8.3: Стабильность РНК

RNA Stability
JoVE Core
Molecular Biology
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JoVE Core Molecular Biology
RNA Stability

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01:53 min
November 23, 2020

Overview

Intact DNA strands can be found in fossils, while scientists sometimes struggle to keep RNA intact under laboratory conditions. The structural variations between RNA and DNA underlie the differences in their stability and longevity. Because DNA is double-stranded, it is inherently more stable. The single-stranded structure of RNA is less stable but also more flexible and can form weak internal bonds. Additionally, most RNAs in the cell are relatively short, while DNA can be up to 250 million nucleotides long. RNA has a hydroxyl group on the second carbon of the ribose sugar, increasing the likelihood of breakage of the sugar-phosphate backbone.

The cell can exploit the instability of RNA, regulating both its longevity and availability. More stable mRNAs will be available for translation for a longer period of time than less stable mRNAs transcripts. RNA binding proteins (RBPs) in cells play a key role in the regulation of RNA stability. RBPs can bind to a specific sequence (AUUUA) in the 3’ untranslated region (UTR) of mRNAs. Interestingly, the number of AUUUA repeats appears to recruit RBPs in a specific way: fewer repeats recruit stabilizing RBPs. Several, overlapping repeats result in the binding of destabilizing RBPs. All cells have enzymes called RNases that break down RNAs. Typically, the 5’cap and polyA tail protect eukaryotic mRNA from degradation until the cell no longer needs the transcript.

The emerging research on epitranscriptomics aims to define regulatory mRNA modifications. Recently, scientists have discovered an important role for methylation in mRNA stability. The methylation of adenosine residues (m6A) appears to increase mRNA translation and degradation. m6A also has roles in stress responses, nuclear export, and mRNA maturation. The presence of a modified uracil residue, pseudouridine, also appears to play an important role in RNA regulation.

Transcript

RNA is a mobile, relatively short-lived molecule that is much less structurally and chemically stable compared to DNA. In RNA, the five-carbon sugar ribose has a hydroxyl group at the second carbon, while deoxyribose has a single hydrogen. The hydrogen of the hydroxyl group is susceptible to being removed in basic solutions. When this occurs, the negatively charged oxygen that remains is capable of breaking the phosphate sugar backbone.

In addition, RNA is usually single stranded, making it less structurally stable than the double helix of DNA. RNA molecules are also much shorter than DNA molecules, so they're more vulnerable to degradation at their ends. External factors can also influence the stability of RNA. For example, specific exonucleases in the cytoplasm called RNases break down RNAs that are not actively being translated. Other proteins, known as RNA-binding proteins effect stability by recognizing and binding to specific RNA nucleotide sequences.

mRNA transcripts with AU-rich elements, usually repeats of AUUUA, in their three-prime untranslated regions, or three-prime UTRs, attract different classes of RNA-binding proteins with opposing roles. Some of these proteins enhance mRNA stability and increase protein translation while bounded to the three-prime UTR, while others destabilize the transcript so that it is degraded more quickly. Thus, the amount of time that an RNA molecule is available for translation is variable and dependent on multiple factors.

Key Terms and definitions​

  • RNA Stability – The capacity of an RNA molecule to withstand degradation.
  • DNA Stability – Relates to DNA's resilience and persistency over time.
  • Ribose Sugar – The sugar component in the backbone of RNA molecules.
  • RNA Binding Proteins – Proteins that interact with RNA influencing RNA functions and stability.
  • RNA Degradation – Breakdown of RNA molecules by cellular machinery.

Learning Objectives

  • Define RNA stability - Explain what this means in molecular biology (e.g., RNA Stability).
  • Contrast RNA Stability vs DNA Stability - Explain key differences (e.g., Degradation rates).
  • Explore examples of RNA Binding Proteins - Describe role in RNA lifespan (e.g., RNA protein interaction).
  • Explain the role of Special RNA structures - uncover how specific sequences affect stability.
  • Apply the concept of RNA degradation - Understanding in cellular processes and genetic expression.

Questions that this video will help you answer

  • What is RNA stability and how it affects the fate of mRNA transcripts?
  • How does DNA stability differ from that of RNA?
  • How do RNA Binding Proteins affect RNA stability and degradation?

This video is also useful for

  • Biotechnology Students – Understands RNA Stability for better genetic expression studies.
  • Biology Educators – Provides a clear concept of RNA degradation for teaching molecular biology.
  • Genetics Researchers – Relevance for studying gene expression and regulation.
  • Science Enthusiasts – Offers insights into RNA lifespan and its broad cellular functions.

Tags

Стабильность РНК является важнейшим аспектом в молекулярной биологии и генетике. Это относится к способности молекулы РНК противостоять деградации или распаду в клеточной среде. Понимание стабильности РНК имеет важное значение для изучения экспрессии генов регуляторных механизмов и различных клеточных процессов. Несколько факторов способствуют стабильности РНК в том числе последовательность и структура самой молекулы РНК а также взаимодействие с белками и другими молекулами. Стабильность РНК может сильно варьироваться между различными транскриптами некоторые из них очень стабильны а другие более подвержены деградации. Стабильность РНК регулируется с помощью сложной сети механизмов. Один из таких механизмов включает в себя добавление защитной структуры колпачка на 5'-конце молекулы РНК известной как 5'-колпачок. Этот колпачок помогает предотвратить деградацию экзонуклеазами ферментами которые разрушают РНК с концов. Другой важный механизм включает в себя добавление поли(А)-хвоста на 3'-конце РНК М