Gemtuzumab ozogamicin in the treatment of adult acute myeloid leukemia

Gemtuzumab ozogamicin (GO) is a humanized anti-CD33 monoclonal antibody conjugated to a derivative of an antitumor antibiotic, calicheamicin. GO was approved for the treatment of relapsed acute myeloid leukemia (AML) in the United States (US) in 2000. However, GO was withdrawn from the US market in June 2010, because a large-scale clinical trial failed to show additive or synergistic effects with conventional chemotherapy for newly diagnosed AML. GO is currently available only in Japan. However, several large clinical studies have demonstrated beneficial effects of GO when added to chemotherapy for AML in recent years;therefore, reconsideration of GO availability is gaining attention. Therefore, the role and efficacy of GO as monotherapy or in combination therapy for de novo or relapsed AML should be positively investigated.

Reinduction Chemotherapy with Gemtuzumab Ozogamicin and Intermediate/High-Dose Cytarabine: A Single-Center Experience

We performed a retrospective analysis of 9 patients with acute myeloid leukemia (AML) treated with gemtuzumab ozogamicin (GO) plus cytarabine as a salvage regimen (GO reinduction) for patients who did not achieve complete remission (CR) after the first cycle of induction chemotherapy or at first relapse. Cases of AML secondary to myelodysplastic syndrome or myeloproliferative disorder were included. CR was achieved in 6 of 9 patients, and 2 of 6 responders became long-term survivors. No non-responders survived longer than 6 months. Toxicity was mild, and the median duration of myelosuppression was less than 30 days. Stomatitis, nausea and sepsis occurred as non-hematological adverse events. Although our sample size was too small to permit definitive conclusions, GO reinduction should be considered for patients who relapse or do not achieve CR after the first cycle of induction chemotherapy. Some AML subtypes may respond more robustly than others, and further investigation is warranted.

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。

CD33抗体为主方案治疗难治性白血病

目的:评估CD33抗体为主方案治疗难治性白血病的疗效和不良反应。方法:采用CD33抗体为主方案对11例难治性白血病进行治疗。结果:CD33抗体为主方案治疗总有效率54%,其中完全缓解(CR)为36%,除血小板未完全缓解外均达到完全缓解标准(CRP)为18%,治疗后中位生存时间4.8月,缓解后中位生存时间8.2月。2例慢性粒细胞白血病急粒变均完全缓解,且BCR/ABL(-)。1例难治性急性淋巴白血病在缓解后即行异基因干细胞移植,至今无病生存已9月。不良反应有骨髓抑制(100%)、输注相关寒战发热(90%),肝静脉闭塞综合症(VOD)发生率55%,发生在干细胞移植后的患者和年龄大于60岁的患者。结论:本组资料显示CD33抗体为主方案对表达CD33的急慢性白血病有一定疗效。对于移植后复发和年龄大于60岁的患者,在使用CD33抗体时需注意患者肝脏情况,一旦出现VOD,及时处理。对于用药后缓解的患者,应尽早行异基因干细胞移植。

吉妥珠单抗奥唑米星显著改善老年急性髓系白血病患者的总生存率

1文献来源Amadori S,Suciu S,Selleslag D,et al.Gemtuzumab Ozogamicin versus best supportive carein older patients with newly diagnosed acute myeloidleukemia unsuitable for intensive chemotherapy：Results of the randomized phaseⅢEORTC-GIMEMAAML-19 trial[J].J Clin Oncol,2016,34（9）：972-979.2证据水平1b。

老年急性髓性白血病的治疗现状

急性髓性白血病(AML)占成人急性白血病近80%。35%新诊断的AML患者年龄≥75岁,诊断时的中位年龄67岁。老年AML患者比年轻个体对标准化疗反应差,完全缓解率和无复发生存率低。老年患者在AML之前常先出现骨髓增生异常综合征(MDS)和预后不良的核型如5q-或7q-更常见。在既往10年间新治疗的应用,其中最先出现的是吉姆单抗(gemtuzumab ozogamicin)。其他药物仍在试用和评估中,包括多药耐药抑制剂、法尼基转移酶抑制剂(FTI)、新的核苷类药物和FLT抑制剂等。

吉妥珠单抗在CD33阳性急性髓系白血病中的研究进展

目前,通过运用传统化疗或造血干细胞移植治疗急性髓系白血病(acute myeloid leukemia,AML)虽然取得一定疗效,但远期预后仍存在局限性。为改善这一缺陷,抗体偶联药物将可能成为这部分患者的最佳选择。吉妥珠单抗(gemtuzumab ozogamicin,GO)是一种由人源化抗CD33单抗与脱氧核糖核酸(deoxyribonucleic acid,DNA)嵌入剂卡奇霉素(calicheamicin,CLM)形成的抗体偶联药物。CD33表达于90%的AML细胞表面,不表达于正常造血干细胞和成熟粒细胞。因此,其成为AML靶向治疗的良好靶点。已有许多研究报道,GO无论是单药还是联合治疗,均能改善CD33阳性AML患者的预后。本文主要就GO的特征及其在CD33阳性AML中的研究进展进行综述。

