is different.For example,the Neutrophil(segmented)class consists of 8,486 images,and Lymphocyte(atypical)class consists of eleven images.The dataset is used to train the CNN for single-cell morphology classification.The proposed work implies the high-class performance server called Nvidia Tesla V100 GPU(Graphics processing unit).

CLAG-M chemotherapy followed by umbilical cord blood stem cell transplantation for primary refractory acute myeloid leukaemia in a child:A case report

BACKGROUND The prognosis of paediatric primary refractory/relapsed acute myeloid leukaemia(R/R AML)remains poor.Intensive therapy is typically used as salvage treatment for those with R/R AML.No data are currently available about the use of the CLAG-M protocol as salvage therapy in paediatric patients with R/R AML.CASE SUMMARY An 8-year-old patient was diagnosed with acute myeloid leukaemia by bone marrow morphology and immunophenotype.The patient showed poor response to two cycles of induction therapy with 60%blast cells in the bone marrow after the second induction cycle.The patient achieved complete remission after being treated with the CLAG-M protocol as salvage therapy before undergoing umbilical cord blood stem cell transplantation.Morphological complete remission with haematological recovery has hitherto been maintained over 4 mo.Abnormal gene mutations detected at diagnosis were undetectable after haematopoietic stem cell transplantation.CONCLUSION Here we present a paediatric patient with primary refractory acute myeloid leukaemia who was successfully treated with the CLAG-M protocol.Given the positive results of the presented patient,large-scale clinical studies are required to assess the role of the CLAG-M protocol in the salvage treatment of refractory or relapsed AML in childhood.

Chronic myeloid leukaemia presenting as acute small bowel gangrene:A case report

Rationale:Chronic myeloid leukaemia is a myeloproliferative disorder due to clonal hyperproliferation of myeloid cells within the bone marrow.It can present both pro-and anti-thrombotic states.CML has different presentations within the gastrointestinal tract.Patient’s concern:A 40-year-old non-diabetic and non-hypertensive male complained of abdominal pain with nausea and emesis for 1 day.Besides,he had a history of abdominal distension and fever for 1 day.Diagnosis:Acute small bowel gangrene due to chronic myeloid leukaemia.Intervention:A limited resection of small intestine with ileostomy and mucus fistula.Outcome:After 3 months following surgery the patient underwent stoma closure.The patient was followed up for more than 3 years postoperatively.During the follow-up,the patient was asymptomatic without any recurrence of the disease.Lesson:Chronic myeloid leukaemia should be considered as one of the causes for small intestine gangrene when there is increased leukocyte count,splenomegaly without evidence of atherosclerotic occlusion or systemic emboli from the heart.

Parametric and Non-Parametric Survival Analysis of Patients with Acute Myeloid Leukemia (AML)

Background: Acute Myeloid leukemia (AML) is the most prominent acute leukemia in adults. In the United States, we experience over 20,000 cases per year. Over the past decade, improvements in the diagnosis of subtypes of AML and advances in therapeutic approaches have improved the outlook for patients with AML. However, despite these advancements, the survival rate among patients who are less than 65 years of age is only 40 percent. Purpose: The purpose of the paper is to study if there exists any significant difference in the survival probabilities of male and female AML patients. Also, we want to investigate if there is any parametric probability distribution that best fits the male and female patient survival and compare the survival probabilities with the non-parametric Kaplan-Meier (KM) method. Methods: We used both parametric and non-parametric statistical methods to perform the survival analysis to assess the survival probabilities of 2015 patients diagnosed with AML. Results: We found evidence of a statistically significant difference between the mean survival time of male and female patients diagnosed with AML. We performed parametric survival analysis and found a Generalized Extreme Value (GEV) distribution best fitting the data of the survival time for male and female patients. We then estimated the survival probabilities and compared them with the frequently used non-parametric Kaplan-Meier (KM) survival method. Conclusion: The comparison between the survival probability estimates of the two methods revealed a better survival probability estimate by the parametric method than the Kaplan-Meier. We also compared the median survival time of male and female patients individually with descriptive, parametric, and non-parametric methods of analysis. The parametric survival analysis is more robust and efficient because it is based on a well-defined parametric probabilistic distribution, hence preferred over the non-parametric Kaplan-Meier estimate. This study offers therapeutic significance for further enhancement to treat patients with Acute Myeloid Leukemia.

