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首页> 外文期刊>Stem Cells >IMT504, the prototype of the immunostimulatory oligonucleotides of the PyNTTTTGT class, increases the number of progenitors of mesenchymal stem cells both in vitro and in vivo: potential use in tissue repair therapy.
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IMT504, the prototype of the immunostimulatory oligonucleotides of the PyNTTTTGT class, increases the number of progenitors of mesenchymal stem cells both in vitro and in vivo: potential use in tissue repair therapy.

机译:IMT504是PyNTTTTGT类免疫刺激性寡核苷酸的原型,在体外和体内均可增加间充质干细胞祖细胞的数量:在组织修复治疗中的潜在用途。

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摘要

Bone marrow (BM)-derived adult mesenchymal stem cells (MSCs) have the capacity to differentiate in vitro into different cell lines. This makes them a likely source for application in tissue repair therapies. Here, we report evidence indicating that, both in vivo and in vitro, IMT504, the prototype of the PyNTTTTGT class of immunostimulatory oligonucleotides, significantly increases the number of fibroblast colony-forming units (CFU-Fs) that originate MSCs. When rat BM cells were cultured with IMT504, the mean number of CFU-Fs increased about three times as compared with untreated controls (CFU-F: 19 +/- 6.3 vs. 6.8 +/- 2.0/2 x 10(6) seeded BM cells, p = .03). Furthermore, rats inoculated with IMT504 had a significantly higher number of CFU-Fs both in BM (CFU-F: 124 +/- 33 vs. 38 +/- 17/femur, p = .04) and in peripheral blood (animals with detectable CFU-Fs in circulation 8/12 vs. 2/12, p = .04) as compared with untreated animals. On the other hand, BM-derived adherent cells either treated in vitro withIMT504 or obtained from animals injected with IMT504 possess the capacity to differentiate to the osteogenic and adipogenic cell lineages as regular MSCs. Finally, we found that repair of a bone defect was accelerated in rats injected with IMT504 as compared with control animals (area with consolidated bone: 80% +/- 6.4% vs. 49% +/- 3.5%, p = .03, n = 10 rats per group). Importantly, when two human BM were cultured in the presence of IMT504, the mean number of fibroblastic adherent colonies also increased as compared with controls. These results suggest the possibility of clinical use of IMT504 in bone, and presumably other, tissue repair therapies.
机译:骨髓(BM)衍生的成人间充质干细胞(MSC)具有体外分化为不同细胞系的能力。这使它们成为组织修复治疗中可能的应用来源。在这里,我们报告的证据表明,在体内和体外,IMT504(PyNTTTTGT类免疫刺激性寡核苷酸的原型)都显着增加了起源于MSC的成纤维细胞集落形成单位(CFU-Fs)的数量。用IMT504培养大鼠BM细胞后,CFU-Fs的平均数量与未处理的对照相比增加了大约三倍(CFU-F:19 +/- 6.3与接种的6.8 +/- 2.0 / 2 x 10(6) BM细胞,p = .03)。此外,接种IMT504的大鼠的BM(CFU-F:124 +/- 33 vs. 38 +/- 17 /股骨,p = .04)和外周血(动物的CFU-F数量均显着更高)与未治疗的动物相比,循环中可检测到的CFU-Fs分别为8/12与2/12,p = .04)。另一方面,用IMT504体外处理或从注射IMT504的动物获得的BM来源的贴壁细胞具有与常规MSC分化为成骨和成脂细胞谱系的能力。最后,我们发现与对照组动物相比,注射IMT504的大鼠的骨缺损修复得到了加速(骨合并区域:80%+/- 6.4%vs. 49%+/- 3.5%,p = .03,每组n = 10只大鼠)。重要的是,当在IMT504存在下培养两个人BM时,与对照相比,成纤维细胞粘附集落的平均数也增加了。这些结果表明,IMT504在骨中以及可能在其他组织修复疗法中临床使用的可能性。

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