Research and Development Laboratory for Biochemical, Molecular and Cellular Applications in Ophthalmological Science, IRCCS-Fondazione Bietti, 00198 Rome, Italy.
Institute of Cell Biology and Neurobiology, CNR, 00143 Rome, Italy.
Int J Mol Sci. 2022 Jun 6;23(11):6337. doi: 10.3390/ijms23116337.
Corroborating data sustain the pleiotropic effect of nerve growth factor (NGF) in the protection of the visual system from dangerous stimuli, including ultraviolet (UV). Since UV exposure might promote ocular surface changes (conjunctival inflammation and matrix rearrangement), as previously reported from in vivo studies sustaining some protective NGF effects, in vitro cultures of human conjunctival fibroblasts (FBs) were developed and exposed to a single UV exposure over 15 min (0.277 W/m), either alone or supplemented with NGF (1-10-100 ng/mL). Conditioned media and cell monolayers were collected and analyzed for protein release (ELISA, ELLA microfluidic) and transcript expression (real-time PCR). A specific "inflammatory to remodeling" pattern (IL8, VEGF, IL33, OPN, and CYR61) as well as a few epigenetic transcripts (known as modulator of cell differentiation and matrix-remodeling ( and )) were investigated in parallel. UV-exposed FBs (i), showed no proliferation or significant cytoskeleton rearrangement; (ii), displayed a trkA/p75 phenotype; and (iii), synthesized/released IL8, VEGF-A, IL33, OPN, and CYR61, as compared to unexposed ones. NGF addition counteracted IL8, IL33, OPN, and CYR61 protein release merely at lower NGF concentrations but not VEGF. NGF supplementation did not affect or transcripts, while it significantly upregulated at lowest NGF doses and did not change expression. Taken together, a single UV exposure activated conjunctival FBs to release pro-inflammatory/fibrogenic factors in association with epigenetic changes. The effects were selectively counteracted by NGF supplementation in a dose-dependent fashion, most probably accountable to the trkA/p75 phenotype. Further in vitro studies are underway to better understand this additional NGF pleiotropic effect. Since UV-shield impairments represent a worldwide alert and UV radiation can slowly affect ocular surface homeostasis (photo-ageing, cataract) or might exacerbate ocular diseases with a preexisting fibrosis (pterygium, VKC), these findings on NGF modulation of UV-exposed FBs might provide additional information for protecting the ocular surface (homeostasis) from low-grade long-lasting UV insults.
证实数据支持神经生长因子 (NGF) 的多效性作用,即在保护视觉系统免受包括紫外线 (UV) 在内的危险刺激方面的作用。由于紫外线照射可能会引起眼表面变化(结膜炎和基质重排),正如之前的活体研究报告中所支持的一些 NGF 保护作用,因此培养了人结膜成纤维细胞 (FB) 的体外培养物,并使其暴露于单次 15 分钟的 UV 照射下(0.277 W/m),或单独暴露,或添加 NGF(1-10-100ng/mL)。收集条件培养基和细胞单层并进行蛋白质释放(ELISA、ELLA 微流控)和转录物表达(实时 PCR)分析。同时研究了特定的“从炎症到重塑”模式(IL8、VEGF、IL33、OPN 和 CYR61)以及一些表观遗传转录物(已知为细胞分化和基质重塑的调节剂)。与未暴露的 FB 相比,暴露于 UV 的 FB(i)显示出无增殖或显著的细胞骨架重排;(ii)显示出 trkA/p75 表型;(iii)合成/释放了 IL8、VEGF-A、IL33、OPN 和 CYR61。NGF 的添加仅在较低 NGF 浓度下拮抗 IL8、IL33、OPN 和 CYR61 的蛋白质释放,但不拮抗 VEGF。NGF 补充剂不影响 或 转录物,但显著上调最低 NGF 剂量的 ,并且不改变 表达。总的来说,单次 UV 照射激活结膜成纤维细胞释放与表观遗传变化相关的促炎/纤维化因子。这种作用通过 NGF 补充以剂量依赖的方式选择性拮抗,最有可能归因于 trkA/p75 表型。正在进行进一步的体外研究以更好地理解这种额外的 NGF 多效性作用。由于 UV 屏蔽损伤是一个全球性的警报,并且 UV 辐射可能会缓慢影响眼表面稳态(光老化、白内障),或者可能会加重已有纤维化的眼部疾病(翼状胬肉、VKC),因此关于 NGF 调节 UV 暴露 FB 的这些发现可能为保护眼表面(稳态)免受低水平长期 UV 损伤提供更多信息。
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