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自体外周血干细胞移植及移植后即刻采用活化自然杀伤细胞的过继免疫治疗。

Autologous peripheral blood stem cell transplantation and adoptive immunotherapy with activated natural killer cells in the immediate posttransplant period.

作者信息

Lister J, Rybka W B, Donnenberg A D, deMagalhaes-Silverman M, Pincus S M, Bloom E J, Elder E M, Ball E D, Whiteside T L

机构信息

Division of Hematology/Bone Marrow Transplantation, Department of Medicine, Pittsburgh Cancer Institute, Pennsylvania 15213-2582,

出版信息

Clin Cancer Res. 1995 Jun;1(6):607-14.

PMID:9816022
Abstract

Relapse after high-dose chemotherapy supported by peripheral blood stem cell transplantation (HDC-PBSCT) is the main cause of therapeutic failure in patients with lymphoma and breast cancer. Adoptive immunotherapy with activated natural killer (A-NK) cells and interleukin 2 might eliminate surviving residual tumor without adding to toxicity. Eleven patients with relapsed lymphoma and one with metastatic breast cancer were entered on a pilot clinical trial of HDC-PBSCT followed on day 2 after transplant by infusion of cultured autologous A-NK cells. Simultaneously, recombinant human interleukin 2 (rhIL-2) was initiated as a 4-day continuous i.v. infusion at 2 x 10(6) IU/m2/day, referred to as high-dose rhIL-2. Therapy with high-dose rhIL-2 was followed by a 90-day continuous i. v. infusion at 3 x 10(5) IU/m2/day, referred to as low-dose rhIL-2. All patients engrafted and nine completed treatment. Posttransplant days to a neutrophil count of 500/microliter and to a platelet count of 50,000/microliter were similar to comparable patients treated with HDC-PBSCT alone. Generation of A-NK cells for therapy was feasible in all patients except the three patients with Hodgkin's disease, whose cells did not proliferate in culture. Overall toxicity associated with early posttransplant transfer of A-NK cells and interleukin 2 did not differ from that observed with peripheral blood stem cell transplantation alone in comparable patients. There was early amplification of natural killer cell activity in the peripheral blood of four patients that appeared to result from the transfused A-NK cells. Adoptive transfer of A-NK cells and rhIL-2 during the pancytopenic phase after HDC-PBSCT was feasible and well tolerated, did not adversely affect engraftment, and resulted in amplified natural killer activity in the peripheral blood during the immediate posttransplantation period.

摘要

外周血干细胞移植支持下的大剂量化疗(HDC-PBSCT)后复发是淋巴瘤和乳腺癌患者治疗失败的主要原因。采用活化自然杀伤(A-NK)细胞和白细胞介素2进行过继性免疫治疗可能消除残留的存活肿瘤细胞而不增加毒性。11例复发性淋巴瘤患者和1例转移性乳腺癌患者进入了HDC-PBSCT的一项初步临床试验,在移植后第2天通过输注培养的自体A-NK细胞进行后续治疗。同时,开始以2×10⁶IU/m²/天的剂量进行为期4天的重组人白细胞介素2(rhIL-2)持续静脉输注,称为大剂量rhIL-2。大剂量rhIL-2治疗后,接着以3×10⁵IU/m²/天的剂量进行为期90天的持续静脉输注,称为小剂量rhIL-2。所有患者均实现造血干细胞植入,9例完成治疗。移植后达到中性粒细胞计数500/微升和血小板计数50,000/微升的天数与仅接受HDC-PBSCT治疗的可比患者相似。除3例霍奇金病患者的细胞在培养中不增殖外,所有患者均可行用于治疗的A-NK细胞生成。与移植后早期输注A-NK细胞和白细胞介素2相关的总体毒性与可比患者仅接受外周血干细胞移植时观察到的毒性无差异。4例患者外周血中自然杀伤细胞活性早期增强,似乎是由输注的A-NK细胞所致。在HDC-PBSCT后的全血细胞减少期进行A-NK细胞和rhIL-2的过继性转移是可行的,耐受性良好,不影响造血干细胞植入,并在移植后即刻导致外周血中自然杀伤活性增强。

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