Sunitinib Reduces Acute Myeloid Leukemia Clonogenic Cells in Vitro and Has Potent Inhibitory Effect on Sorted AML ALDH+ Cells

Sunitinib is an orally administered, multi-target tyrosine kinase inhibitor that has been approved by the FDA for the treatment of renal cell carcinoma and imatinib resistant gastro-intestinal tumors. Anti-leukemic activity of sunitinib has been examined in early clinical trials with limited success. However, recent trials on acute myeloid leukemia (AML) patients carrying FLT3 mutations have shown promising results. Effects of sunitinib on leukemic clonogenic cells and potential leukemic stem cells have not been examined so far. We analyzed the anti-proliferative and apoptotic properties of sunitinib on AML-derived cell lines. We also tested the effect of sunitinib on AML patient derived clonogenic cells (AML-CFC), as well as flow-sorted potential leukemic progenitors. Peripheral blood or bone marrow samples were obtained from newly diagnosed AML patients and flow sorted for CD34+ CD133+ or ALDH+ cells. Umbilical cord blood derived CD34+ cells were used as normal controls. Sunitinib induced growth arrest and apoptosis in AML derived cell lines. In addition, 7 μM sunitinib induced 75% reduction of AML-CFC as compared to DMSO treated control (±6.79%;n = 4). In contrast, 7 μM sunitinib treatment of umbilical cord blood derived normal CD34+ cells showed 29% reduction in AML-CFC (±6.77%;n = 5). Treatment of ALDH+ cells sorted from 2 AML cases and CD34+ CD133+ cells from one patient showed reduction of AML-CFC on treatment with sunitinib. Our study highlighted a potent anti-proliferative and proapoptotic effect of sunitinib on AML cell lines, AML patient derived clonogenic cells and potential leukemic stem cells.

Resveratrol-downregulated Phosphorylated Liver Kinase B1 Is Involved in Senescence of Acute Myeloid Leukemia Stem Cells

Summary： Senescence is an important obstacle to cancer development. Engaging a senescent response may be an effective way to cure acute myeloid leukemia （AML）. The aim of this study was to examine the effect of resveratrol-downregulated phosphorylated liver kinase B1 （pLKB1） on the senescence of acute myeloid leukemia （AML） stem cells. The protein expressions of pLKB 1 and Sirtuin 1 （SIRT1）, a regulator ofpLKB1, were measured in CD34＋CD38-KGla cells treated with resveratrol （40 μmol/L） or not by Western blotting. Senescence-related factors were examined, including p21 mRNA tested by real-time PCR, cell morphology by senescence-associated β-galactosidase （SA-β-gal） staining, cell pro- liferation by MTT assay and cell cycle by flow cytometry. Besides, apoptosis was flow cytometrically determined. The results showed that pLKB1 was highly expressed in CD34＋CD38- KGla cells, and resveratrol, which could downregulate pLKB1 through activation of SIRT1, induced senescence and apoptosis of CD34＋CD38- KGla cells. It was concluded that resveratrol-downregulated pLKB1 is in- volved in the senescence of AML stem cells.

Cutaneous Symptoms Revealing M5 Acute Myeloid Leukemia: A Case Report

Cutaneous presentation revealing acute myeloid leukemia (AML) is rare, and the prognosis is poor. We report a case of an 11-month-old male who presented with cutaneous lesions present as diffuse purplish papulo-nodular lesions, revealing M5 acute myeloid leukemia. Skin biopsy and immunohistochemical examination, combined with routine blood analysis and bone marrow examination, contributed to early diagnosis. However, despite intensive chemotherapy treatment, the prognosis was poor and death occurred during the first months of treatment.

Rare myeloid sarcoma/acute myeloid leukemia with adrenal mass after allogeneic mobilization peripheral blood stem cell transplantation

Myeloid sarcoma(MS)is a rare hematological neoplasm that develops either de novo or concurrently with acute myeloid leukemia(AML).This neoplasm can also be an initial manifestation of relapse in a previously treated AML that is in remission.A 44-year-old male patient was diagnosed with testis MS in a local hospital in August 2010.After one month,bone marrow biopsy and aspiration confirmed the diagnosis of AML.Allogeneic mobilization peripheral blood stem cell transplantation was performed,with the sister of the patient as donor,after complete remission(CR)was achieved by chemotherapy.Five months after treatment,an adrenal mass was detected by positron emission tomography-computed tomography(PET-CT).Radiotherapy was performed for the localized mass after a multidisciplinary team(MDT)discussion.The patient is still alive as of May 2013,with no evidence of recurrent MS or leukemia.

