Synthetic tools conduct messages from station to station in DNA

Rice lab uses customized Cas9 editors to dissect how genetic elements communicate

Bioengineers used deactivated Cas9 fusion proteins to synthetically control gene expression and reveal new details about natural processes in human cells.

Rice University researchers have demonstrated that CRISPR-Cas9, increasingly famous as a gene-editing tool, can be employed in powerful additional ways in human cells.

A team led by Rice bioengineer Isaac Hilton and graduate student Kaiyuan Wang used deactivated Cas9 (dCas9) proteins to target key segments of the human genome and synthetically trigger the transcription of human genes.

Rice University bioengineers are using deactivated Cas9 proteins to target key segments of the human genome and synthetically trigger the transcription of human genes. Illustration by Sofia Escobar
Rice bioengineers are using deactivated Cas9 proteins to target key segments of the human genome and synthetically trigger the transcription of human genes. Illustration by Sofia Escobar

By using dCas9 to recruit proteins that can naturally turn genes on, the Rice team was able to reveal important details about human promoters and enhancers – the pieces of our DNA that coordinate when, and to what extent, our genes are turned on – which in turn controls the behaviors of our cells.

“We’re using these synthetic biology tools to improve the ability to engineer gene expression and program human cells, and consequently to better understand how our genes work naturally,” Hilton said. “These types of studies are important because in the long run this knowledge and these technical capabilities can enable better gene and cell therapies and biotechnologies.”

Hilton said the study in Nucleic Acids Research highlights the growing potential of CRISPR-Cas9-based tools for synthetic gene control and cellular engineering. The team’s strategy also demonstrates the power of dCas9 to influence and understand the epigenetic factors that animate the human genome.

“Only around 2% of our genome contains protein-coding genes, and the remaining 98% is so-called noncoding DNA,” Hilton said. “Enhancers and promoters are key parts of our noncoding genomes and, although the vast majority of these elements do not make conventional genes, there is fascinating genetic variation in noncoding DNA. This variation gives us the magnificent diversity that enables our species to be both amazing and adaptable.

“However, genetic variation in noncoding DNA is also strongly correlated with many diseases, and even subtle differences in these regions can be linked to pathologies,” he said. “A pressing challenge is that it is often very difficult to pinpoint how these differences influence disease onset and treatments.

Isaac Hilton, left, and Kaiyuan Wang led a Rice University study to uncover mechanistic details orchestrating cellular transcription.
Isaac Hilton, left, and Kaiyuan Wang led a Rice University study to uncover mechanistic details orchestrating cellular transcription. 

“Our goal and our hope is that technologies and approaches like ours can help researchers get closer to making those important connections, and to ultimately predict and thoughtfully intervene in disease,” Hilton said.

By synthetically activating noncoding DNA, the researchers demonstrated how promoters – short DNA sequences that mark the start sites of genes – and enhancers can communicate. Remarkably, enhancers can be thousands of base pairs away from their promoters but can stimulate gene transcription by recruiting activator proteins and by forming direct physical contacts with associated promoters.

“Enhancers can also sometimes make mysterious transcripts called enhancer RNAs (eRNAs),” Hilton said. “Kai showed that CRISPR technologies can be used to turn on these eRNAs, and that in some cases, this fosters a type of genomic tracking, wherein an enhancer can be dragged along DNA to engage with downstream promoters.

“It also appears that along the way, vital transcriptional and epigenetic information can be deposited,” he said. “It is exciting to speculate that this information could serve as sort of gene expression bookmarking that reinforces subsequent rounds of transcription in a type of positive epigenetic feedback.”

Their strategy revealed that enhancers and promoters can have “intrinsic reciprocity.” While they knew that signals can be transmitted from an enhancer to a promoter, they learned that this transmission can go the other way as well.

“We see regulation taking place from a promoter to an upstream enhancer,” Wang said. “Mechanistically, that’s considered noncanonical and thus rather surprising.”

