吉西他滨给药后的严重急性毒性:4例病例报告及胞苷脱氨酶多态性评估
Severe acute toxicity following gemcitabine administration: A report of four cases with cytidine deaminase polymorphisms evaluation.
作者信息
Hryciuk Beata, Szymanowski Bartosz, Romanowska Anna, Salt Ewa, Wasąg Bartosz, Grala Bartłomiej, Jassem Jacek, Duchnowska Renata
机构信息
Department of Oncology, Military Institute of Medicine, 04-141 Warsaw, Poland.
Department of Oncology and Radiotherapy, Medical University of Gdańsk, 80-211 Gdańsk, Poland.
出版信息
Oncol Lett. 2018 Feb;15(2):1912-1916. doi: 10.3892/ol.2017.7473. Epub 2017 Nov 22.
Abstract
Gemcitabine (GCB) is a pyrimidine antimetabolite widely used in various solid tumors as a single agent or as a component of multidrug regimens. In the majority of patients, GCB is well tolerated, however life-threatening complications occasionally occur. The current report presents four cases of severe acute toxicity, which included two that were fatal, following administration of GCB alone or in combination with cisplatin. Of the four cases, in one, a Naranjo Adverse Drug Reaction Probability Score was definite, in two, probable and in one possible. To determine the potential causes of these toxicities, polymorphic variants of cytidine deaminase, the primary enzyme involved in the hepatic metabolism of GCB, were assessed. The homogeneous c.435TT variant was detected in one patient and a heterozygotic c.435CT variant in two, one of whom additionally harbored a heterozygotic c.79AC variant.
摘要
吉西他滨(GCB)是一种嘧啶抗代谢物,作为单一药物或多药方案的组成部分广泛用于各种实体瘤。在大多数患者中,GCB耐受性良好,但偶尔会出现危及生命的并发症。本报告介绍了4例严重急性毒性病例,这些病例在单独使用GCB或与顺铂联合使用后发生,其中2例死亡。在这4例病例中,1例的Naranjo药物不良反应概率评分为肯定,2例为很可能,1例为可能。为了确定这些毒性的潜在原因,评估了胞苷脱氨酶(参与GCB肝脏代谢的主要酶)的多态性变体。在1例患者中检测到纯合的c.435TT变体,2例患者中检测到杂合的c.435CT变体,其中1例还携带杂合的c.79AC变体。
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