Analyses of therapeutic effects using rludarabine and cytarabine on acute myeloid leukemia at different stages during treatment

Objective: To evaluate the therapeutic effect of the fludarabine and cytarabine (FA) regimen on acute myeloid leukemia (AML) at different phases during treatment. Methods: A total of 185 patients with AML were divided into 4 groups based on the outcome of previous treatments. Patients in Group 1 had no remission after the first course of induction chemotherapy (n = 55). Patients in Group 2 had no remission after no less than two courses of induction chemotherapy (n = 41). Patients in Group 3 had early relapse (n = 40). Patients in Group 4 had late relapse (n = 49). Patients in groups 2, 3 and 4 had refractory AML or AML with relapse. We assessed the efficacy and toxicity of FA combination chemotherapy in each of these 4 groups. Results: The complete remission (CR) rates of Groups 1, 2, 3 and 4 were 74.5% (41/55), 45.9% (19/41), 17.5% (7/40) and 38.8% (19/49), respectively. The CR rate was higher in Group 1 than in the other 3 groups (34.6%, 45/130) (P = 0.000). A significant correlation was found between CR rate and the number of chemotherapeutic courses (P = 0.023). The main adverse reactions included bone marrow suppression and secondary infection. Conclusion: FA regimen is a good choice for patients with AML, especially those who have failed to achieve CR after the first course of induction chemotherapy.

Clinical Efficacy of Decitabine/Azacitidine in Combination with HAG in the Treatment of Elderly Patients with Acute Myeloid Leukemia

This study was conducted to investigate the clinical effect of combining decitabine/azacitidine with HAG in the treatment of single elderly patients with acute myeloid leukemia.Patients in Shaanxi Provincial People’s Hospital were selected for this study from January 2020 to January 2022,and all of the patients were elderly patients with acute myeloid leukemia.Around 23 patients were selected for this study,subsequently the patients were divided into two groups;Group A contained 11 patients and was given decitabine in combination with HAG;and Group B contained 12 patients,and was given azacitidine in combination with HAG.This study showed that the treatment effective rates of patients in both groups were 90.91%and 58.33%,respectively,with a small difference(p>0.05)in the data comparison.The incidence of adverse reactions in the two groups was 63.64%and 16.67%,respectively,with the incidence in group B is significantly(p<0.05)lower compared with group A.Meanwhile,compared with group B,patients in group A had a significantly(p<0.05)shorter mean time to WBC normalization,higher HB and PLT levels,lower WBC levels were lower,all the survival duration times were longer,and subpopulation indicators of peripheral blood T lymphocytes were more in line with normal values.In summary,this study demonstrated that the combination of azacitidine and HAG therapies for the treatment of elderly patients with acute myeloid leukemia is more effective,furthermore can reduce significantly the incidence of adverse treatment effects in patients.

维奈克拉方案治疗复发/难治性急性髓系白血病的临床研究

目的:评价维奈克拉(venetoclax,VEN)快速剂量递增、最长治疗时间为14天,联合低剂量阿糖胞苷(low-dose cytarabine,LDAC)方案挽救治疗复发/难治性急性髓系白血病(relapsed/refractory acute myeloid leukemia,R/RAML)的安全性和有效性。方法:回顾性分析2018年10月至2023年11月于江苏大学附属医院接受VEN+LDAC方案挽救治疗的16例R/R AML患者,所有患者既往均未接受过含VEN方案治疗。该方案VEN的剂量第1天为200 mg,其后均为400 mg固定剂量;LDAC 20 mg/m^(2)/d皮下注射。患者在治疗第8天复查骨髓,根据骨髓增生情况决定总疗程为10天还是14天。所有患者均不给予VEN单药治疗。有治疗反应的患者采用相同方案维持直到疾病进展或移植。结果:本研究纳入的R/R AML患者,中位随诊时间为27.5个月。治疗期间未发生有临床表现的肿瘤溶解综合症(tumor lysis syndrome,TLS)。治疗后总反应率(overall response rate,ORR)为68.75%,其中4例达完全缓解(complete response,CR),1例达血液学未恢复的完全缓解(CR with incomplete hematologic recovery,CRi),6例达部分缓解(partial response,PR)。达最佳疗效的治疗周期中位数为1个周期。中位总生存期(overall survival,OS)为5.8(0.5~47.2)个月,中位无进展生存期(progression-free survival,PFS)为22.2(7.3~42.9)个月。发生的不良反应主要为3~4级的血液学不良事件和感染。结论:本研究根据治疗第8天骨髓复查结果调整用药天数的VEN+LDAC方案,对于既往没有接受过含VEN方案治疗的R/R AML患者有较好的安全性和有效率。即使14天的VEN+LDAC治疗也是安全的。