They also found that CRISPR activators can increase the frequency of physical contacts between enhancers and promoters, but only when targeted to an enhancer, suggesting a sort of one-way street for increasing physical contacts.

“We now know that these pieces of DNA can send messages in both directions, but that there appears to be an significant aspect of directionality for physical contact,” Hilton said. “There is certainly reciprocity, but it seems that the predominant regulatory mode here is one in which an enhancer tracks toward a corresponding promoter or promoters.”

The researchers said their study is only possible because of CRISPR-Cas9 advances. “Without these genomic targeting tools, we would have to use other more invasive and disruptive synthetic methods, like knocking out or genetically modifying a regulatory element,” Wang said. “Our approaches here make it easier to epigenetically hijack or repurpose native cellular mechanisms to precisely understand and engineer how genes are controlled.”

Co-authors of the paper include Rice postdoctoral researchers Jing Li and Barun Mahata, graduate students Mario Escobar and Jacob Goell, and undergraduates Spencer Shah and Madeleine Cluck. Hilton is an assistant professor of bioengineering and biosciences, and a CPRIT Scholar in Cancer Research.

The Cancer Prevention and Research Institute of Texas (RR170030) and the National Institutes of Health (R35GM143532) supported the research.

Peer-reviewed research

“Systematic comparison of CRISPR-based transcriptional activators uncovers gene-regulatory features of enhancer-promoter interactions" | Nucleic Acids Research | DOI: 10.1093/nar/gkac582

https://academic.oup.com/nar/advance-article/doi/10.1093/nar/gkac582/6643103?searchresult=1

Images for download

Rice University bioengineers are using deactivated Cas9 proteins to target key segments of the human genome and synthetically trigger the transcription of human genes. (Credit: Illustration by Sofia Escobar/Hilton Lab)

https://news-network.rice.edu/news/files/2022/07/0711_GENE-2a-web.jpg

Rice University bioengineers are using deactivated Cas9 proteins to target key segments of the human genome and synthetically trigger the transcription of human genes. (Credit: Illustration by Sofia Escobar/Hilton Lab)

Isaac Hilton, left, and Kaiyuan Wang led a Rice University study to uncover mechanistic details orchestrating cellular transcription. (Credit: Rice University)

https://news-network.rice.edu/news/files/2022/07/0711_GENE-1-WEB.jpg

Isaac Hilton, left, and Kaiyuan Wang led a Rice University study to uncover mechanistic details orchestrating cellular transcription. (Credit: Rice University)

Related materials

CPRIT grant brings epigenetics researcher to Rice: https://news2.rice.edu/2017/05/22/cprit-grant-brings-epigenetics-researcher-to-rice-2/

Trailblazing Rice bioengineer is turning cells into disease fighters: https://news2.rice.edu/2017/05/22/cprit-grant-brings-epigenetics-researcher-to-rice-2/

New CRISPR tech targets human genome’s complex code: https://news.rice.edu/news/2021/new-crispr-tech-targets-human-genomes-complex-code

Hilton Lab: https://hiltonlab.rice.edu

Department of Bioengineering: https://bioengineering.rice.edu

George R. Brown School of Engineering: https://engineering.rice.edu

About Rice

Located on a 300-acre forested campus in Houston, Rice University is consistently ranked among the nation’s top 20 universities by U.S. News & World Report. Rice has highly respected schools of Architecture, Business, Continuing Studies, Engineering, Humanities, Music, Natural Sciences and Social Sciences and is home to the Baker Institute for Public Policy. With 4,240 undergraduates and 3,972 graduate students, Rice’s undergraduate student-to-faculty ratio is just under 6-to-1. Its residential college system builds close-knit communities and lifelong friendships, just one reason why Rice is ranked No. 1 for lots of race/class interaction and No. 1 for quality of life by the Princeton Review. Rice is also rated as a best value among private universities by Kiplinger’s Personal Finance.

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