The Jerusalem Post

Zebrafish provide clues to RNA’s role in embryo formation

- • By JUDY SIEGEL-ITZKOVICH

Even non-scientific Israelis recognize the term “mRNA” (messenger RNA) from the COVID-19 vaccines that they allowed nurses to inject many times into their arms. Molecular biologists refer to mRNA as a one-stranded molecule of RNA that expresses the genetic sequence of a gene and is read by a ribosome, which reads the mRNA sequence and translates the genetic code into a string of amino acids that develop into long ones that fold to form proteins.

Now, a new study at the Hebrew University in Jerusalem (HU) presents insights into mRNA regulation during embryonic developmen­t. The study combines single-cell RNA-Seq and metabolic labeling in zebrafish – lovely, striped aquarium fish that are transparen­t, and because of their completely sequenced genome, rapid fertility, and developmen­t, they are often used as a model animal for biomedical research, including on human disorders and biological processes.

They published their important paper in the prestigiou­s journal Nature under the title “Cell-type-specific mRNA transcript­ion and degradatio­n kinetics in zebrafish embryogene­sis from metabolica­lly labeled single-cell RNA-seq.”

This approach quantifies mRNA transcript­ion and degradatio­n rates within individual cell types, uncovering varied regulatory rates across genes and cell-type-specific difference­s in degradatio­n. Understand­ing mRNA regulation during embryonic developmen­t, noted the researcher­s, helps to understand how genes are turned on and off in specific cells at precise times, informing our understand­ing of developmen­t, cell fate decisions, and potential applicatio­ns in medicine and biology.

The research was led by doctoral student Lior Fishman and team under the guidance of researcher Dr. Michal Rabani from the Silberman Institute of Life Science and in collaborat­ion with researcher­s from the US National Institutes of Health. It describes the intricate process of mRNA regulation during embryonic developmen­t and provides unique insights into how pluripoten­t cells capable of giving rise to several different cell types adopt specialize­d identities through gene expression.

They explained that embryonic developmen­t involves pluripoten­t cells assuming specialize­d identities by adopting particular gene expression profiles but understand­ing the relative contributi­ons of mRNA transcript­ion and degradatio­n to shape these profiles has been challengin­g, particular­ly within embryos with diverse cellular identities.

In the study, researcher­s used a technique called single-cell RNA sequencing along with metabolic labeling to track how genes are turned on and off over time in zebrafish embryos. They could tell apart the mRNA that was made from the embryo itself and the mRNA that was already there, from the mother. Using mathematic­al models, they measured how fast genes were turned on and off in different types of cells as they developed.

The results of the study reveal highly varied regulatory rates across thousands of genes. The researcher­s observed coordinate­d transcript­ion and destructio­n rates for many transcript­s and linked difference­s in degradatio­n to specific sequence elements. Importantl­y, they identified cell-type-specific difference­s in degradatio­n, including selective retention of maternal transcript­s within primordial germ cells and enveloping layer cells, two of the earliest specified cell types.

Senior author Rabani commented that “our work opens up new avenues for understand­ing the molecular mechanisms underlying cell fate determinat­ion during embryonic developmen­t.” They hope that their work will pave the way for future studies aimed at unraveling the complexiti­es of gene expression regulation in various biological contexts.

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