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用干细胞激活剂 WNT3A 对自体骨移植物进行再工程化。

Reengineering autologous bone grafts with the stem cell activator WNT3A.

机构信息

Division of Plastic and Reconstructive Surgery, Department of Surgery, Stanford School of Medicine, Stanford, CA 94305, USA.

Dental School University Paris Descartes PRES Sorbonne Paris Cité, EA 2496, Montrouge, France; AP-HP Odontology Department Bretonneau, Hôpitaux Universitaires Paris Nord Val de Seine, Paris, France.

出版信息

Biomaterials. 2015 Apr;47:29-40. doi: 10.1016/j.biomaterials.2014.12.014. Epub 2015 Feb 2.

Abstract

Autologous bone grafting represents the standard of care for treating bone defects but this biomaterial is unreliable in older patients. The efficacy of an autograft can be traced back to multipotent stem cells residing within the bone graft. Aging attenuates the viability and function of these stem cells, leading to inconsistent rates of bony union. We show that age-related changes in autograft efficacy are caused by a loss in endogenous Wnt signaling. Blocking this endogenous Wnt signal using Dkk1 abrogates autograft efficacy whereas providing a Wnt signal in the form of liposome-reconstituted WNT3A protein (L-WNT3A) restores bone forming potential to autografts from aged animals. The bioengineered autograft exhibits significantly better survival in the hosting site. Mesenchymal and skeletal stem cell populations in the autograft are activated by L-WNT3A and mitotic activity and osteogenic differentiation are significantly enhanced. In a spinal fusion model, aged autografts treated with L-WNT3A demonstrate superior bone forming capacity compared to the standard of care. Thus, a brief incubation in L-WNT3A reliably improves autologous bone grafting efficacy, which has the potential to significantly improve patient care in the elderly.

摘要

自体骨移植是治疗骨缺损的标准治疗方法,但这种生物材料在老年患者中不可靠。自体移植物的功效可以追溯到存在于骨移植物中的多能干细胞。随着年龄的增长,这些干细胞的活力和功能减弱,导致骨融合率不一致。我们表明,与年龄相关的自体移植物功效变化是由于内源性 Wnt 信号的丧失引起的。使用 Dkk1 阻断这种内源性 Wnt 信号会破坏自体移植物的功效,而以脂质体重构的 WNT3A 蛋白 (L-WNT3A) 的形式提供 Wnt 信号则可以恢复来自老年动物的自体移植物的成骨潜能。生物工程化的自体移植物在宿主部位的存活率显著提高。L-WNT3A 激活了自体移植物中的间充质和骨骼干细胞群体,细胞有丝分裂活性和成骨分化显著增强。在脊柱融合模型中,用 L-WNT3A 处理的老年自体移植物显示出比标准治疗更好的成骨能力。因此,短暂孵育 L-WNT3A 可可靠地提高自体骨移植的功效,这有可能显著改善老年患者的治疗效果。

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