Enschede S H, Shahidi H, Venugopal P, Riley M B, Huang R, Jajeh A, Preisler H D, Gregory S A
Rush Cancer Institute, Chicago, IL 60612, USA.
Leuk Lymphoma. 2001 Jan;40(3-4):325-34. doi: 10.3109/10428190109057931.
Interferon-alfa in combination with cytotoxic chemotherapy has been shown to be effective in treating certain types of non-Hodgkin's lymphoma (NHL) (1). However, there is no published data on upfront induction treatment of aggressive NHL with IFN-alfa containing regimens. Studies have also shown that one can overcome regrowth resistance by administering mid-cycle agents which slow tumor proliferation between courses of cytotoxic therapy (2). Based on this, we treated 32 consecutive patients between 1/93 and 9/96 with a regimen containing cyclophosphamide 750 mg/m2, mitoxantrone 12 mg/m2, and teniposide 60 mg/m2 IV on day 1 with prednisone 100 mg PO given on days 1-5. On day 15, patients received vincristine 1.4 mg/m2 (2 mg max.) and bleomycin 10 units/m2 IV. Interferon-alfa-2b 5x10(6) units/m2 SQ was administered on days 22-26. The median age was 55 (range 26-83), M:F ratio was 2.5:1, and the median International Prognostic Index was 2. 38% of patients had stages I-II and 62% had stages III-IV disease. Fifty-nine percent of the patients achieved a complete response, 22% a partial response, and 19% had progressive disease. The overall survival (OS) was 81% and the progression free survival (PFS) was 56% at 4.3 years. There were no severe (grade IV) hematologic, flu-like, GI and infectious toxicities from IFN-alpha. Leukopenia was the main severe toxicity related to the chemotherapy regimen (days 1-15), but not IFN-alpha. Severe infection secondary to the chemotherapy regimen occurred in one patient. Interferon-alfa-2b and mid-cycle chemotherapy added to an anthracycline based regimen is effective induction treatment for patients with aggressive NHL. The OS and PFS using this regimen, based on regrowth resistance, appears to be at least as or more effective than CHOP therapy for this group of patients. Severe toxicities were rare.
干扰素-α联合细胞毒性化疗已被证明对治疗某些类型的非霍奇金淋巴瘤(NHL)有效(1)。然而,关于含干扰素-α方案对侵袭性NHL进行初始诱导治疗,尚无公开数据。研究还表明,通过给予在细胞毒性治疗疗程之间减缓肿瘤增殖的中期药物,可以克服肿瘤再生长耐药性(2)。基于此,我们在1993年1月至1996年9月期间,连续治疗了32例患者,采用的方案为第1天静脉注射环磷酰胺750mg/m²、米托蒽醌12mg/m²和替尼泊苷60mg/m²,同时第1 - 5天口服泼尼松100mg。第15天,患者接受长春新碱1.4mg/m²(最大剂量2mg)和博来霉素10单位/m²静脉注射。第22 - 26天皮下注射干扰素-α-2b 5×10⁶单位/m²。中位年龄为55岁(范围26 - 83岁),男女比例为2.5:1,中位国际预后指数为2。38%的患者为Ⅰ - Ⅱ期,62%的患者为Ⅲ - Ⅳ期疾病。59%的患者达到完全缓解,22%的患者部分缓解,19%的患者病情进展。4.3年时总生存率(OS)为81%,无进展生存率(PFS)为56%。干扰素-α未引起严重(Ⅳ级)血液学、类流感、胃肠道和感染性毒性。白细胞减少是与化疗方案(第1 - 15天)相关的主要严重毒性,但与干扰素-α无关。化疗方案继发的严重感染发生在1例患者中。在基于蒽环类药物的方案中加入干扰素-α-2b和中期化疗,对侵袭性NHL患者是有效的诱导治疗。基于再生长耐药性,使用该方案的OS和PFS对这组患者似乎至少与CHOP疗法一样有效或更有效。严重毒性罕见。
