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Paternal imprinting of dosage-effect defectivel contributes to seed weight xenia in maize

Agriculture

Paternal imprinting of dosage-effect defectivel contributes to seed weight xenia in maize

D. Dai, J. S. Mudunkothge, et al.

Discover how the paternal regulator *Ded1* in maize influences seed size and development! This groundbreaking research reveals that xenia effects are not just genetic contributions of pollen, but pivotal for grain set and size, as shown by the collaborative work of Dawei Dai, Janaki S. Mudunkothge, and others.

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Playback language: English
Abstract
Historically, xenia effects were hypothesized to be unique genetic contributions of pollen to seed phenotype, but most examples represent standard complementation of Mendelian traits. We identified the imprinted dosage-effect defectivel (*ded1*) locus in maize (*Zea mays*) as a paternal regulator of seed size and development. Hypomorphic alleles show a 5–10% seed weight reduction when *ded1* is transmitted through the male, while homozygous mutants are defective with a 70–90% seed weight reduction. *Ded1* encodes an R2R3-MYB transcription factor expressed specifically during early endosperm development with paternal allele bias. DEDI directly activates early endosperm genes and endosperm adjacent to scutellum cell layer genes, while directly repressing late grain-fill genes. These results demonstrate xenia as originally defined: Imprinting of *Ded1* causes the paternal allele to set the pace of endosperm development thereby influencing grain set and size.
Publisher
Nature Communications
Published On
Sep 13, 2022
Authors
Dawei Dai, Janaki S. Mudunkothge, Mary Galli, Si Nian Char, Ruth Davenport, Xiaojin Zhou, Jeffery L. Gustin, Gertraud Spielbauer, Junya Zhang, W. Brad Barbazuk, Bing Yang, Andrea Gallavotti, A. Mark Settles
Tags
xenia effects
maize
seed size
endosperm development
paternal regulator
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