口服抗利尿激素V2受体拮抗剂VPA-985治疗伴肝硬化或抗利尿激素分泌不当综合征的低钠血症患者溶质排泄的差异

G. Decaux
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引用次数: 62

摘要

VPA-985是一种口服活性的抗利尿激素V(2)受体拮抗剂,在正常人中增加水排泄而不影响溶质排泄。由于抗利尿激素(SIADH)分泌不当或使用VPA-985治疗肝硬化导致的低钠血症患者的溶质排泄是否受到影响尚不清楚。6例低钠血症合并SIADH患者和5例低钠血症合并肝硬化合并腹水炎(CWAs)患者接受50或100 mg VPA-985治疗,每日2次。测定肌酐、尿素、尿酸、钠、钾和渗透清除率的变化。同时测定治疗前后血浆肾素(PR)、醛固酮(醛固酮)、抗利尿激素(ADH)、房利钠因子(ANF)。SIADH患者的血清钠浓度(SNa)通常在1天内得到纠正(SNa: t = 0小时时126 +/- 4.5 mmol/L, t = 24小时时133 +/- 5.6 mmol/L),并与钠排泄减少相关(从82 +/- 22 mmol/24小时降至45 +/- 21 mmol/24小时;P < 0.05),钾排泄量无明显变化。尽管利尿增加(从0.84 +/- 0.2 ml/min增加到1.46 +/- 0.4 ml/min),但尿素和尿酸清除率下降。尿渗透压从414 +/- 148 mOsm/kg H(2)O降至209 +/- 55 mOsm/kg H(2)O。激素量没有变化。在CWAs中,SNa的上升更为渐进(t = 0时SNa为126 +/- 2.8 mmol/L, t = 48小时时为133 +/- 4.9 mmol/L),并与钠排泄的增加平行(从23 +/- 18 mmol/24小时增加到VPA给药第二天的65 6 60 mmol/24小时)。高钠排泄也与钾排泄的进展有关(从22 6 7 mmol/24小时到36 +/- 18 mmol/24小时)。VPA下利尿从0.42 +/- 0.2 mL/min增加到1.7 +/- 0.9 mL/min,导致尿素清除率升高。尿液渗透压由VPA前的509 +/- 142 mOsm/kg H(2)O降至VPA后的194 +/- 106 mOsm/kg H(2)O。VPA处理的CWAs ADH升高,从1.9 +/- 1.2 pg/mL增加到5.3 +/- 2.8 pg/mL (P < 0.05),而其他体积激素没有变化。VPA-985是一种短期治疗伴有SIADH或CWAs的低钠血症患者的高效药物。在SIADH中,SNa校正与尿钠潴留有关,而在CWAs中,观察到钠排泄轻度增加。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Difference in solute excretion during correction of hyponatremic patients with cirrhosis or syndrome of inappropriate secretion of antidiuretic hormone by oral vasopressin V2 receptor antagonist VPA-985.
VPA-985 is an orally active, competitive vasopressin V(2) receptor antagonist that in normal human beings increases water excretion without affecting solute excretion. Whether solute excretion is affected in patients with hyponatremia resulting from inappropriate secretion of antidiuretic hormone (SIADH) or from cirrhosis treated with VPA-985 is unknown. Six hyponatremic patients with SIADH and 5 hyponatremic patients with cirrhosis with ascitis (CWAs) were treated with 50 or 100 mg VPA-985 twice daily. Evolution of creatinine, urea, uric acid, sodium, potassium, and osmotic clearance were determined. Volume hormones (plasma renin [PR], aldosterone, antidiuretic hormone [ADH], atrial natriuretic factor [ANF]) were also determined before and after treatment. In patients with SIADH, serum sodium concentration (SNa) was generally corrected in 1 day (SNa: 126 +/- 4.5 mmol/L at t = 0 hours and 133 +/- 5.6 mmol/L at t = 24 hours) and associated with a decrease in sodium excretion (from 82 +/- 22 mmol/24 hours to 45 +/- 21 mmol/24 hours; P < 0.05) without modification in potassium excretion. Despite an increase in diuresis (from 0.84 +/- 0.2 ml/min to 1.46 +/- 0.4 ml/min) urea and uric acid clearances decreased. Urine osmolality decreased from 414 +/- 148 mOsm/kg H(2)O to 209 +/- 55 mOsm/kg H(2)O. Volume hormones did not change. In the CWAs the rise of SNa was more progressive (SNa: 126 +/- 2.8 mmol/L at t = H0 to 133 +/- 4.9 mmol/L at t = 48 hours) and parallel to an augmentation in sodium excretion (from 23 +/- 18 mmol/24 hours to 65 6 60 mmol/24 hours the second day of VPA administration). The higher sodium excretion was also connected with a progression in potassium excretion (from 22 6 7 mmol/24 hours to 36 +/- 18 mmol/24 hours). The increase in diuresis under VPA from 0.42 +/- 0.2 mL/min to 1.7 +/- 0.9 mL/min resulted in a higher urea clearance. Urine osmolality decreased from 509 +/- 142 mOsm/kg H(2)O before VPA to 194 +/- 106 mOsm/kg H(2)O after VPA. ADH increased in CWAs treated with VPA, from 1.9 +/- 1.2 pg/mL to 5.3 +/- 2.8 pg/mL (P <.05) while other volume hormones did not change. VPA-985 is a highly effective drug in the short-term management of hyponatremic patients with SIADH or CWAs. SNa correction is associated with urinary sodium retention in SIADH, whereas in CWAs a mild increase in sodium excretion is observed.
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