Jacobsen P, Rossing K, Rossing P, Tarnow L, Mallet C, Poirier O, Cambien F, Parving H H
Steno Diabetes Center, Gentofte, Denmark.
Kidney Int. 1998 Apr;53(4):1002-6. doi: 10.1111/j.1523-1755.1998.00847.x.
The antiproteinuric effect of angiotensin converting enzyme (ACE) inhibition in insulin-dependent diabetes mellitus (IDDM) patients with diabetic nephropathy varies considerably. Therefore, we tested the potential role of an insertion (I)/deletion (D) polymorphism of the ACE gene on this early antiproteinuric responsiveness in an observational follow-up study. Sixty (II, N = 13; ID, N = 26 and DD, N = 21) young hypertensive IDDM patients suffering from diabetic nephropathy were investigated during three months before and for the initial six month period during ACE inhibition [captopril 44 (SD 22) mg/24 hr, no differences in drug dose between groups]. Blood pressure (MABP) and albuminuria (ELISA) were measured three (1 to 6) times before and three (1 to 13) times during ACE inhibition. At baseline the groups (II/ID/DD) had comparable (1) mean arterial blood pressure (MABP mm Hg) of 113 +/- 10/108 +/- 9/114 +/- 8, (2) albuminuria (geometric mean with 95% CI) 1394 (747 to 2608)/1176 (844 to 1797) and 1261 (827 to 2017) mg/24 hr, and (3) serum creatinine (geometric mean with 95% CI), 80 (68 to 93)/85 (76 to 97)/103 (85 to 119) mumol/liter, respectively. Angiotensin converting enzyme inhibition induced a significant reduction in MABP, albuminuria and kidney function in all three groups (II/ID/DD; P < 0.05): (1) MABP (mean +/- SD) 12 +/- 7/5 +/- 7/8 +/- 9 mm Hg (ANOVA, P = 0.02); (2) albuminuria [mean (95% CI)] 61 (34 to 77)/22 (3 to 37)/31 (13 to 46) %, (ANOVA, P < 0.01); and (3) increasing serum creatinine [mean (95% CI)] 8 (4 to 12)/9 (3 to 16)/8 (0 to 16) % (ANOVA, NS), respectively. Adjusting for differences in reduction in MABP did not change the association between decrease in albuminuria and ACE/ID genotypes (P < 0.01). A multiple linear regression analysis revealed that the ACE/ID polymorphism, albuminuria and MABP at baseline independently influenced the decline in albuminuria after initiation of ACE inhibition (R2 = 0.21, P < 0.01). A significant association between changes in MABP and albuminuria was demonstrated (R2 = 0.16, P < 0.01). Our data show that hypertensive albuminuric IDDM patients with the II genotype are particularly susceptible to commonly advocated renoprotective treatment.
血管紧张素转换酶(ACE)抑制剂对胰岛素依赖型糖尿病(IDDM)合并糖尿病肾病患者的抗蛋白尿作用差异很大。因此,在一项观察性随访研究中,我们检测了ACE基因插入(I)/缺失(D)多态性对这种早期抗蛋白尿反应性的潜在作用。对60例(II型,N = 13;ID型,N = 26;DD型,N = 21)患有糖尿病肾病的年轻高血压IDDM患者在ACE抑制治疗前3个月及开始治疗的最初6个月期间进行了研究[卡托普利44(标准差22)mg/24小时,各组药物剂量无差异]。在ACE抑制治疗前测量血压(平均动脉压)和蛋白尿(酶联免疫吸附测定法)3次(第1至6次),治疗期间测量3次(第1至13次)。基线时,各组(II/ID/DD)具有可比性:(1)平均动脉血压(MABP,毫米汞柱)分别为113±10/108±9/114±8;(2)蛋白尿(几何平均数及95%可信区间)分别为1394(747至2608)/1176(844至1797)和1261(827至2017)mg/24小时;(3)血清肌酐(几何平均数及95%可信区间)分别为80(68至93)/85(76至97)/103(85至119)μmol/升。ACE抑制治疗在所有三组(II/ID/DD)中均导致MABP、蛋白尿和肾功能显著降低(P < 0.05):(1)MABP(平均值±标准差)降低12±7/5±7/8±9毫米汞柱(方差分析,P = 0.02);(2)蛋白尿[平均值(95%可信区间)]降低61(34至77)/22(3至37)/31(13至46)%(方差分析,P < 0.01);(3)血清肌酐升高[平均值(95%可信区间)]8(4至12)/9(3至16)/8(0至16)%(方差分析,无显著性差异)。校正MABP降低的差异后,蛋白尿降低与ACE/ID基因型之间的关联未改变(P < 0.01)。多元线性回归分析显示,ACE/ID多态性、基线时的蛋白尿和MABP独立影响ACE抑制治疗开始后蛋白尿的下降(R2 = 0.21,P < 0.01)。MABP变化与蛋白尿之间存在显著关联(R2 = 0.16,P < 0.01)。我们的数据表明,II基因型的高血压蛋白尿IDDM患者对普遍提倡的肾脏保护治疗特别敏感。
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