首页> 外文期刊>American Journal of Physiology >Endothelial colony-forming cell conditioned media promote angiogenesis in vitro and prevent pulmo-' nary hypertension in experimental bronchopulmonary dysplasia.
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Endothelial colony-forming cell conditioned media promote angiogenesis in vitro and prevent pulmo-' nary hypertension in experimental bronchopulmonary dysplasia.

机译:在实验性支气管肺发育不良中,内皮细胞集落形成细胞条件培养基可促进体外血管生成并预防肺动脉高压。

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Late-outgrowth endothelial colony-forming cells (ECFCs), a type of circulating endothelial progenitor cell (EPC), may contribute to pulmonary angiogenesis during development. Cord blood ECFCs from preterm new-borns proliferate more rapidly than term ECFCs but are more susceptible to the adverse effects of hyperoxia. Recent studies suggest that bone marrow-derived EPCs protect against experimental lung injury via paracrine mechanisms independent of vascular engraftment. To determine whether human umbilical cord blood ECFCs from preterm and term newborns have therapeutic benefit in experimental neonatal lung injury, we isolated cord blood ECFCs from full-term and preterm newborns and prepared ECFC-conditioned medium (CM) to test its therapeutic benefit on fetal pulmonary artery endothelial cell (PAEC) proliferation and function as well as alveolar type 2 (AT2) cell growth. PAECs and AT2 cells were isolated from late-gestation fetal sheep. Additionally, we administered both ECFCs and ECFC-CM to bleomycin-exposed newborn rats, an experimental model of broncho pulmonary dysplasia (BPD). Both term ECFC-CM and preterm ECFC-CM promoted cell growth and angiogenesis in vitro. However, when ECFC-CM was. collected during exposure to mild hyperoxia, the benefit of preterm ECFC-CM was no longer observed. In the bleomycin model of BPD, treatment with ECFC-CM (or CM from mature EC) effectively decreased right ventricular hypertrophy but had no effect on alveolar septation. We conclude that term ECFC-CM is beneficial both in vitro and in experimental BPD. During oxidative stress, preterm ECFC-CM, but not term ECFC-CM, loses its benefit. The inability of term ECFC-CM to promote alveolarization may limit its therapeutic potential.
机译:晚期内皮细胞集落形成细胞(ECFC)是一种循环内皮祖细胞(EPC),在发育过程中可能有助于肺血管新生。早产儿的脐带血ECFC的增殖比足月ECFC的增殖更快,但更容易遭受高氧血症的不利影响。最近的研究表明,骨髓来源的EPC通过独立于血管植入的旁分泌机制保护免受实验性肺损伤。为了确定早产和足月新生儿的脐带血ECFC在实验性新生儿肺损伤中是否具有治疗益处,我们从足月和早产新生儿中分离了脐带血ECFC,并准备了ECFC条件培养基(CM)以测试其对胎儿的治疗益处肺动脉内皮细胞(PAEC)的增殖和功能以及2型肺泡(AT2)细胞的生长。 PAECs和AT2细胞是从妊娠晚期胎羊中分离出来的。此外,我们还向暴露于博来霉素的新生大鼠施用了ECFC和ECFC-CM,这是支气管肺发育不良(BPD)的实验模型。 ECFC-CM和早产ECFC-CM均可在体外促进细胞生长和血管生成。但是,当时是ECFC-CM。在暴露于轻度高氧期间收集到的碳,不再观察到早产ECFC-CM的益处。在BPD博来霉素模型中,ECFC-CM(或成熟EC的CM)治疗可有效减轻右心室肥大,但对肺泡分隔没有影响。我们得出结论,术语ECFC-CM在体外和实验性BPD中均有益。在氧化应激期间,早产ECFC-CM(而非ECFC-CM)会失去其优势。术语ECFC-CM无法促进肺泡化可能会限制其治疗潜力。

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