Preprint Article Version 1 This version is not peer-reviewed

Protein-Encoding RNA-to-RNA Information Transfer in Mammalian Cells: Principles of RNA-Dependent mRNA Amplification

Version 1 : Received: 17 February 2019 / Approved: 19 February 2019 / Online: 19 February 2019 (10:39:43 CET)
Version 2 : Received: 27 February 2019 / Approved: 27 February 2019 / Online: 27 February 2019 (08:40:04 CET)
Version 3 : Received: 26 March 2019 / Approved: 26 March 2019 / Online: 26 March 2019 (14:46:54 CET)
Version 4 : Received: 12 June 2019 / Approved: 12 June 2019 / Online: 12 June 2019 (12:21:59 CEST)

How to cite: Volloch, V. Protein-Encoding RNA-to-RNA Information Transfer in Mammalian Cells: Principles of RNA-Dependent mRNA Amplification. Preprints 2019, 2019020172 (doi: 10.20944/preprints201902.0172.v1). Volloch, V. Protein-Encoding RNA-to-RNA Information Transfer in Mammalian Cells: Principles of RNA-Dependent mRNA Amplification. Preprints 2019, 2019020172 (doi: 10.20944/preprints201902.0172.v1).

Abstract

The transfer of protein-encoding genetic information from DNA to RNA to protein, a process formalized as the “Central Dogma of Molecular Biology”, has undergone a significant evolution since its inception. It was amended to account for the information flow from RNA to DNA, the reverse transcription, and for the information transfer from RNA to RNA, the RNA-dependent RNA synthesis. These processes, both potentially leading to protein production, were initially described only in viral systems, and although RNA-dependent RNA polymerase activity was shown to be present, and RNA-dependent RNA synthesis found to occur, in most, if not all, mammalian cells, its function was presumed to be restricted to regulatory. However, recent results, obtained in several systems, strongly indicate the occurrence of protein-encoding RNA to RNA information transfer in mammalian cells. It can result in the rapid production of the extraordinary quantities of specific proteins as was seen in cases of terminal cellular differentiation and during cellular deposition of extracellular matrix molecules. A malfunction of this process may be involved in pathologies associated either with the deficiency of a protein normally produced by this mechanism or with the abnormal abundance of a protein or of its C-terminal fragment. It seems to be responsible for some types of familial thalassemia and may underlie the overproduction of beta amyloid in sporadic Alzheimer’s disease. The potential physiological, therapeutic and bioengineering significance of this process appears to be substantial. The aim of the present article is to systematize the current knowledge and understanding of RNA-dependent amplification of mammalian mRNA. The outlined framework introduces unexpected features of the mRNA amplification such as its second Tier, a physiologically occurring intracellular PCR, iPCR, a “Two-Tier Paradox” and RNA “Dark Matter”. It also describes novel experimental bioengineering designs and may serve as a basis for new directions of investigations into the mechanisms underlying the mammalian mRNA amplification processes.

Subject Areas

RNA-dependent amplification of mammalian mRNA; physiologically occurring intracellular PCR, iPCR; RNA-dependent RNA polymerase, RdRp; chimeric RNA; sense-strand RNA; antisense-strand RNA

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