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Biomaterials-enabled cornea regeneration in patients at high risk for rejection of donor tissue transplantation

机译:高风险的供体组织移植排斥患者中使用生物材料的角膜再生

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摘要

The severe worldwide shortage of donor organs, and severe pathologies placing patients at high risk for rejecting conventional cornea transplantation, have left many corneal blind patients untreated. Following successful pre-clinical evaluation in mini-pigs, we tested a biomaterials-enabled pro-regeneration strategy to restore corneal integrity in an open-label observational study of six patients. Cell-free corneal implants comprising recombinant human collagen and phosphorylcholine were grafted by anterior lamellar keratoplasty into corneas of unilaterally blind patients diagnosed at high-risk for rejecting donor allografts. They were followed-up for a mean of 24 months. Patients with acute disease (ulceration) were relieved of pain and discomfort within 1–2 weeks post-operation. Patients with scarred or ulcerated corneas from severe infection showed better vision improvement, followed by corneas with burns. Corneas with immune or degenerative conditions transplanted for symptom relief only showed no vision improvement overall. However, grafting promoted nerve regeneration as observed by improved touch sensitivity to near normal levels in all patients tested, even for those with littleo sensitivity before treatment. Overall, three out of six patients showed significant vision improvement. Others were sufficiently stabilized to allow follow-on surgery to restore vision. Grafting outcomes in mini-pig corneas were superior to those in human subjects, emphasizing that animal models are only predictive for patients with non-severely pathological corneas; however, for establishing parameters such as stable corneal tissue and nerve regeneration, our pig model is satisfactory. While further testing is merited, we have nevertheless shown that cell-free implants are potentially safe, efficacious options for treating high-risk patients.
机译:全球范围内供体器官严重短缺,严重的病理使患者处于拒绝常规角膜移植的高风险中,使许多角膜盲患者得不到治疗。在对小型猪进行成功的临床前评估之后,我们在六名患者的开放标签观察研究中测试了生物材料促成的再生策略,以恢复角膜完整性。通过前板状角膜移植术将包含重组人胶原蛋白和磷酸胆碱的无细胞角膜植入物移植到被诊断为拒绝供体同种异体移植的高风险的单侧盲患者的角膜中。平均随访24个月。患有急性疾病(溃疡)的患者在术后1-2周内缓解了疼痛和不适。严重感染导致角膜瘢痕形成或溃疡的患者视力改善更好,其次是角膜烧伤。具有免疫或退行性疾病症状缓解的角膜移植仅显示整体视力没有改善。但是,在所有接受测试的患者中,即使对治疗前几乎没有/没有敏感性的患者,通过将触觉敏感性提高到接近正常水平,移植可以促进神经再生。总体而言,六分之三的患者显示出明显的视力改善。其他患者则足够稳定,可以进行后续手术以恢复视力。小型猪角膜的移植效果优于人类受试者,强调动物模型仅可预测非严重病理性角膜的患者。但是,对于建立稳定的角膜组织和神经再生等参数,我们的猪模型是令人满意的。尽管还需要进行进一步的测试,但我们已经表明,无细胞植入物是治疗高危患者的潜在安全,有效的选择。

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