首页> 美国卫生研究院文献>Bulletin of the New York Academy of Medicine >Low-dose cyclophosphamide and low-dose interleukin-2 for malignant melanoma.
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Low-dose cyclophosphamide and low-dose interleukin-2 for malignant melanoma.

机译:低剂量环磷酰胺和低剂量白介素-2用于恶性黑色素瘤。

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摘要

We have studied the effects of low-dose recombinant interleukin-2 preceded by low-dose cyclophosphamide on malignant melanoma. Thirty eight outpatients aged from 25 to 75 years were treated with interleukin-2, 3.6 million Cetus units/m2 i.v. daily for five days on two successive weeks beginning three days after 350 mg/m2 of intravenous cyclophosphamide. This schedule was repeated at least twice more with a one-week interval between cycles, usually at the same dosage level. Ten of the 38 patients (26.3%) had clinically significant remissions: two complete (5.3%), seven partial (18.4%), and one ongoing, long-term (greater than 18 mo) "minor" response (2.6%). Four others (10.5%) had shorter minor responses and four (10.5%) a mixed response. One patient with disease restricted to the skin had a complete remission, while the other patient with a complete remission had had three lung nodules and an enlarged hilar lymph node. It was gratifying that one of the major sites of disease responding to treatment was the liver. Two complete and two partial remissions (i.e., greater than 50% regressions for greater than four weeks at this site) were obtained in 10 patients with liver involvement. Lung metastases also responded in four of 16 patients (one complete and three partial remissions). Subcutaneous nodules responded in seven of 21 patients (two complete, five partial remissions), while lymph node metastases diminished significantly in four of 14 patients (one complete, three partial remissions). The median duration of response was nine months (range, 1.5-20 months), with four patients treated for more than one year. Toxicity was moderate and controllable, and only two patients required hospitalization, both overnight. Lymphokine activated killer cell activation was induced in 24 of 38 patients, including all nine of the major responders. Conversely, none of 14 patients without lymphokine activated killer cell activation had a significant clinical remission. This regimen appeared to be as effective in melanoma as those involving ex vivo activation of lymphokine activated killer cells, and was more tolerable than therapy with high doses of interleukin-2.
机译:我们已经研究了低剂量的重组白细胞介素2,然后低剂量的环磷酰胺对恶性黑色素瘤的影响。 25名年龄在25至75岁之间的38名门诊患者接受了IL-2的IL-2疗法,治疗量为360万Cetus单位/平方米。从350 mg / m2静脉注射环磷酰胺开始的三天后,连续两周每天五天。通常在相同的剂量水平下,以两次间隔一个星期的间隔重复该计划至少两次。 38例患者中有10例(26.3%)具有临床显着缓解:2例完全缓解(5.3%),7例部分缓解(18.4%)和1例持续的长期(大于18 mo)“轻微”缓解(2.6%)。其他四个(10.5%)的次要反应较短,四个(10.5%)的混合反应。一名患有皮肤疾病的患者已完全缓解,而另一名已完全缓解的患者则出现了三个肺结节和肺门淋巴结肿大。令人欣慰的是,肝脏是治疗的主要疾病之一。在10位有肝脏受累的患者中获得了两次完全缓解和两次部分缓解(即,在该部位的缓解期超过50%超过4周)。 16例患者中有4例也发生了肺转移(1例完全缓解和3例部分缓解)。皮下结节在21例患者中有7例缓解(2个完全缓解,部分缓解5例),而淋巴结转移在14例患者中有4例显着减少(1例完全缓解3例缓解)。中位缓解期为9个月(1.5-20个月),其中四名患者接受了一年以上的治疗。毒性是中度和可控的,只有两名患者需要过夜住院。 38名患者中有24名患者诱导了淋巴因子激活的杀伤细胞激活,包括所有9名主要应答者。相反,没有淋巴因子激活的杀伤细胞激活的14例患者中没有一个具有明显的临床缓解。该方案在黑素瘤中似乎与涉及淋巴因子活化的杀伤细胞的体外活化一样有效,并且比高剂量白介素-2的治疗更耐受。

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