Acute Promyelocytic Leukemia in Children: A Model of Precision Medicine and Chemotherapy-Free Therapy

Acute promyelocytic leukemia (APL) represents a paradigm of precision medicine. Indeed, in the last decades, the introduction of all-trans retinoic acid (ATRA) and arsenic trioxide (ATO) completely revolutionized the therapeutic approach to this previously highly fatal disorder. This entirely chemotherapy-free treatment, which provided excellent survival rates, has been initially validated in adults and, recently, translated in the pediatric setting. This review summarizes currently available data on the use of ATRA and ATO combination in pediatric APL, providing a particular focus on peculiar issues and challenges, such as the occurrence of pseudotumor cerebri and death during induction (early death), as well as the advantage offered by the ATO/ATRA combination in sparing long-term sequelae.     

三氧化二砷联合全反式维甲酸治疗初发急性早幼粒细胞白血病50例疗效观察

目的 观察三氧化二砷(ATO)联合全反式维甲酸(ATRA)治疗初发急性早幼粒细胞白血病(APL)的疗效.方法 98例初发APL患者分为对照组和治疗组,对照组48例,治疗组50例.对照组采用常规ATRA+DA双诱导方案治疗;治疗组采用ATRA每天25 mg/m2,ATO每天0.15 mg/kg(ATRA后第10天开始)联合治疗,直至完全缓解(CR),CR后接受ATO和ATRA联合巩固治疗.比较两组CR率、PML-RAR α融合基因转阴时间及5年无病生存率.结果 对照组和治疗组CR率分别为89.5%(43/48)和90.0%(45/50),获得CR时间分别为(30.0±5.1)d和(28.1±4.4)d,两组CR率(x2=-0.068,P=0.946)及获得CR时间(t=1.757,P=0.083)相比差异均无统计学意义.在所有获得CR的患者中,3例分别在CR后第276、385和394天复发.所有患者发病时PML-RAR α融合基因均阳性,对照组和治疗组CR时分别有25.0%(5/20)和29.4%(5/17)转阴,巩固后分别有92.5%(37/40)和97.6%(41/42)转阴.对照组和治疗组5年无病生存率分别为(85.3±5.9)%和(87.6±5.6)%,差异无统计学意义(x2=0.232,P=0.630).结论 ATO联合ATRA能有效治疗初发APL患者,可以作为常规化疗方案外的另一选择.     

复方黄黛片治疗急性早幼粒细胞白血病的系统评价

目的 评价复方黄黛片( CRNTT)治疗急性早幼粒细胞白血病(APL)的疗效与安全性。方法计算机检索SinoMed、CNKI、VIP、万方、CBA、PubMed、MEDLINE、EMBASE、Cochrane图书馆临床对照试验资料库,并辅以手工检索,收集国内外公开发表的CRNIT治疗APL的随机对照试验(RCT)文献,检索年限截至201 1年3月。按纳入标准与排除标准筛选文献并评价纳入研究的质量,以完全缓解(CR)率、达CR所需时间、复发率、病死率、不良反应率等为评价指标,采用RevMan 5.1软件进行Meta分析。结果纳入6项RCT,包括391例APL患者,其中2项RCT研究目的为CRNIT与三氧化二砷(ATO)的比较,4项RCT研究目的为CRNIT与全反式维甲酸(ATRA)的比较,其中1项RCT增设CRNIT+ ATRA与ATRA的比较。达CR所需时间：CRNIT比ATRA、ATO长[加权均数差(WMD)=3.14,95％CI 0.99 ～5.29,P=0.004];头痛发生率：CRNTT低于ATRA（OR=0.10,95％CI 0.02～0.45,P=0.003）;5年无病生存率：CRNIT优于ATRA（OR= 7.22,95％CI 1.40～37.25,P=0.02）;CR率、复发率、病死率和4项不良反应指标（胃肠道症状、肝肾功能损害、皮肤损害、发热）的Meta分析结果差异无统计学意义。结论服用CRNIT达CR所需时间比ATRA、ATO长,CRNIT近期疗效与ATRA、ATO相近。服用CRNIT的5年无病生存率可能优于ATRA。     

