与成簇重复序列相关的早期基因和基因编辑技术对人体器官发育的影响

Alaa Shaheen
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摘要

早期生长应答 1(EGR-1)和同源染色体(Hox)蛋白在调节体内基因、促进细胞更新和加快伤口愈合过程中发挥着至关重要的作用。与此相反,聚类正则间隔排列反转录/相关(CRISPR-Cas)技术主要参与基因编辑。然而,在了解 EGR-1、CRISPR/Cas 和 HOX 基因等关键基因在器官发育中的作用机制方面仍存在很大差距。揭示其机制对于促进器官发育和发现新的治疗策略至关重要。本研究旨在探讨EGR-1、CRISPR/Cas和HOX基因在器官发育和生长中的作用。该研究利用CRISPR/Cas来研究过氧化氢酶突变对器官再生的影响。研究人员将gRNA和Cas9蛋白注入胚胎,产生早期胚胎突变体,然后对幼虫进行断尾。此外,研究还探讨了特定Hox基因在轴突伸长和Wnt信号调节中的作用。TGF-β1诱导的EGR-1促进了胶原蛋白的生成,突出了其在伤口愈合中的重要性。整合 EGR-1、HOX 蛋白和 CRISPR-Cas 发现了影响器官发育的调控复合物。整合 EGR-1、HOX 蛋白和 CRISPR-Cas 发现了一个调控复合物。EGR-1有助于伤口愈合,HOX蛋白影响胎儿发育和器官形成,而CRISPR-Cas则能精确修改基因组。
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The Impact of Early Genes and Gene Editing Technology Associated with Clustered Repeats on the Development of Human Body Organs
Early growth response 1 (EGR-1) and homeobox (Hox) proteins play crucial roles in regulating genes within the body, promoting cell renewal, and expediting the wound healing process. Conversely, Clustered Regularly Interspaced Palindromic Re-peats/Associated (CRISPR-Cas) technology is primarily involved in gene editing. However, significant gaps persist in understanding the mechanisms of key genes like EGR-1, CRISPR/Cas, and HOX genes in organ development. Unveiling their mechanisms is crucial for advancing organ development and discovering new therapeutic strategies. This study aims to investigate the roles of EGR-1, CRISPR/Cas, and HOX genes in organ development and growth. The study used CRISPR/Cas to investigate the impact of catalase mutations on organ regeneration. Early embryonic mutants were generated by injecting gRNAs and Cas9 protein into zygotes, followed by tail amputation in larvae. Additionally, the study explored the role of specific Hox genes in axon elongation and Wnt signaling regulation. EGR-1, induced by TGF-β1, enhanced collagen production, underscoring its importance in wound healing. Integration of EGR-1, HOX proteins, and CRISPR-Cas revealed a regulatory complex influencing organ development. The integration of EGR-1, HOX proteins, and CRISPR-Cas revealed a regulatory complex. EGR-1 aids wound healing, HOX proteins influence fetal development and organ formation, and CRISPR-Cas enables precise genome modifications.
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