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乳腺癌细胞系MDA-MB 231对成熟破骨细胞具有强大而直接的抗凋亡作用。

Breast cancer cell line MDA-MB 231 exerts a potent and direct anti-apoptotic effect on mature osteoclasts.

作者信息

Gallet Marlène, Sévenet Nicolas, Dupont Claude, Brazier Michel, Kamel Saïd

机构信息

Unité d'Etude des Mécanismes de la Résorption Osseuse, UPRES-EA 2086, Faculté de Pharmacie, 1, rue des Louvels, 80037 Amiens Cedex, France.

出版信息

Biochem Biophys Res Commun. 2004 Jun 25;319(2):690-6. doi: 10.1016/j.bbrc.2004.05.033.

Abstract

Cancer cells metastasized to bone stimulate osteoclastogenesis resulting in bone destruction. However, the influence of tumor cells on fully differentiated osteoclasts is much less known. We postulated that breast cancer cells directly stimulate the survival of mature osteoclasts. We thus tested the effect of conditioned media (CM) prepared from MDA-MB-231 cells on the activity and apoptosis of osteoclasts isolated from 10-day-old rabbit long bones. First, we demonstrated that CM increased the bone resorbing activity in our cell model of rabbit mature osteoclasts. Using a highly purified osteoclast cell population, we found that MDA-MB-231 CM dramatically inhibited osteoclast apoptosis. In the presence of 20% CM, apoptosis was decreased by approximately 60%. LY294002, a PI3 kinase inhibitor, strongly prevented the CM anti-apoptotic effect. Neutralizing experiments with human antibody revealed that macrophage-colony stimulating factor originating from MDA-MB 231 cells was possibly involved in the CM anti-apoptotic effect. These results suggest that breast cancer cells, in addition to stimulating osteoclastogenesis, potently inhibit mature osteoclast apoptosis, a mechanism which may greatly contribute to their osteolytic potential.

摘要

转移至骨的癌细胞会刺激破骨细胞生成,导致骨质破坏。然而,肿瘤细胞对完全分化的破骨细胞的影响却鲜为人知。我们推测乳腺癌细胞会直接刺激成熟破骨细胞的存活。因此,我们测试了由MDA-MB-231细胞制备的条件培养基(CM)对从10日龄兔长骨分离出的破骨细胞的活性和凋亡的影响。首先,我们证明CM在我们的兔成熟破骨细胞模型中增加了骨吸收活性。使用高度纯化的破骨细胞群体,我们发现MDA-MB-231 CM显著抑制破骨细胞凋亡。在存在20% CM的情况下,凋亡减少了约60%。PI3激酶抑制剂LY294002强烈阻止了CM的抗凋亡作用。用人抗体进行的中和实验表明,源自MDA-MB 231细胞的巨噬细胞集落刺激因子可能参与了CM的抗凋亡作用。这些结果表明,乳腺癌细胞除了刺激破骨细胞生成外,还能有效抑制成熟破骨细胞凋亡,这一机制可能对其溶骨潜能有很大贡献。

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