Soybean TILLING-by-Sequencing+ reveals the role of novel GmSACPD members in unsaturated fatty acid biosynthesis while maintaining healthy nodules

A high-resolution target capture technology, TILLING-by-Sequencing+, was developed to functionally characterize GmSACPD family members, finding novel mutations that had a positive impact on soybean stearic acid content. Abstract Developing soybean lines with high levels of stearic acid is a primary...

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Veröffentlicht in:Journal of experimental botany 2020-12, Vol.71 (22), p.6969-6987
Hauptverfasser: Lakhssassi, Naoufal, Zhou, Zhou, Liu, Shiming, Piya, Sarbottam, Cullen, Mallory A, El Baze, Abdelhalim, Knizia, Dounya, Patil, Gunvant B, Badad, Oussama, Embaby, Mohamed G, Meksem, Jonas, Lakhssassi, Aicha, AbuGhazaleh, Amer, Hewezi, Tarek, Meksem, Khalid
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Sprache:eng
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Zusammenfassung:A high-resolution target capture technology, TILLING-by-Sequencing+, was developed to functionally characterize GmSACPD family members, finding novel mutations that had a positive impact on soybean stearic acid content. Abstract Developing soybean lines with high levels of stearic acid is a primary goal of the soybean industry. Most high-stearic-acid soybeans carry different GmSACPD-C mutated alleles. However, due to the dual role of GmSACPD-C in seeds and nodule development, all derived deleterious GmSACPD-C mutant alleles are of extremely poor agronomic value because of defective nodulation. The soybean stearoyl-acyl carrier protein desaturase (GmSACPD) gene family is composed of five members. Comparative genomics analysis indicated that SACPD genes were duplicated and derived from a common ancestor that is still present in chlorophytic algae. Synteny analysis showed the presence of segment duplications between GmSACPD-A/GmSACPD-B, and GmSACPD-C/GmSACPD-D. GmSACPD-E was not contained in any duplicated segment and may be the result of tandem duplication. We developed a TILLING by Target Capture Sequencing (Tilling-by-Sequencing+) technology, a versatile extension of the conventional TILLING by sequencing, and successfully identified 12, 14, and 18 ethyl methanesulfonate mutants at the GmSACPD-A, GmSACPD-B, and GmSACPD-D genes, respectively. Functional analysis of all identified mutants revealed an unprecedented role of GmSACPD-A, GmSACPD-B, and GmSACPD-D in unsaturated fatty acid biosynthesis without affecting nodule development and structure. This discovery will positively impact the development of high-stearic-acid lines to enhance soybean nutritional value without potential developmental tradeoffs.
ISSN:0022-0957
1460-2431
DOI:10.1093/jxb/eraa402