Cis to trans: small ORF functions emerging through evolution.

IF 13.6 2区生物学 Q1 GENETICS & HEREDITY

Trends in Genetics Pub Date : 2024-11-26 DOI:10.1016/j.tig.2024.10.012

Casimiro Baena-Angulo, Ana Isabel Platero, Juan Pablo Couso

引用次数: 0

Abstract

Hundreds of thousands of small open reading frames (smORFs) of less than 100 codons exist in every genome, especially in long noncoding RNAs (lncRNAs) and in the 5' leaders of mRNAs. smORFs are often discarded as nonfunctional, but ribosomal profiling (RiboSeq) reveals that thousands are translated, while characterised smORF functions have risen from anecdotal to identifiable trends: smORFs can either have a cis-noncoding regulatory function (involving low translation of nonfunctional peptides) or full coding function mediated by robustly translated peptides, often having cellular and physiological roles as membrane-associated regulators of canonical proteins. The evolutionary context reveals that many smORFs represent new genes emerging de novo from noncoding sequences. We suggest a mechanism for this process, where cis-noncoding smORF functions provide niches for the subsequent evolution of full peptide functions.

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从顺式到反式：进化过程中出现的小型 ORF 功能。

每个基因组中，尤其是在长非编码 RNA（lncRNA）和 mRNA 的 5' 首部中，都存在成千上万个密码子少于 100 个的小型开放阅读框（smORF）。smORF 通常被认为是无功能的，但核糖体图谱分析（RiboSeq）显示，成千上万的 smORF 被翻译，而 smORF 的功能特征已从传闻上升为可识别的趋势：smORF 既可以具有顺式非编码调控功能（涉及无功能肽的低翻译），也可以通过强翻译肽介导的完全编码功能，通常作为典型蛋白的膜相关调控因子发挥细胞和生理作用。进化背景显示，许多 smORF 代表了从非编码序列中新出现的新基因。我们为这一过程提出了一种机制，即顺式非编码 smORF 功能为随后完整多肽功能的进化提供了龛位。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Trends in Genetics 生物-遗传学

CiteScore

20.90

自引率

0.90%

发文量

160

审稿时长

6-12 weeks

期刊介绍： Launched in 1985, Trends in Genetics swiftly established itself as a "must-read" for geneticists, offering concise, accessible articles covering a spectrum of topics from developmental biology to evolution. This reputation endures, making TiG a cherished resource in the genetic research community. While evolving with the field, the journal now embraces new areas like genomics, epigenetics, and computational genetics, alongside its continued coverage of traditional subjects such as transcriptional regulation, population genetics, and chromosome biology. Despite expanding its scope, the core objective of TiG remains steadfast: to furnish researchers and students with high-quality, innovative reviews, commentaries, and discussions, fostering an appreciation for advances in genetic research. Each issue of TiG presents lively and up-to-date Reviews and Opinions, alongside shorter articles like Science & Society and Spotlight pieces. Invited from leading researchers, Reviews objectively chronicle recent developments, Opinions provide a forum for debate and hypothesis, and shorter articles explore the intersection of genetics with science and policy, as well as emerging ideas in the field. All articles undergo rigorous peer-review.