甘草查尔酮A对HL-60细胞恶性生物学行为的抑制作用及其机制

目的 探究甘草查尔酮A(LA)对急性髓系白血病(AML)细胞HL-60的作用及其机制。方法 将人AML细胞系HL-60细胞分为对照组、LA组(30μmol/L)、IL-6组(100 ng/mL,JAK2/STAT3信号通路激活剂)和LA+IL-6组。培养48 h后,采用MTT法和克隆形成实验检测HL-60细胞增殖活性;采用流式细胞术检测HL-60细胞周期分布和细胞凋亡;采用Transwell实验检测HL-60细胞侵袭和迁移;采用Western blot检测p21、p27、cyclin E2、CDK2、Bcl-2、Bax、cleaved-Caspase-3、p-JAK2,JAK2,p-STAT3和STAT3蛋白表达水平。结果 与对照组比较,LA组细胞活力、克隆形成数、侵袭和迁移细胞数均降低(P<0.05),Bcl-2、cyclin E2和CDK2蛋白表达量均降低(P<0.05),JAK2和STAT3蛋白的磷酸化水平均降低(P<0.05);G0/G1期细胞比例和细胞凋亡率均升高(P<0.05),p21、p27、Bax和cleaved Caspase-3蛋白表达量均升高(P<0.05)。与对照组比较,IL-6组细胞活力、克隆形成数、侵袭和迁移细胞数均升高(P<0.05),Bcl-2、cyclin E2和CDK2蛋白表达量均升高(P<0.05),JAK2和STAT3蛋白的磷酸化水平均升高(P<0.05),G0/G1期细胞比例和细胞凋亡率均降低(P<0.05),p21、p27、Bax和cleaved Caspase-3蛋白表达量均降低(P<0.05)。与IL-6组比较,LA+IL-6组细胞活力、克隆形成数、侵袭和迁移细胞数均降低(P<0.05),Bcl-2、cyclin E2和CDK2蛋白表达量均降低(P<0.05),JAK2和STAT3蛋白的磷酸化水平均降低(P<0.05),G0/G1期细胞比例和细胞凋亡率均升高(P<0.05),p21、p27、Bax和cleaved-Caspase-3蛋白表达量均升高(P<0.05)。LA+IL-6组和LA组间上述指标差异没有统计学意义。结论 甘草查尔酮A可抑制AML细胞系HL-60细胞增殖、侵袭和迁移,诱导细胞凋亡并将细胞阻滞在G0/G1期,其作用机制可能与抑制JAK2/STAT3信号通路激活有关。

蛋白精氨酸甲基转移酶5表达与非M3型急性髓系白血病疗效关系的临床观察

目的讨论蛋白精氨酸甲基转移酶5(PRMT5)与急性髓系白血病(AML)患者低甲基化药物(HMA)治疗敏感性的关系。方法通过GEPIA和TCGA数据库分析AML患者PRMT5表达及其与AML患者生存的关系。收集2020年1月至2023年10月收治的81例AML患者,包括50例非M3型患者和31例M3型患者。采用实时荧光定量PCR(qPCR)检测骨髓样本中PRMT5表达。采用全基因组重亚硫酸盐测序(WGBS)检测基因组甲基化水平。结果TCGA数据库中AML患者PRMT5表达显著高于健康对照人群(P<0.01);PRMT5高表达组患者总生存期更短(P=0.036)。进一步分析TCGA数据库,巩固期给予HMA后,PRMT5表达对无事件生存率(EFS)和OS的有明显影响(P<0.010)。81例新诊断AML患者PRMT5表达显著高于23例健康志愿者[3.25(1.69,5.16)vs.1.00(0.72,1.35),P<0.001]。非M3型AML患者PRMT5表达高于M3型患者[4.51(2.05,7.25)vs.2.01(1.53,3.35),(P<0.001)]。在非M3型AML患者中,PRMT5高表达与BM原始细胞百分率以及不良基因突变和高危患者比例更高有关(P<0.05)。与未接受HMA治疗患者比较,接受HMA治疗的PRMT5高表达非M3型AML患者CR率显著增加(P=0.003)。通过WGBS测序,PRMT5高表达组CpG岛甲基化比率以及转录起始位点、转录终止位点CpG岛甲基化比率高于PRMT5低表达组(P<0.001)。结论在非M3型AML患者中PRMT5高表达,PRMT5高表达预示着更多非M3型AML患者从HMA治疗中获益。PRMT5可能是评估肿瘤甲基化富集和预测疾病预后的潜在生物标志物。