伴3'RARα亚显微缺失的急性早幼粒细胞白血病一例

目的 报道1例伴RARα 3'-末端(3'RARα)亚显微缺失的M3r亚型急性早幼粒细胞白血病(APL)病例及其形态学、细胞遗传学、分子遗传学和分子生物学的研究结果.方法 骨髓细胞直接法和短期培养法制备染色体,应用反带技术进行核型分析;分别用CEPX/Yα-卫星DNA探针、LSI PML-RARα双色双融合探针和LSI RAR α双色断裂点分离探针进行荧光原位杂交(FISH)分析;实时定量反转录聚合酶链反应(RT-PCR)方法检测PML-RARα融合基因转录本;多重巢式RT-PCR技术检测急性白血病29种染色体畸变所形成的融合基因,包括PML-RARα,PLZF-RARα和NPM-RARα融合基因转录本.结果 反带分析显示核型为45,X,-Y[6]/46,XY[8],CEPX/Y探针FISH进一步证实了Y染色体丢失;RARα双色断裂点分离探针FISH分析显示1个RARα等位基因的整个3'-末端缺失;通过细胞遗传学、FISH以及RT-PCR等方法检测,排除PML-RARα、PLZF-RARα、NPM-RARα、NuMA-RARα和STAT5b-RARα重排.结论 识别APL中一种新的RARα基因重排类型(3'RARα亚显微缺失而无X-RARα融合),RARα双色断裂点分离探针FISH分析是明确该异常的有效手段,其分子学结果有待进一步阐明.     

三氧化二砷联合全反式维甲酸治疗初发急性早幼粒细胞白血病的临床观察

目的 观察全反式维甲酸(ATRA)联合三氧化二砷(As2O3)治疗初诊急性早幼粒细胞白血病(APL)的疗效及不良反应.方法 对ATRA每天25mg/m2联合As2O310mg/d(联合组)治疗的35例APL患者达完全缓解(CR)时间、CR率、早期病死率及不良反应进行观察,并与单用As2O3 10 mg/d(单药组)治疗的33例进行比较.结果 联合组CR率为94.3%(33/35),与单药组[90.9%(30/33)]比较差异无统计学意义(P>0.05);联合组获得CR时间为26.1 d,短于单药组的30.5 d,差异有统计学意义(P<0.05);联合组与单药组APL分化综合征及不良反应发生率、早期病死率比较,差异均无统计学意义(均P>0.05);高WBC组比中、低WBC组CR率低,死亡率高,差异均有统计学意义(均P<0.05),低WBC组与中WBC组差异无统计学意义(P>0.05).结论 As2O3联合ATRA较单用As2O3治疗初诊APL获得CR时间短,WBC>10×109/L为预后不良的因素,APL分化综合征应尽早发现,及时处理.     

全反式维甲酸、三氧化二砷、化疗联合治疗急性早幼粒细胞白血病疗效观察

目的 评估全反式维甲酸(ATRA)、三氧化二砷(As2O3)、化疗联合治疗初诊急性早幼粒细胞白血病(APL)的疗效和患者不良反应.方法 对40例采用ATRA、As2O3、化疗三联疗法治疗的APL患者的临床资料进行回顾性分析,观察其疗效及不良反应.结果 总体CR率92.5%(37/40),完全缓解所需中位时间27(22～61)d;白细胞≥10×109/L组CR率72.7%(8/11),白细胞<10×109/L组CR率100%(29/29),差异有统计学意义(x2=8.550,P=0.004);治疗过程中无严重不良反应,仅1例发生维甲酸综合征.结论 ATRA、As2O3、化疗联合应用可作为APL患者的首选治疗方案.     

