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间歇性白细胞介素-2用于HIV-1感染的诱导和维持治疗。

Induction and maintenance therapy with intermittent interleukin-2 in HIV-1 infection.

作者信息

Farel Claire E, Chaitt Doreen G, Hahn Barbara K, Tavel Jorge A, Kovacs Joseph A, Polis Michael A, Masur Henry, Follmann Dean A, Lane H Clifford, Davey Richard T

机构信息

Laboratory of Immunoregulation, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Blood. 2004 May 1;103(9):3282-6. doi: 10.1182/blood-2003-09-3283. Epub 2004 Jan 15.

DOI:10.1182/blood-2003-09-3283
PMID:14726376
Abstract

Studies establishing that intermittent subcutaneous interleukin-2 (IL-2) therapy can lead to substantial CD4 cell increases in many HIV-infected patients have generally been of limited duration. We studied 77 patients participating in active longitudinal studies of subcutaneous IL-2 therapy at our center in order to determine the long-term feasibility of this approach. Following initial induction, patients in each trial were eligible to receive intermittent 5-day cycles of subcutaneous IL-2 treatment at individualized doses and frequencies capable of maintaining CD4 counts at postinduction levels. The mean duration of study participation to date is 5.9 years (range, 1.0-9.3 years). Mean baseline CD4 cell count and CD4 percent values of 0.521 x 10(9)/L (521 cells/microL) and 27% have risen to 1.005 x 10(9)/L (1005 cells/microL) and 38%, respectively, at 90 months. The mean number of subcutaneous IL-2 cycles required to achieve and maintain these increases was 10 cycles (range, 3-29 cycles), and the current mean interval of cycling required to maintain these elevations is 39 months (median, 35 months; range, 2-91 months). We conclude that subcutaneous IL-2 therapy is capable of maintaining CD4 cell increases for an extended period using a remarkably low frequency of intermittent cycling. These observations may contribute to patients' acceptance of subcutaneous IL-2 as a favorable long-term treatment strategy.

摘要

多项研究证实,间歇性皮下注射白细胞介素-2(IL-2)疗法可使许多HIV感染患者的CD4细胞显著增加,但这些研究的持续时间通常有限。我们对在本中心参与皮下IL-2治疗积极纵向研究的77名患者进行了研究,以确定该方法的长期可行性。初始诱导后,每个试验中的患者有资格接受间歇性的5天周期皮下IL-2治疗,剂量和频率个体化,以维持诱导后的CD4细胞计数水平。截至目前,研究参与的平均持续时间为5.9年(范围为1.0 - 9.3年)。在90个月时,平均基线CD4细胞计数和CD4百分比值分别从0.521×10⁹/L(521个细胞/微升)和27%升至1.005×10⁹/L(1005个细胞/微升)和38%。实现并维持这些增加所需的皮下IL-2周期平均数量为10个周期(范围为3 - 29个周期),维持这些升高所需的当前平均循环间隔为39个月(中位数为35个月;范围为2 - 91个月)。我们得出结论,皮下IL-2疗法能够以极低的间歇性循环频率长期维持CD4细胞增加。这些观察结果可能有助于患者接受皮下IL-2作为一种良好的长期治疗策略。

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