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Bioengineered vocal fold mucosa for voice restoration

机译:生物工程声带粘膜修复语音

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摘要

Patients with voice impairment caused by advanced vocal fold (VF) fibrosis or tissue loss have few treatment options. A transplantable, bioengineered VF mucosa would address the individual and societal costs of voice-related communication loss. Such a tissue must be biomechanically capable of aerodynamic-to-acoustic energy transfer and high-frequency vibration, and physiologically capable of maintaining a barrier against the airway lumen. Here, we isolated primary human VF fibroblasts and epithelial cells and cocultured them under organotypic conditions. The resulting engineered mucosae showed morphologic features of native tissue, proteome-level evidence of mucosal morphogenesis and emerging extracellular matrix complexity, and rudimentary barrier function in vitro. When grafted into canine larynges ex vivo, the mucosae generated vibratory behavior and acoustic output that were indistinguishable from those of native VF tissue. When grafted into humanized mice in vivo, the mucosae survived and were well tolerated by the human adaptive immune system. This tissue engineering approach has the potential to restore voice function in patients with otherwise untreatable VF mucosal disease.
机译:由晚期声带(VF)纤维化或组织丢失引起的声音障碍患者几乎没有治疗选择。可移植的,生物工程的VF粘膜将解决与语音相关的通讯损失的个人和社会成本。这样的组织必须在生物力学上能够进行气动到声学的能量传递和高频振动,并且在生理上必须能够保持对气道内腔的屏障。在这里,我们分离了原代人VF成纤维细胞和上皮细胞,并在器官型条件下对其进行了共培养。所得的工程化粘膜显示出天然组织的形态学特征,蛋白质组水平的粘膜形态发生和新兴的细胞外基质复杂性的证据,以及体外的基本屏障功能。当离体移植到犬喉中时,粘膜产生的振动行为和声音输出与天然VF组织的声音行为没有区别。当在体内移植到人源化小鼠中时,粘膜存活并被人类适应性免疫系统很好地耐受。这种组织工程方法具有恢复原本无法治疗的VF粘膜疾病患者语音功能的潜力。

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