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卡培他滨相关手足综合征的潜在机制。

Candidate mechanisms for capecitabine-related hand-foot syndrome.

作者信息

Milano Gérard, Etienne-Grimaldi Marie-Christine, Mari Mireille, Lassalle Sandra, Formento Jean-Louis, Francoual Mireille, Lacour Jean-Philippe, Hofman Paul

机构信息

INSERM ERI-21, Faculté de Médecine, CHU de Nice, Nice, France.

出版信息

Br J Clin Pharmacol. 2008 Jul;66(1):88-95. doi: 10.1111/j.1365-2125.2008.03159.x. Epub 2008 Mar 13.

Abstract

AIMS

The oral fluoropyrimidine prodrug capecitabine is widely used in oncology. Capecitabine was designed to generate 5FU via the thymidine phosphorylase (TP) enzyme, preferentially expressed in tumoral tissues. Hand-foot syndrome (HFS) is a limiting toxicity of capecitabine. A pilot study on healthy volunteers was conducted in order to test the hypothesis that the occurrence of HFS could be related to tissue-specific expression of drug-metabolizing enzymes in the skin of the palm and sole. To this end, the expression of TP (activating pathway), dihydropyrimidine dehydrogenase (DPD, catabolic pathway) and cell proliferation (Ki67) were measured in the skin of the palm (target tissue for HFS) and of the lower back (control area).

METHODS

Two paired 4-mm diameter punch biopsy specimens (palm and back) were taken in 12 healthy volunteers. Immunohistochemical analyses were performed on frozen tissues.

RESULTS

Proliferation rate (Ki67 staining) was significantly higher in epidermal basal cells of the palm compared with the back (P = 0.008). Also, TP and DPD expression were significantly greater in the palm relative to the back (P = 0.039 and 0.012, respectively). TP and Ki67 expression were positively and significantly correlated in the palm.

CONCLUSIONS

The high proliferation rate of epidermal basal cells in the palm could make them more sensitive to the local action of cytotoxic drugs. TP-facilitated local production of 5FU in the palm during capecitabine treatment could explain the occurrence of HFS. This observation may support future strategies to limit the occurrence of HFS during capecitabine therapy.

摘要

目的

口服氟嘧啶前药卡培他滨在肿瘤学中广泛应用。卡培他滨经设计可通过胸苷磷酸化酶(TP)生成5-氟尿嘧啶(5FU),该酶在肿瘤组织中优先表达。手足综合征(HFS)是卡培他滨的一种剂量限制性毒性反应。开展了一项针对健康志愿者的初步研究,以检验HFS的发生可能与手掌和足底皮肤中药物代谢酶的组织特异性表达有关这一假说。为此,在手掌(HFS的靶组织)和下背部(对照区域)皮肤中测量了TP(激活途径)、二氢嘧啶脱氢酶(DPD,分解代谢途径)的表达以及细胞增殖(Ki67)情况。

方法

在12名健康志愿者身上采集了两对直径4毫米的打孔活检标本(手掌和背部)。对冷冻组织进行免疫组织化学分析。

结果

与背部相比,手掌表皮基底细胞的增殖率(Ki67染色)显著更高(P = 0.008)。此外,相对于背部,手掌中TP和DPD的表达也显著更高(分别为P = 0.039和0.012)。手掌中TP和Ki67的表达呈显著正相关。

结论

手掌表皮基底细胞的高增殖率可能使其对细胞毒性药物的局部作用更敏感。卡培他滨治疗期间手掌中TP促进5FU的局部生成可能解释了HFS的发生。这一观察结果可能为限制卡培他滨治疗期间HFS发生的未来策略提供支持。

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