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三磷酸肌苷焦磷酸水解酶活性:相比于肌苷三磷酸焦磷酸水解酶(ITPA)基因型,它是丙型肝炎感染患者中利巴韦林诱导贫血的更准确预测指标。

Inosine triphosphate pyrophosphohydrolase activity: more accurate predictor for ribavirin-induced anemia in hepatitis C infected patients than ITPA genotype.

作者信息

Peltenburg Nicole Chantal, Bakker Jaap A, Vroemen Wim H M, de Knegt Robert J, Leers Mathie P G, Bierau Jörgen, Verbon Annelies

出版信息

Clin Chem Lab Med. 2015 Nov;53(12):2021-9. doi: 10.1515/cclm-2015-0057.

Abstract

BACKGROUND

ITPA polymorphisms have been associated with protection against ribavirin-induced anemia in chronic hepatitis C (HCV) patients. Here we determined the association of inosine triphosphate pyrophosphohydrolase (inosine triphosphatase or ITPase) enzyme activity with ITPA genotype in predicting ribavirin-induced anemia.

METHODS

In a cohort of 106 HCV patients, hemoglobin (Hb) values were evaluated after 4 weeks (T4) and at the time of lowest Hb value (Tnadir). ITPase activity was measured and ITPA genotype determined. Single-nucleotide polymorphisms (SNPs) tested were c.124+21A>C and c.94C>A. ITPase activity ≥1.11 mU/mol Hb was considered as normal.

RESULTS

After 4 weeks of treatment, 78% of the patients with normal ITPase activity were anemic and 21% of the patients with low ITPase activity (p<0.001). Stratified by genotype, the percentages of anemic patients were: wt/wt 76%, wt/c.124+21A>C 46% (p=0.068), and wt/c.94C>A 29% (p=0.021). At Tnadir, virtually all patients with normal ITPase activity were anemic, compared to only 64% of the patients with low activity (p=0.02). Thirteen patients had wt/c.124+241A>C genotype. Within this group all five patients with normal ITPase activity and only four of eight with decreased activity developed anemia. Presence of HCV RNA did not influence ITPase activity.

CONCLUSIONS

This study is the first to report that ITPase activity predicts the development of anemia during ribavirin treatment. ITPase activity and ITPA genotype have high positive predictive values for development of ribavirin-induced anemia at any time during treatment, but ITPase activity predicts ribavirin-induced anemia more accurately.

摘要

背景

肌苷三磷酸酶(ITPA)基因多态性与慢性丙型肝炎(HCV)患者对利巴韦林诱导的贫血具有保护作用有关。在此,我们确定了三磷酸肌苷焦磷酸水解酶(肌苷三磷酸酶或ITP酶)活性与ITPA基因型在预测利巴韦林诱导的贫血方面的相关性。

方法

在一组106例HCV患者中,在4周后(T4)和血红蛋白(Hb)值最低时(Tnadir)评估Hb值。测量ITP酶活性并确定ITPA基因型。检测的单核苷酸多态性(SNP)为c.124+21A>C和c.94C>A。ITP酶活性≥1.11 mU/mol Hb被视为正常。

结果

治疗4周后,ITP酶活性正常的患者中有78%出现贫血,而ITP酶活性低的患者中有21%出现贫血(p<0.001)。按基因型分层,贫血患者的百分比分别为:野生型/野生型76%,野生型/c.124+21A>C 46%(p=0.068),野生型/c.94C>A 29%(p=0.021)。在Tnadir时,几乎所有ITP酶活性正常的患者都出现了贫血,而活性低的患者中只有64%出现贫血(p=0.02)。13例患者具有野生型/c.124+241A>C基因型。在该组中,ITP酶活性正常的5例患者全部出现贫血,而活性降低的8例患者中只有4例出现贫血。HCV RNA的存在不影响ITP酶活性。

结论

本研究首次报道ITP酶活性可预测利巴韦林治疗期间贫血的发生。ITP酶活性和ITPA基因型对治疗期间任何时候利巴韦林诱导的贫血发生具有较高的阳性预测价值,但ITP酶活性能更准确地预测利巴韦林诱导的贫血。

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