Gisbert Javier P, Niño Pilar, Rodrigo Luis, Cara Carlos, Guijarro Luis G
Gastroenterology Unit, Hospital Universitario de la Princesa, Universidad Autónoma, Madrid, Spain.
Am J Gastroenterol. 2006 Dec;101(12):2769-76. doi: 10.1111/j.1572-0241.2006.00843.x. Epub 2006 Oct 6.
To prospectively evaluate whether a relationship between thiopurine methyltransferase (TPMT) activity and incidence of adverse effects (especially myelotoxicity) exists, in a long-term follow-up study of a large group of patients with inflammatory bowel disease treated with azathioprine.
TPMT activity in red blood cells (RBC) was measured by a radiochemical method in 394 consecutive patients with Crohn's disease (238) or ulcerative colitis (156) starting treatment with azathioprine. The relationship among several variables and TPMT values was assessed, and the correlation between such levels and the incidence of adverse effects was evaluated.
Mean TPMT value was 18.6 +/- 4 U/mL RBCs (range 9.4-33.7). No patient had low levels (<5), 7.1% had intermediate levels (5-13.7), and 92.9% had high levels (>13.8). Differences (P < 0.001) were demonstrated in TPMT activity depending on the type of inflammatory bowel disease, but not on the remaining variables (including treatment with 5-aminosalycilates). Adverse effects were reported in 74 patients (18.8%), the most frequent being gastrointestinal intolerance (9.1%) and myelotoxicity (4.3%). No patient having adverse effects had low TPMT levels. However, mean TPMT activity was lower in those with adverse effects (16.6 +/- 3 vs 19.1 +/- 4 U/mL, P < 0.001). Moreover, the probability of suffering myelotoxicity in the high TPMT group was only 3.5%, compared with 14.3% in the TPMT intermediate group (95% CI = 1.37-14.9; OR = 4.5).
The strategy of determining TPMT activity in all patients prior to initiating treatment with azathioprine could help to minimize the risk of myelotoxicity, as patients with intermediate TPMT activity had fourfold more risk than high TPMT activity patients.
在一项对大量接受硫唑嘌呤治疗的炎症性肠病患者的长期随访研究中,前瞻性评估硫嘌呤甲基转移酶(TPMT)活性与不良反应(尤其是骨髓毒性)发生率之间是否存在关联。
采用放射化学方法测定了394例开始接受硫唑嘌呤治疗的克罗恩病患者(238例)或溃疡性结肠炎患者(156例)红细胞中的TPMT活性。评估了几个变量与TPMT值之间的关系,并评价了这些水平与不良反应发生率之间的相关性。
TPMT的平均活性值为18.6±4 U/mL红细胞(范围9.4 - 33.7)。没有患者TPMT水平低(<5),7.1%的患者为中等水平(5 - 13.7),92.9%的患者为高水平(>13.8)。根据炎症性肠病的类型,TPMT活性存在差异(P < 0.001),但在其他变量(包括使用5 - 氨基水杨酸治疗)方面无差异。74例患者(18.8%)报告有不良反应,最常见的是胃肠道不耐受(9.1%)和骨髓毒性(4.3%)。没有出现不良反应的患者TPMT水平低。然而,出现不良反应患者的TPMT平均活性较低(16.6±3 vs 19.1±4 U/mL,P < 0.001)。此外,TPMT高水平组发生骨髓毒性的概率仅为3.5%,而TPMT中等水平组为14.3%(95%可信区间 = 1.37 - 14.9;比值比 = 4.5)。
在开始硫唑嘌呤治疗前对所有患者测定TPMT活性的策略有助于将骨髓毒性风险降至最低,因为TPMT活性中等的患者发生骨髓毒性的风险比TPMT活性高的患者高四倍。