The success and the challenge of all-trans retinoic acid in the treatment of cancer

Abstract

All-trans retinoic acid (ATRA), an active metabolite of vitamin A, plays important roles in cell proliferation, cell differentiation, apoptosis, and embryonic development. The effects of ATRA are mediated by nuclear retinoid receptors as well as non-genomic signal pathway, such as MAPK and PKA. The great success of differentiation therapy with ATRA in acute promyelocytic leukemia (APL) not only improved the prognosis of APL but also spurred the studies of ATRA in the treatment of other tumors. Since the genetic and physiopathological simplicity of APL is not common in human malignancies, the combination of ATRA with other agents (chemotherapy, epigenetic modifiers, and arsenic trioxide, etc) had been extensively investigated in a variety of tumors. In this review, we will discuss in details about ATRA and its role in cancer treatment.     

人急性早幼粒细胞白血病小鼠模型的建立

目的: 探索稳定、可靠且重复性较好的人急性早幼粒细胞白血病Nod/SCID小鼠模型的建立方法,并观察模型的病程特点。方法: Nod/SCID小鼠经⁶⁰Co γ射线照射,照后第5天,外周血白细胞降至较低水平,此时尾静脉注射接种HL60细胞。通过流式细胞计数分析外周血中HL60细胞比例,以观察白血病细胞在外周血中分布变化;日常观察小鼠身体浅表部位实体瘤的形成及生长;并应用组织病理学方法确认组织脏器中肿瘤播散状况。结果: 接种第7天,Nod/SCID小鼠外周血中可检测到HL60细胞;接种 30 d 左右,可观察到小鼠出现全身播散的实体瘤;40 d 左右,动物体质状况显著衰退,小鼠陆续死亡。小鼠的造血系统及非造血系统的组织及脏器均出现肿瘤的浸润。重复实验结果一致。结论: Nod/SCID小鼠经⁶⁰Co γ射线照射后第5天,尾静脉注射接种HL60细胞,小鼠的病程可控制在 40 d 左右,且该模型符合临床疾病发展规律,可应用于骨髓毒性较低的受试药物的药效筛选及评价。     

New Evidence of the Importance of Weak Interactions in the Formation of PML-Bodies

In this work, we performed a comparative study of the formation of PML bodies by full-length PML isoforms and their C-terminal domains in the presence and absence of endogenous PML. Based on the analysis of the distribution of intrinsic disorder predisposition in the amino acid sequences of PML isoforms, regions starting from the amino acid residue 395 (i.e., sequences encoded by exons 4–6) were assigned as the C-terminal domains of these proteins. We demonstrate that each of the full-sized nuclear isoforms of PML is capable of forming nuclear liquid-droplet compartments in the absence of other PML isoforms. These droplets possess dynamic characteristics of the exchange with the nucleoplasm close to those observed in the wild-type cells. Only the C-terminal domains of the PML-II and PML-V isoforms are able to be included in the composition of the endogenous PML bodies, while being partially distributed in the nucleoplasm. The bodies formed by the C-terminal domain of the PML-II isoform are dynamic liquid droplet compartments, regardless of the presence or absence of endogenous PML. The C-terminal domain of PML-V forms dynamic liquid droplet compartments in the knockout cells (PML^−/−), but when the C-terminus of the PML-V isoform is inserted into the existing endogenous PML bodies, the molecules of this protein cease to exchange with the nucleoplasm. It was demonstrated that the K490R substitution, which disrupts the PML sumoylation, promotes diffuse distribution of the C-terminal domains of PML-II and PML-V isoforms in endogenous PML knockout HeLa cells, but not in the wild-type cells. These data indicate the ability of the C-terminal domains of the PML-II and PML-V isoforms to form dynamic liquid droplet-like compartments, regardless of the ordered N-terminal RBCC motifs of the PML. This indicates a significant role of the non-specific interactions between the mostly disordered C-terminal domains of PML isoforms for the initiation of liquid–liquid phase separation (LLPS) leading to the formation of PML bodies.