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用于骨髓移植的全身照射:纪念斯隆凯特琳癌症中心的经验

Total body irradiation for bone marrow transplantation: the Memorial Sloan-Kettering Cancer Center experience.

作者信息

Shank B, O'Reilly R J, Cunningham I, Kernan N, Yaholom J, Brochstein J, Castro-Malaspina H, Kutcher G J, Mohan R, Bonfiglio P

机构信息

Radiation Oncology Department, Memorial Sloan-Kettering Cancer Center, New York, NY.

出版信息

Radiother Oncol. 1990;18 Suppl 1:68-81. doi: 10.1016/0167-8140(90)90180-5.

Abstract

In May 1979, Memorial Sloan-Kettering embarked on a programme of hyperfractionated TBI (HFTBI), 1320 cGy in 11 fractions over 4 days with partial lung shielding (1 HVL), followed by cyclophosphamide (60 mg/kg/d x 2d) for cytoreduction prior to allogeneic bone marrow transplantation (BMT). Anterior and posterior chest wall electron "boosts" were given to the areas blocked (600 cGy in 2 fractions) on the last two days of treatment. Since then, we have treated over 600 patients with HFTBI, the majority for allogeneic BMT. Several modifications have occurred over the years. We have added a "boost" electron dose of 400 cGy to the testes in all male leukemic patients; this reduced testicular relapses from a rate of 14% (4/28) to 0%. In an attempt to increase engraftment of T-depleted BMTs, we added one additional fraction; since our present dose/fraction was also increased to 125 cGy, we now deliver a total dose of 1500 cGy in 12 fractions over 4 days for allogeneic transplants. Tolerance to HFTBI has been excellent relative to the single dose (SD) regimen utilised prior to May, 1979. The incidence of fatal interstitial pneumonitis (IP) decreased from 50% in the SD regimen to 18% after the introduction of HFTBI. In children, the incidence of IP was only 4% with HFTBI. With the introduction of T-depleted marrows, fatal IP in adults has decreased also, e.g. to less than 10% in CML patients. With conventional BMT after HFTBI, relapse at 5 years has been exceedingly low (e.g. in children, 13% for ALL, 2nd remission and 0% for AML, 1st remission) and engraftment has been 100%. With matched T-depleted BMT, rejections have occurred in 15% overall; the incidence of graft failure has not been reduced by the higher dose of HFTBI. Relapses in this setting are equivalent to relapses with conventional BMT for AML, but appear to be increased for ALL. Radiobiological findings related to HFTBI will also be discussed.

摘要

1979年5月,纪念斯隆-凯特琳癌症中心开始了一项超分割全身照射(HFTBI)计划,在4天内分11次给予1320厘戈瑞剂量,同时采用部分肺屏蔽(1个半值层),随后给予环磷酰胺(60毫克/千克/天,共2天)进行细胞减灭,为异基因骨髓移植(BMT)做准备。在治疗的最后两天,对受遮挡区域给予前胸壁和后胸壁电子“增强剂量”(分2次给予600厘戈瑞)。从那时起,我们已经用HFTBI治疗了600多名患者,大多数是进行异基因BMT。多年来,该方案有了一些改进。我们给所有男性白血病患者的睾丸增加了400厘戈瑞的“增强”电子剂量;这使得睾丸复发率从14%(4/28)降至0%。为了提高去除T细胞的BMT的植入率,我们增加了一个照射野;由于我们目前每次照射剂量也增加到了125厘戈瑞,现在对于异基因移植,我们在4天内分12次给予总剂量1500厘戈瑞。相对于1979年5月之前使用的单次照射(SD)方案,HFTBI的耐受性非常好。致命性间质性肺炎(IP)的发生率从SD方案中的50%降至HFTBI引入后的18%。在儿童中,HFTBI治疗时IP的发生率仅为4%。随着去除T细胞骨髓的引入,成人中的致命性IP也有所下降,例如在慢性粒细胞白血病(CML)患者中降至不到10%。采用HFTBI后的传统BMT治疗,5年复发率极低(例如在儿童中,急性淋巴细胞白血病(ALL)第二次缓解期为13%,急性髓系白血病(AML)第一次缓解期为0%),植入率为100%。在匹配的去除T细胞的BMT中,总体排斥率为15%;更高剂量的HFTBI并未降低移植物失败率。在这种情况下,AML的复发率与传统BMT相当,但ALL的复发率似乎有所增加。还将讨论与HFTBI相关的放射生物学研究结果。

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