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Syndecan-1 (CD138) Immunoreactivity in Bone Marrow Biopsies of Multiple Myeloma: Shed Syndecan-1 Accumulates in Fibrotic Regions

机译:多发性骨髓瘤骨髓活检中的Syndecan-1(CD138)免疫反应性:脱落的Syndecan-1在纤维化区域积聚。

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Syndecan-1 (CD138) mediates myeloma cell adhesion, and loss of syndecan-1 from the cell surface may contribute to myeloma proliferation and dissemination. Flow cytometry analysis of myeloma cells in bone marrow specimens shows heterogeneity in cell surface syndecan-1 expression. It is not known whether weaker expression correlates with more aggressive disease. However, recent reports suggest that variations in syndecan-1 staining intensity on myeloma cells may be an artifact of specimen handling. In this study, we evaluate syndecan-1 expression in bone marrow biopsy sections from 28 multiple myeloma patients, to elucidate the heterogeneity of syndecan-1 expression in situ. Immunoreactivity for syndecan-1, using the antibody B-B4 (CD138), was found in more than 95% of multiple myeloma cells in 27 of 28 biopsies. However, one biopsy had more than 50% CD138-negative cells and cells with weak CD138 expression were identified in the majority of cases. Loss of syndecan-1 did not appear to relate to myeloma cell differentiation. In addition, syndecan-1 was detected on intravascular and intrasinusoidal myeloma cells suggesting that loss of syndecan-1 may not be required for extramedullary dissemination. Bone marrow biopsies from nine additional patients, with variable CD138 staining intensity on myeloma cells as determined by flow cytometry, were studied by immunohistochemistry. The heterogenous CD138 expression was confirmed in situ, with weakly positive cells concentrated in areas of reticulin fibrosis. These cells had a disrupted pattern of membrane staining in contrast to the strong linear membrane staining seen in the other multiple myeloma cells. In addition, the fibrotic stroma stained intensely for syndecan-1. Accumulation of syndecan-1 within the extracellular matrix of the marrow likely is derived by shedding of the molecule from the surface of myeloma cells. Because syndecan-1 can act to regulate the activity of heparan-binding growth factors, these reservoirs of syndecan-1 may play a critical role in promoting myeloma pathogenesis, or in regeneration of the tumor after chemotherapy.
机译:Syndecan-1(CD138)介导骨髓瘤细胞粘附,而syndecan-1从细胞表面的丢失可能有助于骨髓瘤的增殖和传播。流式细胞仪分析骨髓标本中的骨髓瘤细胞显示细胞表面syndecan-1表达的异质性。尚不清楚表达较弱是否与更具侵略性的疾病有关。但是,最近的报道表明,骨髓瘤细胞上syndecan-1染色强度的变化可能是标本处理的伪影。在这项研究中,我们评估了来自28位多发性骨髓瘤患者的骨髓活检切片中的syndecan-1表达,以阐明syndecan-1表达的原位异质性。在28次活检中的27次中,超过95%的多发性骨髓瘤细胞中发现使用抗体B-B4(CD138)对syndecan-1的免疫反应性。但是,一次活检的CD138阴性细胞超过50%,并且在大多数情况下都鉴定出CD138表达较弱的细胞。 syndecan-1的丢失似乎与骨髓瘤细胞分化无关。另外,在血管内和窦内骨髓瘤细胞上检测到了syndecan-1,这表明髓外传播可能并不需要syndecan-1的丧失。通过免疫组织化学研究了另外9名患者的骨髓活检,通过流式细胞术确定了骨髓瘤细胞上CD138染色强度的变化。在原位证实了异源CD138表达,弱阳性细胞集中在网状蛋白纤维化区域。与在其他多发性骨髓瘤细胞中看到的强线性膜染色相反,这些细胞的膜染色模式被破坏。此外,纤维化基质的syndecan-1染色强烈。 syndecan-1在骨髓细胞外基质中的积累可能是由于分子从骨髓瘤细胞表面脱落而引起的。由于syndecan-1可以调节肝素结合生长因子的活性,因此这些syndecan-1的储库可能在促进骨髓瘤的发病机理或化疗后肿瘤的再生中起关键作用。

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