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三氧化二砷治疗新诊断和复发急性早幼粒细胞白血病患者的比较:对耐药机制的深入了解

Comparison of newly diagnosed and relapsed patients with acute promyelocytic leukemia treated with arsenic trioxide: insight into mechanisms of resistance.

作者信息

Chendamarai Ezhilarasi, Ganesan Saravanan, Alex Ansu Abu, Kamath Vandana, Nair Sukesh C, Nellickal Arun Jose, Janet Nancy Beryl, Srivastava Vivi, Lakshmi Kavitha M, Viswabandya Auro, Abraham Aby, Aiyaz Mohammed, Mullapudi Nandita, Mugasimangalam Raja, Padua Rose Ann, Chomienne Christine, Chandy Mammen, Srivastava Alok, George Biju, Balasubramanian Poonkuzhali, Mathews Vikram

机构信息

Department of Haematology, Christian Medical College, Vellore, India.

Department of Transfusion Medicine and Immunohaematology, Christian Medical College, Vellore, India.

出版信息

PLoS One. 2015 Mar 30;10(3):e0121912. doi: 10.1371/journal.pone.0121912. eCollection 2015.

Abstract

There is limited data on the clinical, cellular and molecular changes in relapsed acute promyeloytic leukemia (RAPL) in comparison with newly diagnosed cases (NAPL). We undertook a prospective study to compare NAPL and RAPL patients treated with arsenic trioxide (ATO) based regimens. 98 NAPL and 28 RAPL were enrolled in this study. RAPL patients had a significantly lower WBC count and higher platelet count at diagnosis. IC bleeds was significantly lower in RAPL cases (P=0.022). The ability of malignant promyelocytes to concentrate ATO intracellularly and their in-vitro IC50 to ATO was not significantly different between the two groups. Targeted NGS revealed PML B2 domain mutations in 4 (15.38%) of the RAPL subset and none were associated with secondary resistance to ATO. A microarray GEP revealed 1744 genes were 2 fold and above differentially expressed between the two groups. The most prominent differentially regulated pathways were cell adhesion (n=92), cell survival (n=50), immune regulation (n=74) and stem cell regulation (n=51). Consistent with the GEP data, immunophenotyping revealed significantly increased CD34 expression (P=0.001) in RAPL cases and there was in-vitro evidence of significant microenvironment mediated innate resistance (EM-DR) to ATO. Resistance and relapse following treatment with ATO is probably multi-factorial, mutations in PML B2 domain while seen only in RAPL may not be the major clinically relevant cause of subsequent relapses. In RAPL additional factors such as expansion of the leukemia initiating compartment along with EM-DR may contribute significantly to relapse following treatment with ATO based regimens.

摘要

与新诊断的急性早幼粒细胞白血病(NAPL)相比,复发性急性早幼粒细胞白血病(RAPL)的临床、细胞和分子变化的数据有限。我们进行了一项前瞻性研究,以比较接受基于三氧化二砷(ATO)方案治疗的NAPL和RAPL患者。本研究纳入了98例NAPL和28例RAPL患者。RAPL患者诊断时白细胞计数显著较低,血小板计数较高。RAPL病例中颅内出血显著较少(P = 0.022)。两组之间恶性早幼粒细胞在细胞内浓缩ATO的能力及其对ATO的体外IC50无显著差异。靶向二代测序显示,RAPL亚组中有4例(15.38%)存在PML B2结构域突变,且均与对ATO的继发性耐药无关。基因表达谱微阵列显示,两组之间有1744个基因的表达差异达到2倍及以上。最显著的差异调节通路是细胞黏附(n = 92)、细胞存活(n = 50)、免疫调节(n = 74)和干细胞调节(n = 51)。与基因表达谱数据一致,免疫表型分析显示RAPL病例中CD34表达显著增加(P = 0.001),并且有体外证据表明存在显著的微环境介导的对ATO的固有耐药(EM-DR)。ATO治疗后的耐药和复发可能是多因素的,PML B2结构域的突变虽然仅在RAPL中出现,但可能不是随后复发的主要临床相关原因。在RAPL中,其他因素如白血病起始细胞池的扩大以及EM-DR可能对基于ATO方案治疗后的复发有显著影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e346/4378855/5a0f68395fef/pone.0121912.g001.jpg

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