Pentatricopeptide repeat protein CNS1 regulates maize mitochondrial complex III assembly and seed development

Author:

Ma Shuai1ORCID,Yang Wenzhu1,Liu Xiaoqing1,Li Suzhen1,Li Ye12,Zhu Jiameng3,Zhang Chunyi14ORCID,Lu Xiaoduo5ORCID,Zhou Xiaojin1ORCID,Chen Rumei1ORCID

Affiliation:

1. Crop Functional Genome Research Center, Biotechnology Research Institute, Chinese Academy of Agricultural Sciences , Beijing 100081, China

2. Key Laboratory of Chemical and Biological Processing Technology for Farm Products of Zhejiang Province , Zhejiang University of Science and Technology, Hangzhou 310023, China

3. National Engineering Laboratory of Crop Stress Resistance Breeding, Anhui Agricultural University , Hefei 230036, China

4. Institute of Crop Sciences, Chinese Academy of Agricultural Sciences , Beijing 100081, China

5. Institute of Molecular Breeding for Maize, Qilu Normal University , Jinan 250200, China

Abstract

Abstract Mitochondrial function relies on the assembly of electron transport chain complexes, which requires coordination between proteins encoded by the mitochondrion and those of the nucleus. Here, we cloned a maize (Zea mays) cytochrome c maturation FN stabilizer1 (CNS1) and found it encodes a pentatricopeptide repeat (PPR) protein. Members of the PPR family are widely distributed in plants and are associated with RNA metabolism in organelles. P-type PPR proteins play essential roles in stabilizing the 3′-end of RNA in mitochondria; whether a similar process exists for stabilizing the 5′-terminus of mitochondrial RNA remains unclear. The kernels of cns1 exhibited arrested embryo and endosperm development, whereas neither conventional splicing deficiency nor RNA editing difference in mitochondrial genes was observed. Instead, most of the ccmFN transcripts isolated from cns1 mutant plants were 5′-truncated and therefore lacked the start codon. Biochemical and molecular data demonstrated that CNS1 is a P-type PPR protein encoded by nuclear DNA and that it localizes to the mitochondrion. Also, one binding site of CNS1 located upstream of the start codon in the ccmFN transcript. Moreover, abnormal mitochondrial morphology and dramatic upregulation of alternative oxidase genes were observed in the mutant. Together, these results indicate that CNS1 is essential for reaching a suitable level of intact ccmFN transcripts through binding to the 5′-UTR of the RNAs and maintaining 5′-integrity, which is crucial for sustaining mitochondrial complex III function to ensure mitochondrial biogenesis and seed development in maize.

Funder

National Key Research and Development Program of China

National Special Program for GMO Development of China

National Natural Science Foundation of China

Publisher

Oxford University Press (OUP)

Subject

Plant Science,Genetics,Physiology

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