Radisic M, Lattes R, Chapman J F, del Carmen Rial M, Guardia O, Seu F, Gutierrez P, Goldberg J, Casadei D H
Instituto de Nefrología, Cabello 3889, Capital Federal 1425, Buenos Aires, Argentina.
Transpl Infect Dis. 2003 Jun;5(2):84-93. doi: 10.1034/j.1399-3062.2003.00018.x.
To analyze risk factors for Pneumocystis carinii pneumonia (PCP) in kidney transplant recipients.
In a case-control study, 17 PCP cases diagnosed between July 1994 and July 2000 were matched with two controls each (previous and subsequent kidney transplant recipients who did not develop PCP during the same follow-up period). Demographics, organ origin, human leukocyte antigen (HLA) mismatches, use of poly- or monoclonal anti-CD3 antibodies (Po/MoAb) for induction or rejection treatment, rejection episodes, cumulative steroid dose for rejection treatment, immunosuppressive regimens, and other infections were analyzed.
No significant differences were seen in gender (male 10 vs. 15), mean age (39.7 vs. 35.4 years), organ origin (cadaver donor 13 vs. 19), HLA mismatches, or Po/MoAb use in induction treatment. Significant differences were observed in PCP cases for rejection history (P=0.02), and median and total number of rejection episodes (P=0.0018). The relative risks for PCP for 1, 2, and > or =3 rejection treatments vs. no such treatment were 1, 1.05, and 6.30, respectively (P=0.021). The relative risk for PCP for steroid-resistant rejection was 4.34 (95% confidence interval [CI], 1.04-18.89) (P=0.019), and that for the use of Po/MoAb for rejection treatment was 7.23 (95% CI, 1.28-49.34) (P=0.006). The relative risk for PCP for 0, 1, and > or =2 previous or concomitant cytomegalovirus (CMV) infection vs. no such infections were 1.0, 2.32, and 13.0, respectively (P=0.012). The relative risks for PCP for tuberculosis (TB) was 18 (95% CI, 1.76-852.03), that for bacterial pneumonia was 14.22 (95% CI, 2.16-150.23), and that for hepatitis C virus infection was 5.25 (95% CI, 1.03-28.91). Immunosuppressive regimens with tacrolimus, mycophenolate mofetil (MMF), steroids (P=0.06), and MMF as a single variable (P=0.05) were more frequently used in cases. Primary trimethoprim-sulfamethoxazole prophylaxis failure was observed in 12 patients in association with heavy immunosuppression and concomitant infections.
The risk of PCP in kidney transplant recipients is related to the number and type of rejection treatments. It is also related to the occurrence of CMV infection, and to other immunomodulating infections such as TB and hepatitis C, and might also be increased with the use of newer and more potent immunosuppressive agents. Primary prophylaxis failure may occur in association with some of these risk factors.
分析肾移植受者发生卡氏肺孢子虫肺炎(PCP)的危险因素。
在一项病例对照研究中,选取1994年7月至2000年7月期间确诊的17例PCP病例,每例病例匹配两名对照(同期接受肾移植且未发生PCP的前后对照受者)。分析人口统计学资料、器官来源、人类白细胞抗原(HLA)错配情况、诱导或抗排斥治疗中使用多克隆或单克隆抗CD3抗体(Po/MoAb)的情况、排斥反应发作次数、抗排斥治疗累积使用类固醇剂量、免疫抑制方案以及其他感染情况。
在性别(男性10例对15例)、平均年龄(39.7岁对35.4岁)、器官来源(尸体供者13例对19例)、HLA错配情况或诱导治疗中Po/MoAb的使用方面,未观察到显著差异。在PCP病例中,排斥反应病史(P = 0.02)、排斥反应发作次数的中位数和总数(P = 0.0018)存在显著差异。与未接受抗排斥治疗相比,接受1次、2次和≥3次抗排斥治疗发生PCP的相对风险分别为1、1.05和6.30(P = 0.021)。对类固醇耐药性排斥反应发生PCP的相对风险为4.34(95%置信区间[CI],1.04 - 18.89)(P = 0.019),使用Po/MoAb进行抗排斥治疗发生PCP的相对风险为7.23(95%CI,1.28 - 49.34)(P = 0.006)。与未发生巨细胞病毒(CMV)感染相比,既往或同时发生0次、1次和≥2次CMV感染发生PCP的相对风险分别为1.0、2.32和13.0(P = 0.012)。发生PCP的相对风险,结核病(TB)为18(95%CI,1.76 - 852.03),细菌性肺炎为14.22(95%CI,2.16 - 150.23),丙型肝炎病毒感染为5.25(95%CI,1.03 - 28.91)。病例组更频繁使用含他克莫司、霉酚酸酯(MMF)、类固醇的免疫抑制方案(P = 0.06)以及单独使用MMF作为变量(P = 0.05)。观察到12例患者因免疫抑制严重和合并感染导致一线甲氧苄啶 - 磺胺甲恶唑预防治疗失败。
肾移植受者发生PCP的风险与抗排斥治疗的次数和类型有关。还与CMV感染的发生有关,以及与其他免疫调节性感染如TB和丙型肝炎有关,并且使用更新更强效的免疫抑制药物可能也会增加风险。一线预防治疗失败可能与其中一些危险因素相关。
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