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Terminal modification, sequence, length, and PIWI-protein identity determine piRNA stability.


ABSTRACT: In animals, PIWI-interacting RNAs (piRNAs) silence transposons, fight viral infections, and regulate gene expression. piRNA biogenesis concludes with 3' terminal trimming and 2'-O-methylation. Both trimming and methylation influence piRNA stability. Our biochemical data show that multiple mechanisms destabilize unmethylated mouse piRNAs, depending on whether the piRNA 5' or 3' sequence is complementary to a trigger RNA. Unlike target-directed degradation of microRNAs, complementarity-dependent destabilization of piRNAs in mice and flies is blocked by 3' terminal 2'-O-methylation and does not require base pairing to both the piRNA seed and the 3' sequence. In flies, 2'-O-methylation also protects small interfering RNAs (siRNAs) from complementarity-dependent destruction. By contrast, pre-piRNA trimming protects mouse piRNAs from a degradation pathway unaffected by trigger complementarity. In testis lysate and in vivo, internal or 3' terminal uridine- or guanine-rich tracts accelerate pre-piRNA decay. Loss of both trimming and 2'-O-methylation causes the mouse piRNA pathway to collapse, demonstrating that these modifications collaborate to stabilize piRNAs.

SUBMITTER: Gainetdinov I 

PROVIDER: S-EPMC8642287 | biostudies-literature | 2021 Dec

REPOSITORIES: biostudies-literature

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Terminal modification, sequence, length, and PIWI-protein identity determine piRNA stability.

Gainetdinov Ildar I   Colpan Cansu C   Cecchini Katharine K   Arif Amena A   Jouravleva Karina K   Albosta Paul P   Vega-Badillo Joel J   Lee Yongjin Y   Özata Deniz M DM   Zamore Phillip D PD  

Molecular cell 20211008 23


In animals, PIWI-interacting RNAs (piRNAs) silence transposons, fight viral infections, and regulate gene expression. piRNA biogenesis concludes with 3' terminal trimming and 2'-O-methylation. Both trimming and methylation influence piRNA stability. Our biochemical data show that multiple mechanisms destabilize unmethylated mouse piRNAs, depending on whether the piRNA 5' or 3' sequence is complementary to a trigger RNA. Unlike target-directed degradation of microRNAs, complementarity-dependent d  ...[more]

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