Pachytene piRNAs instruct massive mRNA elimination during late spermiogenesis

Lan Tao Gou; Peng Dai; Jian Hua Yang; Yuanchao Xue; Yun Ping Hu; Yu Zhou; Jun Yan Kang; Xin Wang; Hairi Li; Min Min Hua; Shuang Zhao; Si Da Hu; Li Gang Wu; Hui Juan Shi; Yong Li; Xiang Dong Fu; Liang Hu Qu; En Duo Wang; Mo Fang Liu

doi:10.1038/cr.2014.41

Pachytene piRNAs instruct massive mRNA elimination during late spermiogenesis

Lan Tao Gou
, Peng Dai
, Jian Hua Yang
, Yuanchao Xue
, Yun Ping Hu
, Yu Zhou
, Jun Yan Kang
, Xin Wang
, Hairi Li
, Min Min Hua
, Shuang Zhao
, Si Da Hu
, Li Gang Wu
, Hui Juan Shi
, Yong Li
, Xiang Dong Fu
, Liang Hu Qu
, En Duo Wang
, Mo Fang Liu

Research output: Contribution to journal › Article › peer-review

341 Scopus citations

Abstract

Spermatogenesis in mammals is characterized by two waves of piRNA expression: one corresponds to classic piRNAs responsible for silencing retrotransponsons and the second wave is predominantly derived from nontransposon intergenic regions in pachytene spermatocytes, but the function of these pachytene piRNAs is largely unknown. Here, we report the involvement of pachytene piRNAs in instructing massive mRNA elimination in mouse elongating spermatids (ES). We demonstrate that a piRNA-induced silencing complex (pi-RISC) containing murine PIWI (MIWI) and deadenylase CAF1 is selectively assembled in ES, which is responsible for inducing mRNA deadenylation and decay via a mechanism that resembles the action of miRNAs in somatic cells. Such a highly orchestrated program appears to take full advantage of the enormous repertoire of diversified targeting capacity of pachytene piRNAs derived from nontransposon intergenic regions. These findings suggest that pachytene piRNAs are responsible for inactivating vast cellular programs in preparation for sperm production from ES.

Original language	English
Pages (from-to)	680-700
Number of pages	21
Journal	Cell Research
Volume	24
Issue number	6
DOIs	https://doi.org/10.1038/cr.2014.41
State	Published - Jun 2014
Externally published	Yes

Keywords

CAF1
ES
MIWI
mRNA deadenylation
pachytene piRNAs
pi-RISC

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10.1038/cr.2014.41

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@article{46b43bc06c4541fca011aad9869d16dc,

title = "Pachytene piRNAs instruct massive mRNA elimination during late spermiogenesis",

abstract = "Spermatogenesis in mammals is characterized by two waves of piRNA expression: one corresponds to classic piRNAs responsible for silencing retrotransponsons and the second wave is predominantly derived from nontransposon intergenic regions in pachytene spermatocytes, but the function of these pachytene piRNAs is largely unknown. Here, we report the involvement of pachytene piRNAs in instructing massive mRNA elimination in mouse elongating spermatids (ES). We demonstrate that a piRNA-induced silencing complex (pi-RISC) containing murine PIWI (MIWI) and deadenylase CAF1 is selectively assembled in ES, which is responsible for inducing mRNA deadenylation and decay via a mechanism that resembles the action of miRNAs in somatic cells. Such a highly orchestrated program appears to take full advantage of the enormous repertoire of diversified targeting capacity of pachytene piRNAs derived from nontransposon intergenic regions. These findings suggest that pachytene piRNAs are responsible for inactivating vast cellular programs in preparation for sperm production from ES.",

