Hu Zhengqing, Ulfendahl Mats, Prieskorn Diane M, Olivius Petri, Miller Josef M
Center for Hearing and Communication Research, Karolinska Institute, Stockholm, Sweden.
Otol Neurotol. 2009 Jun;30(4):551-8. doi: 10.1097/MAO.0b013e31819fe70a.
Cell replacement therapy in the inner ear will contribute to the functional recovery of hearing loss.
Cell replacement therapy is a potentially powerful approach to replace degenerated or severely damaged spiral ganglion neurons. This study aimed at stimulating the neurite outgrowth of the implanted neurons and enhancing the potential therapeutic of inner ear cell implants.
Chronic electrical stimulation (CES) and exogenous neurotrophic growth factor (NGF) were applied to 46 guinea pigs transplanted with embryonic dorsal root ganglion (DRG) neurons 4 days postdeafening. The animals were evaluated with the electrically evoked auditory brainstem responses (EABRs) at experimental Days 7, 11, 17, 24, and 31. The animals were euthanized at Day 31, and the inner ears were dissected for immunohistochemistry investigation.
Implanted DRG cells, identified by enhanced green fluorescent protein fluorescence and a neuronal marker, were found close to Rosenthal canal in the adult inner ear for up to 4 weeks after transplantation. Extensive neurite projections clearly, greater than in nontreated animals, were observed to penetrate the bony modiolus and reach the spiral ganglion region in animals supplied with CES and/or NGF. There was, however, no significant difference in the thresholds of EABRs between DRG-transplanted animals supplied with CES and/or NGF and DRG-transplanted animals without CES or NGF supplement.
The results suggest that CES and/or NGF can stimulate neurite outgrowth from implanted neurons, although based on EABR measurement, these interventions did not induce functional connections to the central auditory pathway. Additional time or novel approaches may enhance functional responsiveness of implanted cells in the adult cochlea.
内耳细胞替代疗法将有助于听力损失的功能恢复。
细胞替代疗法是一种潜在的强大方法,用于替代退化或严重受损的螺旋神经节神经元。本研究旨在刺激植入神经元的神经突生长,并增强内耳细胞植入物的潜在治疗效果。
对46只在致聋后4天移植胚胎背根神经节(DRG)神经元的豚鼠应用慢性电刺激(CES)和外源性神经营养生长因子(NGF)。在实验第7、11、17、24和31天用电诱发听性脑干反应(EABR)对动物进行评估。在第31天对动物实施安乐死,并解剖内耳进行免疫组织化学研究。
通过增强绿色荧光蛋白荧光和神经元标记物鉴定的植入DRG细胞,在移植后长达4周的时间里,在成年内耳中靠近罗森塔尔管处被发现。在接受CES和/或NGF的动物中,观察到广泛的神经突投射明显比未治疗的动物更多,穿过骨蜗轴并到达螺旋神经节区域。然而,在接受CES和/或NGF的DRG移植动物与未补充CES或NGF的DRG移植动物之间,EABR阈值没有显著差异。
结果表明,CES和/或NGF可以刺激植入神经元的神经突生长,尽管基于EABR测量,这些干预措施并未诱导与中枢听觉通路的功能连接。延长时间或采用新方法可能会增强成年耳蜗中植入细胞的功能反应性。