造血干细胞移植治疗老年髓系肿瘤的临床分析

目的:探讨造血干细胞移植(hematopoietic stem cell transplantation,HSCT)对老年髓系肿瘤患者生存结局的影响。方法:回顾性分析2018年1月至2023年5月于南方医科大学附属珠江医院54例接受HSCT且年龄≥55岁髓系肿瘤患者的治疗结局。结果:54例患者中急性髓系白血病(acute myeloid leukemia,AML)患者45例,骨髓增生异常综合征患者9例,中位年龄57.5(55.0~68.0)岁。53例成功造血重建,中性粒细胞植入中位时间为13(8~24)天,血小板植入中位时间为15(9~75)天。急性移植物抗宿主病(graft-versus-host diseas,GVHD)累积发生率23.3%,3年慢性GVHD累积发生率24.6%。中位随访时间28.2个月,3年累积复发率(cumulative relapse rates,CIR)18.0%,3年非复发死亡率28.3%。3年无复发生存(relapse-free survival,RFS)率为58.2%,3年总生存(overall survival,OS)率为56.5%。结论:HSCT是老年髓系肿瘤患者获得长期生存的有效、安全的治疗手段。

地西他滨联合改良CAG方案治疗AML1-ETO阳性复发、难治急性髓系白血病的临床研究

本研究旨在分析AML1-ETO阳性复发、难治急性髓系白血病的临床特点及地西他滨联合改良CAG方案对该类白血病患者的治疗效果及副作用。回顾性分析2013年1月至8月5例AML1-ETO阳性复发、难治急性髓系白血病,并分析临床特点,包括年龄、性别、初诊时伴随症状、外周血和骨髓特点等;同时分析地西他滨联合改良的CAG方案对该类患者的治疗效果和副作用。5例患者中复发2例,难治合并复发3例,初治时白细胞中位数12.55(7.8-66.55)×109/L、血小板中位数44(20-72)×109/L,血红蛋白中位数110(77-128)g/L、乳酸脱氢酶中位数312.9(123.6-877.8)μ/L。治疗结果表明:经过1个疗程地西他滨联合改良的CAG方案治疗后4例完全缓解,1例未缓解,总缓解率为80%;治疗的副作用主要为骨髓抑制,1例未缓解经FLAG方案治疗后在移植动员过程中突发心衰死亡。结论:初步结果表明AML1-ETO阳性复发、难治急性髓系白血病经本方案治疗后,其缓解率比较高、并发症较少,值得进一步研究和在临床推广应用。

AML-1/ETO基因相关的AML-M_2型白血病免疫表型分析

本研究探讨AML/ETO基因重排的FAB分型为AML-M2患者的骨髓免疫表型的特征和预测性,以及与急性早幼粒白血病(APL)的区别。应用流式细胞术分析17例经荧光原位杂交(FISH)检测AML-1/ETO融合基因阳性、FAB分型为AML-M2(M2/ETO+)患者骨髓的免疫表型,并与34例AML-1/ETO阴性、FAB分型AML-M3、临床诊断为APL患者进行了比较。结果发现,17例M2/ETO+患者骨髓中均可见一群(15.89%-68.53%)原始细胞和一群SSC较高异质性的粒细胞。原始细胞表达干细胞相关抗原CD34、HLA-DR和髓系抗原CD33、CD13、MPO。在M2/ETO+患者中CD33表达强度显著低于APL患者(P<0.001),HLA-DR、CD19和CD34+CD56+共表达的阳性率均显著高于APL患者(P<0.001),而CD9的表达率则显著低于APL患者(P<0.001)。M2/ETO+患者粒细胞表达分化的髓系抗原CD11b和CD15,并可分为CD15+CD11b-和CD15+CD11b+两群,而成熟的粒细胞标志CD10均为阴性,与早幼粒细胞的表达图形相似。17例(100%)M2/ETO+患者的粒细胞均表达CD56,显著高于M3患者(6/34例,17.56%)。结论:AML-1/ETO基因重排的AML-M2型(FAB分型)白血病具有独特的免疫表型,对其基因重排有较高的预测性。应用多参数免疫分型技术可较容易地将M2/ETO+亚型白血病与APL鉴别。

