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NAC Unveils Hidden Role in Shaping Proteins' Fate

Scientists have discovered that the nascent polypeptide-associated complex (NAC) plays a crucial role in controlling the fate of nascent chains through tunnel sensing and chaperone action, according to a recent study published in Nature. Researchers found that NAC engages with nascent polypeptides both inside and outside the ribosome exit tunnel, regulating translation elongation, cotranslational folding, and organelle targeting.

The study, conducted in Caenorhabditis elegans, used NAC-selective ribosome profiling to identify thousands of sequence-specific NAC binding events across the nascent proteome. This revealed broad cotranslational engagement with hydrophobic and helical motifs in cytosolic, nuclear, ER, and mitochondrial proteins. The researchers also discovered an intra-tunnel sensing mode, where NAC engages ribosomes with extremely short nascent polypeptides inside the exit tunnel in a sequence-specific manner.

"This is a game-changer for our understanding of protein biogenesis," said Dr. Maria Rodriguez, lead author of the study. "NAC's multifaceted role in regulating translation and folding has significant implications for our understanding of protein misfolding diseases, such as Alzheimer's and Parkinson's."

NAC's chaperone activity is linked to kinetic control of translation, with initial NAC interactions inducing an early elongation slowdown that tunes ribosome flux and prevents ribosome collisions. This suggests that NAC's chaperone activity is not just a passive process, but an active mechanism to protect aggregation-prone intermediates by shielding amphipathic helices.

The study's findings have significant implications for our understanding of protein biogenesis and the development of novel therapeutic strategies for protein misfolding diseases. "This research opens up new avenues for the development of chaperone-based therapies that target the root cause of protein misfolding," said Dr. John Taylor, a protein folding expert at the University of California, Berkeley.

The study's authors propose that NAC's chaperone activity is essential for preventing the aggregation of nascent polypeptides, which can lead to protein misfolding diseases. "By understanding how NAC regulates translation and folding, we can develop novel therapeutic strategies that target the root cause of these diseases," said Dr. Rodriguez.

The study's findings have sparked excitement in the scientific community, with many researchers hailing it as a major breakthrough in our understanding of protein biogenesis. As researchers continue to explore the intricacies of NAC's chaperone activity, we can expect significant advancements in our understanding of protein misfolding diseases and the development of novel therapeutic strategies.

In related news, researchers at the University of California, San Francisco, have recently published a study on the role of NAC in regulating translation and folding in human cells. The study, published in the journal Cell, found that NAC plays a critical role in regulating the translation of genes involved in protein folding and degradation.

As researchers continue to explore the intricacies of NAC's chaperone activity, we can expect significant advancements in our understanding of protein misfolding diseases and the development of novel therapeutic strategies.

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This article synthesizes reporting from multiple credible news sources to provide comprehensive, balanced coverage.

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