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CLIN CANCER RES:DNA修复突变状态不同的肿瘤患者药物毒性反应不同

2017-11-02 MedSci MedSci原创

DNA修复突变药物毒性肿瘤
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PARP抑制剂(PARPi)talazoparib可能增强化疗活性以及易出现DNA损伤细胞的毒性。CLIN CANCER RES近期发表了一篇文章研究这一问题。

PARP抑制剂(PARPi)talazoparib可能增强化疗活性以及易出现DNA损伤细胞的毒性。CLIN CANCER RES近期发表了一篇文章研究这一问题。

临床研究评估了talazoparib联合卡铂的安全性、耐受性、药代动力学和疗效。使用药代动力学模型研究DNA易损性与血液毒性之间的关系。共24例实体肿瘤患者纳入4个研究队列,talazoparib 0.75mg和1mg联合卡铂(AUC1和1.5,每2周或每3周),其中14例患者接受过铂类治疗。剂量限制毒性包括3级疲劳和4级血小板减少。未达到最大耐受剂量。3/4级毒性反应包括疲劳(13%)、中性粒细胞减少(63%)、血小板减少(29%)以及贫血(38%)。BRCA1/2患者(gBRCA1/2)中出现1例完全反应和2例部分反应。4个月后4例患者病情稳定,其中3例患者已知存在DNA修复通路突变。药代动力学模型表明卡铂AUC1.5每3周和talazoparib1 mg每天治疗3个周期后,gBRCA患者中性粒细胞下降78%,非gBRCA患者下降63%。药代动力学毒性模型表明gBRCA突变状态不同可能会影响联合治疗的风险/获益比值。

文章最后认为,存在DNA损伤突变的患者卡铂联合talazoparib治疗有效,但是血液学毒性在gBRCA患者中更严重。根据患者DNA损伤突变状态不同,卡铂最好联合不同剂量的talazoparib间歇性进行治疗。

原始出处:
Mallika S.Dhawan,Imke H.Bartelink,et al.Differential Toxicity in Patients with and without DNA Repair Mutations:Phase ⅠStudy of Carboplatin and Talazoparib in Advanced Solid Tumor.CLIN CANCER RES.November 2017 doi:10.1158/1078-0432.CCR-17-0703

本文系梅斯医学(MedSci)原创编译整理,转载需授权!

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    2017-11-04 lanyan20020087

    #肿瘤患者#

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    2017-11-04 jambiya

    #DNA修复#

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