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Association of Extrarenal Adverse Effects of Posttransplant Immunosuppression With Sex and ABCB1 Haplotypes

机译:移植后免疫抑制的肾外不良反应与性别和ABCB1单倍型的关系

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Extrarenal adverse effects (AEs) associated with calcineurin inhibitor (CNI) and mycophenolic acid (MPA) occur frequently but are unpredictable posttransplant complications. AEs may result from intracellular CNI accumulation and low activity of P-glycoprotein, encoded by the ABCB1 gene. Since ABCB1 single nucleotide polymorphisms (SNPs) and sex influence P-glycoprotein, we investigated haplotypes and extrarenal AEs. A prospective, cross-sectional study evaluated 149 patients receiving tacrolimus and enteric coated mycophenolate sodium or cyclosporine and mycophenolate mofetil. Immunosuppressive AE assessment determined individual and composite gastrointestinal, neurologic, aesthetic, and cumulative AEs. Lipids were quantitated after 12-hour fast. ABCB1 SNPs: c.1236C>T (rs1128503), c.2677G>T/A (rs2032582 ), and c.3435C>T (rs1045642) were determined with haplotype associations computed using the THESIAS program, and evaluated by immunosuppression, sex and race using multivariate general linear models. Tacrolimus patients exhibited more frequent and higher gastrointestinal AE scores compared with cyclosporine with association to CTT ( P = 0.018) and sex ( P = 0.01). Aesthetic AE score was 3 times greater for cyclosporine with TTC haplotype ( P = 0.005). Females had higher gastrointestinal ( P = 0.022), aesthetic ( P < 0.001), neurologic ( P = 0.022), and cumulative AE ratios ( P < 0.001). Total cholesterol (TCHOL), low-density lipoproteins (LDL), and triglycerides were higher with cyclosporine. The TTC haplotype had higher TCHOL ( P < 0.001) and LDL ( P = 0.005). Higher triglyceride ( P = 0.034) and lower high-density lipoproteins ( P = 0.057) were associated with TTT with sex-adjusted analysis. ABCB1 haplotypes and sex were associated with extrarenal AEs. Using haplotypes, certain female patients manifested more AEs regardless of CNI. Haplotype testing may identify patients with greater susceptibility to AEs and facilitate CNI individualization.
机译:与钙调神经磷酸酶抑制剂(CNI)和麦考酚酸(MPA)相关的肾外不良反应(AEs)频繁发生,但无法预测移植后并发症。 AE可能是由ABCB1基因编码的细胞内CNI积累和P-糖蛋白活性低引起的。由于ABCB1单核苷酸多态性(SNPs)和性别影响P-糖蛋白,我们调查了单倍型和肾外AE。一项前瞻性的横断面研究评估了149例接受他克莫司和肠溶麦考酚酸钠或环孢菌素和霉酚酸酯的患者。免疫抑制性AE评估确定了个体和复合胃肠道,神经系统,美学和累积性AE。禁食12小时后对脂质进行定量。 ABCB1 SNP:c.1236C> T(rs1128503),c.2677G> T / A(rs2032582)和c.3435C> T(rs1045642)通过使用THESIAS程序计算的单倍型关联来确定,并通过免疫抑制,性别和使用多元通用线性模型进行比赛。与环孢素相比,他克莫司患者表现出更频繁和更高的胃肠道AE评分,并伴有CTT(P = 0.018)和性别(P = 0.01)。具有TTC单倍型的环孢霉素的美学AE得分高3倍(P = 0.005)。女性具有较高的胃肠道(P = 0.022),美学(P <0.001),神经系统(P = 0.022)和累积AE比(P <0.001)。环孢素的总胆固醇(TCHOL),低密度脂蛋白(LDL)和甘油三酸酯较高。 TTC单倍型具有较高的TCHOL(P <0.001)和LDL(P = 0.005)。性别校正后的分析表明,较高的甘油三酸酯(P = 0.034)和较低的高密度脂蛋白(P = 0.057)与TTT相关。 ABCB1单倍型和性别与肾外AE相关。使用单倍型,某些女性患者表现出更多的AE,而与CNI无关。单倍型检测可以识别出对AE更易感的患者,并有助于CNI个体化。

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