keywords = "CAF1, ES, MIWI, mRNA deadenylation, pachytene piRNAs, pi-RISC",

author = "Gou, \{Lan Tao\} and Peng Dai and Yang, \{Jian Hua\} and Yuanchao Xue and Hu, \{Yun Ping\} and Yu Zhou and Kang, \{Jun Yan\} and Xin Wang and Hairi Li and Hua, \{Min Min\} and Shuang Zhao and Hu, \{Si Da\} and Wu, \{Li Gang\} and Shi, \{Hui Juan\} and Yong Li and Fu, \{Xiang Dong\} and Qu, \{Liang Hu\} and Wang, \{En Duo\} and Liu, \{Mo Fang\}",

year = "2014",

month = jun,

doi = "10.1038/cr.2014.41",

language = "英语",

volume = "24",

pages = "680--700",

journal = "Cell Research",

issn = "1001-0602",

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T1 - Pachytene piRNAs instruct massive mRNA elimination during late spermiogenesis

AU - Gou, Lan Tao

AU - Dai, Peng

AU - Yang, Jian Hua

AU - Xue, Yuanchao

AU - Hu, Yun Ping

AU - Zhou, Yu

AU - Kang, Jun Yan

AU - Wang, Xin

AU - Li, Hairi

AU - Hua, Min Min

AU - Zhao, Shuang

AU - Hu, Si Da

AU - Wu, Li Gang

AU - Shi, Hui Juan

AU - Li, Yong

AU - Fu, Xiang Dong

AU - Qu, Liang Hu

AU - Wang, En Duo

AU - Liu, Mo Fang

PY - 2014/6

Y1 - 2014/6

N2 - Spermatogenesis in mammals is characterized by two waves of piRNA expression: one corresponds to classic piRNAs responsible for silencing retrotransponsons and the second wave is predominantly derived from nontransposon intergenic regions in pachytene spermatocytes, but the function of these pachytene piRNAs is largely unknown. Here, we report the involvement of pachytene piRNAs in instructing massive mRNA elimination in mouse elongating spermatids (ES). We demonstrate that a piRNA-induced silencing complex (pi-RISC) containing murine PIWI (MIWI) and deadenylase CAF1 is selectively assembled in ES, which is responsible for inducing mRNA deadenylation and decay via a mechanism that resembles the action of miRNAs in somatic cells. Such a highly orchestrated program appears to take full advantage of the enormous repertoire of diversified targeting capacity of pachytene piRNAs derived from nontransposon intergenic regions. These findings suggest that pachytene piRNAs are responsible for inactivating vast cellular programs in preparation for sperm production from ES.

AB - Spermatogenesis in mammals is characterized by two waves of piRNA expression: one corresponds to classic piRNAs responsible for silencing retrotransponsons and the second wave is predominantly derived from nontransposon intergenic regions in pachytene spermatocytes, but the function of these pachytene piRNAs is largely unknown. Here, we report the involvement of pachytene piRNAs in instructing massive mRNA elimination in mouse elongating spermatids (ES). We demonstrate that a piRNA-induced silencing complex (pi-RISC) containing murine PIWI (MIWI) and deadenylase CAF1 is selectively assembled in ES, which is responsible for inducing mRNA deadenylation and decay via a mechanism that resembles the action of miRNAs in somatic cells. Such a highly orchestrated program appears to take full advantage of the enormous repertoire of diversified targeting capacity of pachytene piRNAs derived from nontransposon intergenic regions. These findings suggest that pachytene piRNAs are responsible for inactivating vast cellular programs in preparation for sperm production from ES.

KW - CAF1

KW - ES

KW - MIWI

KW - mRNA deadenylation

KW - pachytene piRNAs

KW - pi-RISC

UR - https://www.scopus.com/pages/publications/84901826810

U2 - 10.1038/cr.2014.41

DO - 10.1038/cr.2014.41

M3 - 文章

C2 - 24787618

AN - SCOPUS:84901826810

SN - 1001-0602

VL - 24

SP - 680

EP - 700

JO - Cell Research

JF - Cell Research

IS - 6

ER -

Pachytene piRNAs instruct massive mRNA elimination during late spermiogenesis

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Keywords

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