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Merck
  • Bioengineering of physiologically functional intrinsically innervated human internal anal sphincter constructs.

Bioengineering of physiologically functional intrinsically innervated human internal anal sphincter constructs.

Tissue engineering. Part A (2013-12-18)
Robert R Gilmont, Shreya Raghavan, Sita Somara, Khalil N Bitar
摘要

Muscle replacement for patients suffering from extensive tissue loss or dysfunction is a major objective of regenerative medicine. To achieve functional status, bioengineered muscle replacement constructs require innervation. Here we describe a method to bioengineer functionally innervated gut smooth muscle constructs using neuronal progenitor cells and smooth muscle cells isolated and cultured from intestinal tissues of adult human donors. These constructs expressed markers for contractile smooth muscle, glial cells, and mature neuronal populations. The constructs responded appropriately to physiologically relevant neurotransmitters, and neural network integration was demonstrated by responses to electrical field stimulation. The ability of enteric neuroprogenitor cells to differentiate into neuronal populations provides enormous potential for functional innervation of a variety of bioengineered muscle constructs in addition to gut. Functionally innervated muscle constructs offer a regenerative medicine-based therapeutic approach for neuromuscular replacement after trauma or degenerative disorders.

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Sigma-Aldrich
Monoclonal Anti-Caldesmon (Smooth) antibody produced in mouse, clone hHCD, ascites fluid
Sigma-Aldrich
抗小鼠IgG(全分子)–FITC 绵羊抗, affinity isolated antibody, buffered aqueous solution