在晚期慢性期和加速期对伊马替尼敏感的慢性粒细胞白血病(CML)患者中存在新型复合BCR-ABL突变,表明这些突变在CML进展中可能发挥的作用。
Presence of novel compound BCR-ABL mutations in late chronic and advanced phase imatinib sensitive CML patients indicates their possible role in CML progression.
作者信息
Akram Afia Muhammad, Iqbal Zafar, Akhtar Tanveer, Khalid Ahmed Mukhtar, Sabar Muhammad Farooq, Qazi Mahmood Hussain, Aziz Zeba, Sajid Nadia, Aleem Aamer, Rasool Mahmood, Asif Muhammad, Aloraibi Saleh, Aljamaan Khaled, Iqbal Mudassar
机构信息
a Institute of Molecular Biology and Biotechnology, The University of Lahore , Lahore , Pakistan.
b Hematology Oncology and Pharmacogenetic Engineering Sciences (HOPES) Group, Health Sciences Research Laboratories , Department of Zoology, University of the Punjab , Lahore , Pakistan.
出版信息
Cancer Biol Ther. 2017 Apr 3;18(4):214-221. doi: 10.1080/15384047.2017.1294289. Epub 2017 Feb 21.
BCR-ABL kinase domain (K) mutations are well known for causing resistance against tyrosine kinase inhibitors (TKIs) and disease progression in chronic myeloid leukemia (CML). In recent years, compound BCR-ABL mutations have emerged as a new threat to CML patients by causing higher degrees of resistance involving multiple TKIs, including ponatinib. However, there are limited reports about association of compound BCR-ABL mutations with disease progression in imatinib (IM) sensitive CML patients. Therefore, we investigated presence of ABL-K mutations in chronic phase (n = 41), late chronic phase (n = 33) and accelerated phase (n = 16) imatinib responders. Direct sequencing analysis was used for this purpose. Eleven patients (12.22%) in late-CP CML were detected having total 24 types of point mutations, out of which 8 (72.72%) harbored compound mutated sites. SH2 contact site mutations were dominant in our study cohort, with E355G (3.33%) being the most prevalent. Five patients (45%) all having compound mutated sites, progressed to advanced phases of disease during follow up studies. Two novel silent mutations G208G and E292E/E were detected in combination with other mutants, indicating limited tolerance for BCR-ABL1 kinase domain for missense mutations. However, no patient in early CP of disease manifested mutated ABL-K. Occurrence of mutations was found associated with elevated platelet count (p = 0.037) and patients of male sex (p = 0.049). The median overall survival and event free survival of CML patients (n = 90) was 6.98 and 5.8 y respectively. The compound missense mutations in BCR-ABL kinase domain responsible to elicit disease progression, drug resistance or disease relapse in CML, can be present in yet Imatinib sensitive patients. Disease progression observed here, emphasizes the need of ABL-K mutation screening in late chronic phase CML patients for improved clinical management of disease.
BCR-ABL激酶结构域(K)突变因导致慢性髓性白血病(CML)患者对酪氨酸激酶抑制剂(TKIs)产生耐药性及疾病进展而广为人知。近年来,复合BCR-ABL突变对CML患者构成了新威胁,它会导致对包括波纳替尼在内的多种TKIs产生更高程度的耐药性。然而,关于复合BCR-ABL突变与伊马替尼(IM)敏感的CML患者疾病进展之间关联的报道有限。因此,我们调查了慢性期(n = 41)、慢性晚期(n = 33)和加速期(n = 16)伊马替尼反应者中ABL-K突变的存在情况。为此采用了直接测序分析。在慢性晚期CML患者中,有11名患者(12.22%)被检测出共有24种点突变类型,其中8名患者(72.72%)存在复合突变位点。SH2接触位点突变在我们的研究队列中占主导地位,E355G(3.33%)最为常见。5名患者(45%)均有复合突变位点,在后续研究中病情进展至疾病晚期。检测到两个新的沉默突变G208G和E292E/E与其他突变同时存在,这表明BCR-ABL1激酶结构域对错义突变的耐受性有限。然而,疾病早期慢性期的患者均未出现ABL-K突变。发现突变的发生与血小板计数升高(p = 0.037)及男性患者(p = 0.049)有关。CML患者(n = 90)的中位总生存期和无事件生存期分别为6.98年和5.8年。BCR-ABL激酶结构域中的复合错义突变可导致CML患者疾病进展、耐药或疾病复发,但这些突变也可能存在于伊马替尼敏感患者中。此处观察到的疾病进展强调了对慢性晚期CML患者进行ABL-K突变筛查以改善疾病临床管理的必要性。
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