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Nature vs. Nurture: Defining the Effects of Mesenchymal Stromal Cell Isolation and Culture Conditions on Resiliency to Palmitate Challenge

机译:自然与养育:定义间质基质细胞分离和培养条件对棕榈酸酯挑战的复原力的影响。

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摘要

As MSC products move from early development to clinical translation, culture conditions shift from xeno- to xeno-free systems. However, the impact of isolation and culture-expansion methods on the long-term resiliency of MSCs within challenging transplant environments is not fully understood. Recent work in our lab has shown that palmitate, a saturated fatty acid elevated in the serum of patients with obesity, causes MSCs to convert from an immunosuppressive to an immunostimulatory state at moderate to high physiological levels. This demonstrated that metabolically-diseased environments, like obesity, alter the immunomodulatory efficacy of healthy donor MSCs. In addition, it highlighted the need to test MSC efficacy not only in ideal conditions, but within challenging metabolic environments. To determine how the choice of xeno- vs. xeno-free media during isolation and expansion would affect future immunosuppressive function, umbilical cord explants from seven donors were subdivided and cultured within xeno- (fetal bovine serum, FBS) or xeno-free (human platelet lysate, PLT) medias, creating 14 distinct MSC preparations. After isolation and primary expansion, umbilical cord MSCs (ucMSC) were evaluated according to the ISCT minimal criteria for MSCs. Following baseline characterization, ucMSC were exposed to physiological doses of palmitate and analyzed for metabolic health, apoptotic induction, and immunomodulatory potency in co-cultures with stimulated human peripheral blood mononuclear cells. The paired experimental design (each ucMSC donor grown in two distinct culture environments) allowed us to delineate the contribution of inherent (nature) vs. environmentally-driven (nurture) donor characteristics to the phenotypic response of ucMSC during palmitate exposure. Culturing MSCs in PLT-media led to more consistent growth characteristics during the isolation and expansion for all donors, resulting in faster doubling times and higher cell yields compared to FBS. Upon palmitate challenge, PLT-ucMSCs showed a higher susceptibility to palmitate-induced metabolic disturbance, but less susceptibility to palmitate-induced apoptosis. Most striking however, was that the PLT-ucMSCs resisted the conversion to an immunostimulatory phenotype better than their FBS counterparts. Interestingly, examining MSC suppression of PBMC proliferation at physiologic doses of palmitate magnified the differences between donors, highlighting the utility of evaluating MSC products in stress-based assays that reflect the challenges MSCs may encounter post-transplantation.
机译:随着MSC产品从早期开发过渡到临床翻译,培养条件从无异种系统转变为无异种系统。但是,在挑战性移植环境中,分离和培养扩展方法对MSC长期弹性的影响尚未完全了解。我们实验室的最新工作表明,棕榈酸酯是肥胖症患者血清中升高的一种饱和脂肪酸,可导致MSC在中等至高生理水平下从免疫抑制状态转变为免疫刺激状态。这证明了代谢异常的环境,例如肥胖,改变了健康供体MSC的免疫调节功效。此外,它强调了不仅要在理想条件下,还要在具有挑战性的代谢环境下测试MSC的功效。为了确定在分离和扩增过程中选择异种与无异种培养基会如何影响未来的免疫抑制功能,将来自七个供体的脐带外植体细分并在异种(胎牛血清,FBS)或无异种(人类)中培养。血小板裂解液(PLT)培养基,产生14种不同的MSC制剂。分离和初步扩增后,根据ISCT MSC最低标准评估脐带MSC(ucMSC)。基线表征后,将ucMSC暴露于生理剂量的棕榈酸酯中,并在与刺激的人外周血单核细胞共培养的过程中分析代谢健康,凋亡诱导和免疫调节能力。配对实验设计(每个ucMSC供体在两种不同的培养环境中生长)使我们能够描述固有的(自然)与环境驱动的(培养)供体特征在棕榈酸酯暴露期间对ucMSC的表型反应的贡献。与FBS相比,在PLT培养基中培养MSC可在所有供体的分离和扩增过程中产生更一致的生长特征,从而导致更快的倍增时间和更高的细胞产量。接受棕榈酸酯攻击后,PLT-ucMSCs对棕榈酸酯诱导的代谢紊乱表现出较高的敏感性,但对棕榈酸酯诱导的细胞凋亡的敏感性较低。然而,最引人注目的是,PLT-ucMSC比其FBS同类具有更好的抵抗转化为免疫刺激表型的能力。有趣的是,在生理剂量的棕榈酸酯下检查MSC对PBMC增殖的抑制作用放大了供体之间的差异,突显了在基于压力的测定中评估MSC产品的实用性,反映了MSC在移植后可能遇到的挑战。

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