Andrea Barabino, Katia Mellal, Rimi Hamam, Anna Polosa, May Griffith, Jean-François Bouchard, Ananda Kalevar, Roy Hanna, Gilbert Bernier
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引用次数: 0
摘要
视网膜退行性疾病影响着全世界数百万人,而法定失明通常与位于视网膜中心区域黄斑的锥状光感受器的丧失有关。目前还没有替代黄斑的治疗方法。为了解决这一未满足的需求,我们采用对照等基因和低免疫原性诱导多能干细胞系来产生自发极化视网膜片(RSs)。视网膜祖细胞和视锥前体细胞中含有丰富的RSs,长期培养可分化为成熟的S-和M/ l -视锥细胞。单细胞RNA-seq分析表明,RSs再现了发育中的人视网膜的个体发生。分离神经花环用于视网膜下移植有效地消除了RPE细胞等不需要的细胞。在化学诱导的猪视网膜变性模型中,移植物整合了宿主视网膜,形成了一个新的、尚未成熟的感光层。在一个移植动物中,功能和免疫组织化学分析表明移植物对光刺激表现出反应性,并与宿主双极神经元建立了假定的突触连接。这项研究强调了RSs在临床应用中的潜力和挑战。
Molecular characterization and sub-retinal transplantation of hypoimmunogenic human retinal sheets in a minipig model of severe photoreceptor degeneration.
Retinal degenerative diseases affect millions of people worldwide, and legal blindness is generally associated with the loss of cone photoreceptors located in the central region of the retina called the macula. Currently, there is no treatment to replace the macula. Addressing this unmet need, we employed control isogenic and hypoimmunogenic induced pluripotent stem cell lines to generate spontaneously polarized retinal sheets (RSs). RSs were enriched in retinal progenitor and cone precursor cells, which could differentiate into mature S- and M/L-cones in long-term cultures. Single-cell RNA-seq analysis showed that RSs recapitulate the ontogeny of the developing human retina. Isolation of neural rosettes for sub-retinal transplantation effectively eliminated unwanted cells such as RPE cells. In a porcine model of chemically induced retinal degeneration, grafts integrated the host retina and formed a new, yet immature, photoreceptor layer. In one transplanted animal, functional and immunohistochemical assays suggest that grafts exhibited responsiveness to light stimuli and established putative synaptic connections with host bipolar neurons. This study underscores the potential and challenges of RSs for clinical applications.
期刊介绍:
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