美罗他格——CD33单抗偶联物治疗急性髓细胞白血病

CD33抗原大量表达于急性髓细胞白血病(AML)细胞表面,可成为靶向免疫治疗的目标。美罗他格是人源化抗CD33单克隆抗体与强效抗肿瘤抗生素——乙酰棘孢霉素偶联物,与髓性白血病细胞表面CD33抗原结合,进入细胞后释放棘孢霉素,对髓细胞白血病细胞有明显杀灭作用,用于治疗复发、难治的CD33+AML,获得良好疗效,与其它化疗药物联合应用治疗AML的临床试验正在进行中。美罗他格的耐受性一般较好,但肝脏毒性及肝静脉阻塞综合征等毒副反应值得关注。美罗他格的耐药机制可能来自多方面,其中包括P-糖蛋白介导的药物排出等。

吉妥单抗复兴史

采用访谈的形式,以首个上市的抗体偶联药物“吉妥单抗”的传奇历程为明线,靶向药物在化学分子设计和分析检测上的进步为暗线,讲述了抗体偶联药物的发展史。较为全面地介绍了抗体偶联药物的化学结构、设计思路、分析方法与发展前景。

奥佐米星对急性髓细胞性白血病的细胞毒性及其与CD33表达水平的关系研究

目的探索奥佐米星(GO)对急性髓细胞性白血病(AML)细胞毒性与CD33表达水平的关系及作用机制。方法选取人髓系OCI-AML3和KG-1a细胞,采用含CD33质粒的慢病毒对其进行转染,然后根据CD33表达量将细胞分为CD33高表达组和CD33低表达组。两组均采用15μg/L的GO进行处理,然后通过MTT实验测定两组细胞的存活率。采用不同浓度(0、5、10、15μg/L)的GO处理OCI-AML3细胞,然后采用蛋白质印迹法检测细胞的凋亡相关蛋白Bcl-2、cleaved-caspase 3、caspase 3的表达水平。结果转染后,OCI-AML3和KG-1a细胞表面CD33表达水平高于转染前,差异有统计学意义(P<0.05)。相同浓度的GO处理后,CD33高表达组的OCI-AML3和KG-1a细胞存活率均低于CD33低表达组,差异有统计学意义(P<0.05)。GO浓度为5、10、15μg/L时,OCI-AML3细胞Bcl-2水平低于GO浓度为0时,cleaved-caspase 3、caspase 3水平均高于GO浓度为0时;GO浓度为10、15μg/L时OCI-AML3细胞Bcl-2水平低于GO浓度为5μg/L时,cleaved-caspase 3、caspase 3水平均高于GO浓度为5μg/L时;GO浓度为15μg/L时,OCI-AML3细胞Bcl-2水平低于GO浓度为10μg/L时,cleaved-caspase 3、caspase 3水平均高于GO浓度为10μg/L时,差异有统计学意义(P<0.05)。结论GO对CD33高表达的人髓系细胞增殖的抑制作用增强,可通过调控凋亡蛋白的表达发挥促进AML细胞凋亡的作用。

地西他滨联合抗CD33单抗治疗难治性急性髓细胞性白血病(附2例报告)

目的探讨地西他滨(DAC)联合抗CD33单抗(GO)治疗难治性急性髓细胞性白血病(AML)的疗效和安全性。方法对2例难治性AML(M4)患者均进行1个疗程的DAC联合GO治疗(具体剂量为DAC:20 mg.m-2.d-1×5 d,第1～5天,GO 9 mg/m2,第6天),应用骨髓涂片、定期监测血常规评价其疗效。结果经过1个疗程的DAC联合GO治疗后,1例患者未出现疾病进展,骨髓中原幼细胞由35%降至27.5%,巨核细胞由2个/片增加至(200个/片,血小板由减少改善为数量基本正常,临床上血小板恢复正常水平,一般情况良好。另1例在治疗期间高白细胞得以控制,治疗后第15天复查骨髓提示原幼细胞由38.5%降至12.5%,获得部分缓解。2例患者均未出现肝静脉闭塞病(VOD)及其他脏器功能损害表现。结论 DAC联合GO治疗难治性AML安全可行,尤其是对于一般情况差、不能耐受高剂量化疗或高剂量挽救化疗失败的患者,不失为一种新的治疗选择。

The evolving landscape in the therapy of acute myeloid leukemia

Acute myeloid leukemia(AML)is a heterogeneous clonal disorder of myeloid precursors arrested in their matura-tion,creating a diverse disease entity with a wide range of responses to historically standard treatment approaches.While signifi cant progress has been made in character-izing and individualizing the disease at diagnosis to op-timally inform those affected,progress in treatment to reduce relapse and induce remission has been limited thus far.In addition to a brief summary of the factors that shape prognostication at diagnosis,this review attempts to expand on the current therapies under investigation that have shown promise in treating AML,including hy-pomethylating agents,gemtuzumab ozogamicin,FLT3 ty-rosine kinase inhibitors,antisense oligonucleotides,and other novel therapies,including aurora kinases,mTOR and PI3 kinase inhibitors,PIM kinase inhibitors,HDAC inhibitors,and IDH targeted therapies.With these,and undoubtedly many others in the future,it is the hope that by combining more accurate prognostication with more effective therapies,patients will begin to have a different,and more complete,outlook on their disease that allows for safer and more successful treatment strategies.