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Surprisingly, while CMV promoters were not methylated and histone acetylation/methylation was present, these epigenetic markers did not trend with mRNA transcription and protein expression in our TI model. Instead, ATAC-seq data analysis revealed that differences in chromatin accessibility within the TI site could be a major factor impacting these observed differences. However, neither chromatin accessibility nor histone acetylation/methylation profiles in early cultures were predictive of high-expressing clones early during the CLD process. Finally, modulation of the histone profiles (H3K27ac and H3K4me3) at the CMV promoters within the TI integration site using dCas9 fusion proteins was not effective in further increasing mAb titers which could have been likely due to interference of the dCas9 fusion proteins with transcription from the CMV promoters. Overall, our data suggests increasing chromatin accessibility at the TI site is the most effective way to increase mRNA transcription and hence, productivity in TI cell lines.</p>\n </div>","PeriodicalId":134,"journal":{"name":"Biotechnology Journal","volume":"19 10","pages":""},"PeriodicalIF":3.2000,"publicationDate":"2024-10-29","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Chromatin Accessibility Plays an Important Epigenetic Role on Antibody Expression From CMV Promoter and DNA Elements Flanking the CHO TI Host Landing-Pad\",\"authors\":\"Kavya Ganapathy, Andrew McKay, Steffen Durinck, Minyi Shi, Kristel Dorighi, Cynthia Lam, Yuxin Liang, Amy Shen, Gavin Barnard, Shahram Misaghi\",\"doi\":\"10.1002/biot.202400487\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<div>\\n \\n <p>Targeted integration (TI) Chinese hamster ovary (CHO) platforms are commonly used for protein expression. 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引用次数: 0
摘要
靶向整合(TI)中国仓鼠卵巢(CHO)平台通常用于蛋白质表达。然而,表观遗传修饰对 TI 细胞系蛋白质表达的影响仍然难以捉摸,因为几乎所有的表观遗传学研究都集中在相关基因的随机整合(RI)上,而且只在启动子区域内进行。为了研究表观遗传修饰对 TI CHO 细胞的影响,我们利用标准 mAb-1 来鉴定和描述具有相同转基因拷贝数但转基因转录和滴度水平不同的 TI 克隆。令人惊讶的是,虽然 CMV 启动子没有甲基化,组蛋白也存在乙酰化/甲基化,但在我们的 TI 模型中,这些表观遗传标记与 mRNA 转录和蛋白质表达无关。相反,ATAC-seq 数据分析显示,TI 位点内染色质可及性的差异可能是影响这些观察到的差异的主要因素。然而,早期培养物中的染色质可及性和组蛋白乙酰化/甲基化图谱都不能预测CLD过程早期的高表达克隆。最后,使用 dCas9 融合蛋白调节 TI 整合位点内 CMV 启动子的组蛋白图谱(H3K27ac 和 H3K4me3)并不能有效地进一步提高 mAb 滴度,这可能是由于 dCas9 融合蛋白干扰了 CMV 启动子的转录。总之,我们的数据表明,提高 TI 位点染色质的可及性是增加 mRNA 转录从而提高 TI 细胞系产量的最有效方法。
Chromatin Accessibility Plays an Important Epigenetic Role on Antibody Expression From CMV Promoter and DNA Elements Flanking the CHO TI Host Landing-Pad
Targeted integration (TI) Chinese hamster ovary (CHO) platforms are commonly used for protein expression. However, the impact of epigenetic modifications on protein expression in TI cell lines remains elusive since almost all the epigenetic studies focus on random integration (RI) of the gene of interest and only within the promoter region. To address the impact of epigenetic modifications on TI CHO cells, we utilized a standard mAb-1 to identify and characterize TI clones with the same transgene copy numbers but different levels of transgene transcription and titer. Surprisingly, while CMV promoters were not methylated and histone acetylation/methylation was present, these epigenetic markers did not trend with mRNA transcription and protein expression in our TI model. Instead, ATAC-seq data analysis revealed that differences in chromatin accessibility within the TI site could be a major factor impacting these observed differences. However, neither chromatin accessibility nor histone acetylation/methylation profiles in early cultures were predictive of high-expressing clones early during the CLD process. Finally, modulation of the histone profiles (H3K27ac and H3K4me3) at the CMV promoters within the TI integration site using dCas9 fusion proteins was not effective in further increasing mAb titers which could have been likely due to interference of the dCas9 fusion proteins with transcription from the CMV promoters. Overall, our data suggests increasing chromatin accessibility at the TI site is the most effective way to increase mRNA transcription and hence, productivity in TI cell lines.
Biotechnology JournalBiochemistry, Genetics and Molecular Biology-Molecular Medicine
CiteScore
8.90
自引率
2.10%
发文量
123
审稿时长
1.5 months
期刊介绍:
Biotechnology Journal (2019 Journal Citation Reports: 3.543) is fully comprehensive in its scope and publishes strictly peer-reviewed papers covering novel aspects and methods in all areas of biotechnology. Some issues are devoted to a special topic, providing the latest information on the most crucial areas of research and technological advances.
In addition to these special issues, the journal welcomes unsolicited submissions for primary research articles, such as Research Articles, Rapid Communications and Biotech Methods. BTJ also welcomes proposals of Review Articles - please send in a brief outline of the article and the senior author''s CV to the editorial office.
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Omics technologies
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Biosafety, Biotech Ethics, Science Communication
Methods and Advances.