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Cytokine Consistency Between Bone Marrow and Peripheral Blood in Patients With Philadelphia-Negative Myeloproliferative Neoplasms

机译:费城阴性髓原肿瘤患者骨髓和外周血之间的细胞因子一致性

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Background: Inflammation might play a critical role in the pathogenesis and progression of Philadelphia-negative myeloproliferative neoplasms (Ph ? MPNs) with elevated inflammatory cytokines in peripheral blood (PB). However, the inflammatory status inside the bone marrow (BM), which is the place of malignancy origin and important microenvironment of neoplasm evolution, has not yet been elucidated. Methods: Inflammatory cytokine profiles in PB and BM of 24 Ph-MPNs patients were measured by a multiplex quantitative inflammation array. Cytokines that correlated between PB and BM were selected and then validated by ELISA in a separate cohort of 52 MPN patients. Furthermore, a panel of cytokines was identified and examined for potential application as non-invasive markers for the diagnosis and prediction of fibrosis progress of MPN subtypes. Results: The levels of G-CSF, I-309, IL-1β, IL-1ra, IL-12p40, IL-15, IL-16, M-CSF, MIG, PDGF-BB, and TIMP-1 in BM supernatants were significantly higher than those in PB (all p 0.4 and p 1 group was significantly higher than that in MF ≤ 1 group. Conclusion: Abnormal inflammatory status is present in MPN, especially in its BM microenvironment. Consistency between PB and BM levels was found in multiple inflammatory cytokines. Circulating cytokine levels of BLC, M-CSF, Eotaxin-2, and TIMP-1 reflected inflammation inside BM niche, suggesting potential diagnostic value for MPN subtypes and prognostic value for fibrosis progression.
机译:背景:炎症可能在费城 - 阴性肌酚瘤的发病机制和进展中发挥关键作用,在外周血(Pb)中具有升高的炎性细胞因子。然而,骨髓内部(BM)内的炎症状况,即恶性源性和肿瘤演化的重要微环境,尚未得到阐明。方法:通过多重定量炎症阵列测量24个pH-MPNS患者的PB和BM中的炎症细胞因子谱。选择Pb和BM之间的细胞因子,然后通过ELISA验证在52个MPN患者的单独队列中。此外,鉴定了细胞因子面板,并检查潜在应用作为非侵入性标志物,用于诊断和预测纤维化进展的MPN亚型。结果:GM上清液中的G-CSF,I-309,IL-1β,IL-1RA,IL-12P40,IL-15,IL-16,M-CSF,MIG,PDGF-BB和TIMP-1的水平显着高于Pb(所有P 0.4和P 1组的Pb)显着高于MF≤1组。结论:在MPN中存在异常炎症状态,特别是在其BM MicroEn环境中。发现PB和BM水平之间的一致性在多种炎症细胞因子。循环细胞因子水平的BLC,M-CSF,Eotaxin-2和TIMP-1反射在BM Niche内的反射炎症,表明MPN亚型的潜在诊断价值和纤维化进展的预后值。

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