地西他滨联合CAG方案治疗AML1-ETO^+ AML的临床效果

目的:观察AML1-ETO^+复发/难治急性髓系白血病患者经地西他滨联合CAG方案治疗的临床治疗效果。方法:收集2015年6月至2016年1月我院收治的8例AML1-ETO+复发/难治急性髓系白血病患者临床资料,分析患者入院一般资料及初诊伴随症状、骨髓特点等,同时分析患者经地西他滨联合CAG方案治疗的临床观察指标及不良反应。结果:8例患者中复发1例,难治合并复发7例,初治时白细胞23.57(7.5-65.29)×10~9/L、血小板40(19-69)×10~9/L,血红蛋白107(79-131)g/L、乳酸脱氢酶313.5(124.1-865.9)U/L。8例患者经地西他滨联合CAG方案1个疗程治疗后7例症状完全缓解,1例症状未缓解,总缓解率为87.5%;本方案的不良反应为骨髓抑制,1例症状未缓解患者经FLAG方案治疗后突发心衰死亡。结论:AML1-ETO^+复发/难治急性髓系白血病患者经地西他滨联合CAG方案治疗后,各临床观察指标较理想,缓解率较高,并发症较少。

CD56表达对伴有AML/ETO的急性髓系白血病患者预后影响的分析

目的:探讨CD56表达对伴有AML/ETO的急性髓系白血病患者的预后影响。方法:回顾性分析西安交通大学第一附属医院2012年1月至2016年12月60例伴有AML/ETO的初发AML患者临床资料,比较CD56^+阳性与阴性组的临床特征。结果:CD56^+与CD56^-2组患者在1个疗程诱导缓解治疗后CR率、1年复发率和基因突变率方面有明显的差异(P<0.05);CD56^+患者RFS和OS均低于CD56^-患者,差异有统计学意义(P<0.05)。结论:CD56^+可能是伴有AML/ETO的AML患者预后差的重要因素。

吉妥珠单抗治疗急性髓系白血病的疗效影响因素分析

急性髓系白血病(acute myeloid leukemia,AML)是一种异质性髓系恶性肿瘤,目前化疗联合造血干细胞移植是主要治疗方法,但是总体预后较差。吉妥珠单抗(gemtuzumab ozogamicin,GO)是一种人源化抗CD33单抗与卡奇霉素结合的抗体偶联药物,主要用于治疗CD33阳性AML。虽然研究发现GO可以改善CD33阳性AML患者的预后,但是仍有部分AML患者并未获益。GO治疗AML的疗效主要与CD33表达及单核苷酸多态性(single nucleotide polymorphism,SNP)、ATP结合盒亚家族B成员1(ATP-binding cassette subfamily B member 1,ABCB1)基因及SNP、特异的分子生物学和细胞遗传学等因素有关。本文就GO对AML疗效影响因素的研究进展进行综述。

急性髓系白血病新型预后分子标志物NKX2-3的发现

【目的】通过分析生物信息数据库中影响急性髓系白血病(AML)患者的预后的分子标志物的表达,为进一步探索AML预后的新型分子标志物提供实验基础。【方法】从癌症基因组图谱(TCGA)生物信息数据库中的179例AML患者的预后数据进行差异性基因分析及生存分析;利用基因表达集锦(GEO)数据库中的GSE13159数据集的74例健康人(HI)骨髓标本与542例AML初发患者骨髓标本进行分析,检测差异性目的基因表达水平在AML初发患者与健康人中的差异性;收集初发18例AML患者的外周血及骨髓样本,同时收集年龄和性别匹配的20例健康志愿者的样本作为对照,采用实时荧光定量PCR验证差异基因在AML患者体内的表达水平。【结果】生物信息数据分析显示,根据R语言计算出的NK2转录因子相关基因位点3(NKX2-3)的最佳截断值0.051进行生存分析,发现与低表达NKX2-3的AML初发患者相比,高表达NKX2-3的AML初发患者总体生存率较差(P=0.0036);与HI相比,NKX2-3在AML初发组患者中显著高表达(P<0.001);实时荧光定量PCR的验证结果也证实NKX2-3-1和NKX2-3-2在AML初发组患者中高表达,且与健康人组相比有显著相关性(P=0.000,P=0.000)。【结论】NKX2-3在AML初发组患者中高表达,且高表达NKX2-3的AML患者总体生存较差;NKX2-3可能与AML临床转归与预后密切相关。