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白细胞介素-2免疫疗法对肾功能的影响。

Effects of interleukin-2 immunotherapy on renal function.

作者信息

Kozeny G A, Nicolas J D, Creekmore S, Sticklin L, Hano J E, Fisher R I

机构信息

Department of Medicine, Loyola University Medical Center, Maywood, IL 60153.

出版信息

J Clin Oncol. 1988 Jul;6(7):1170-6. doi: 10.1200/JCO.1988.6.7.1170.

Abstract

Recombinant interleukin-2 (IL-2) infusions have recently been evaluated as a new form of immunotherapy for the treatment of malignancies. This form of therapy has been complicated by the development of fluid retention, azotemia, and hypophosphatemia. To evaluate the effects of IL-2 on renal function, we prospectively studied eight patients who received IL-2 (10(5) micron/kg every eight hours intravenously [IV]) for five days as the initial phase of a treatment protocol using IL-2 plus lymphokine activated killer (LAK) cells. Dopamine and fluids were used to maintain blood pressure and all patients received indomethacin (100 mg/d). IL-2 therapy produced a syndrome similar to endotoxemia with the development of respiratory alkalosis (pH = 7.44 +/- .2, pCO2 = 30 +/- 2) and hypotension (mean BP, 71.3 mm Hg). These changes were accompanied by marked sodium avidity, edema formation, and mild elevations of BUN and creatinine. Hypophosphatemia, hypocalcemia, and hypomagnesemia were commonly seen. No defects in renal calcium, magnesium, phosphorous, net acid excretion, or glycosuria were demonstrated. We conclude: (1) IL-2 induces an increase in vascular permeability causing the development of edema, sodium avidity, and prerenal azotemia as occurs during endotoxemia; (2) IL-2 therapy induces respiratory alkalosis with the subsequent intracellular shift of phosphorous accompanied by increased renal phosphorous reabsorption; and (3) there is no evidence of renal tubular dysfunction (renal tubular acidosis [RTA], renal leak of glucose, phosphorous, or magnesium).

摘要

重组白细胞介素-2(IL-2)输注最近被评估为一种用于治疗恶性肿瘤的新型免疫疗法。这种治疗形式因出现液体潴留、氮质血症和低磷血症而变得复杂。为了评估IL-2对肾功能的影响,我们前瞻性地研究了8例患者,他们接受IL-2(每8小时静脉注射[IV]10⁵微克/千克),持续5天,作为使用IL-2加淋巴因子激活的杀伤细胞(LAK)的治疗方案的初始阶段。使用多巴胺和液体维持血压,所有患者均接受吲哚美辛(100毫克/天)。IL-2治疗产生了一种类似于内毒素血症的综合征,出现呼吸性碱中毒(pH = 7.44±0.2,pCO₂ = 30±2)和低血压(平均血压,71.3毫米汞柱)。这些变化伴有明显的钠潴留、水肿形成以及血尿素氮和肌酐轻度升高。低磷血症、低钙血症和低镁血症很常见。未发现肾钙、镁、磷、净酸排泄或糖尿方面的缺陷。我们得出结论:(1)IL-2诱导血管通透性增加,导致水肿、钠潴留和肾前性氮质血症的发生,如同内毒素血症期间那样;(2)IL-2治疗诱导呼吸性碱中毒,随后磷发生细胞内转移,并伴有肾磷重吸收增加;(3)没有证据表明存在肾小管功能障碍(肾小管酸中毒[RTA]、肾性葡萄糖、磷或镁泄漏)。

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