自体骨髓支持和转移性乳腺癌的骨病。

The Canadian journal of oncology Pub Date : 1995-12-01
J M Nabholtz, T al-Tweigeri, N Jacquelin, P M Venner
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引用次数: 0

摘要

高剂量化疗(HDCT)和自体造血细胞移植作为转移性或局部高危乳腺癌的治疗方法正在研究中。乳腺癌有转移到骨骼和骨髓(BM)的倾向,因此在收集用于自体移植的干细胞时,收获恶性细胞的可能性似乎很高。因此,在移植产品中消除或减少这种污染似乎是强制性的。自体外周血干细胞移植(PBSCT)在提高HDCT可行性方面比自体骨髓移植(ABMT)有显著优势,同时可能限制骨髓污染。仅移植CD34+产物可能是进一步的进展。体外清除癌细胞的作用尚未在ABMT或PBSCT中得到证实。问题仍然是CD34+产物的阳性选择是否足以控制癌细胞污染,或者是否也应该清除该产物。文献综述表明,骨髓污染可能对复发风险有影响,因此可能作为预后不良因素发挥作用。这些数据虽然并不完全适合自体移植,但也引起了人们对HDCT后自体移植时再输注恶性细胞的可能性的关注。在实验室和前瞻性临床试验中解决这些问题是非常必要的。在获得进一步的数据之前,当以治愈为目的对乳腺癌患者进行治疗时,必须考虑到这种风险。
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Autologous bone marrow support and bone disease in metastatic breast cancer.

High-dose chemotherapy (HDCT) and autotransplantation of hematopoietic cell is being investigated as a therapy for either metastatic or localized high-risk breast cancer. Breast cancer has a tendency to metastasize to the bones and the bone marrow (BM) and therefore the probability of harvesting malignant cells when collecting stem cells for autotransplantation appears high. Thus, the elimination or decrease of this contamination in the transplanted product appears mandatory. Autologous peripheral blood stem cell transplantation (PBSCT) has shown significant advantages over autologous bone marrow transplantation (ABMT) in improving the feasibility of HDCT, while possibly limiting the BM contamination. The transplantation of only CD34+ products may even be a further advance. The role of ex vivo purging of cancer cells has not been established in ABMT or PBSCT. The question remains if the positive selection of CD34+ products is sufficient for controlling cancer cell contamination or if this product should be purged as well. The review of the literature suggests that contamination of the bone marrow could have an impact in terms or risk of relapse and could thus play a role as a pejorative prognostic factor. These data, although not totally adequate for the autotransplantation setting, are raising concerns over the probability of reinfusing malignant cells at time of autotransplantation following HDCT. There is a tremendous need to address these concerns in the laboratory along with prospective clinical trials. Until further data is available, this risk must be taken into consideration when patients with breast cancer are treated with curative intent.

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