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通过色素沉着和光合作用的恢复快速且可靠地生产转基因烟草植株。

Rapid and proven production of transplastomic tobacco plants by restoration of pigmentation and photosynthesis.

作者信息

Klaus Sebastian M J, Huang Fong-Chin, Eibl Christian, Koop Hans-Ulrich, Golds Timothy J

机构信息

ICON Genetics AG, Research Centre Freising, Lise-Meitner-Str. 30, 85354 Freising, Germany.

出版信息

Plant J. 2003 Sep;35(6):811-21. doi: 10.1046/j.1365-313x.2003.01838.x.

Abstract

Tobacco chloroplast transformation is typically achieved using dominant, selectable antibiotic resistance genes such as aadA, nptII and aphA-6. An improvement would be the combination of such a marker with a visual screening system for the early and conclusive detection of plastid transformants. As such, we investigated the use of three photosynthesis-deficient plastid mutants, DeltapetA, Deltaycf3 and DeltarpoA, for the development of a phenotypic selection system. Mutant plants were used as an alternative to the wild-type as source tissue for transformation, re-introducing deleted plastid sequences and using the aphA-6 gene as a selection marker. The reconstitution of the deleted genes in transformed regenerants resulted in shoots with a visually distinct phenotype comparable to the wild-type. This transformation/selection system overcomes the common problems associated with plastid transformation, e.g. the recovery of spontaneous mutants or nuclear insertions. In addition to the benefits offered by phenotypic selection, phenotype reconstitution leads to restoration of photosynthesis, which we assume drives reconstituted plants rapidly towards homoplasmy. As such, repeated cycles of regeneration in the presence of an antibiotic selection agent are no longer required.

摘要

烟草叶绿体转化通常使用显性的、可选择的抗生素抗性基因来实现,如aadA、nptII和aphA-6。改进方法是将此类标记与用于早期和确定性检测质体转化体的视觉筛选系统相结合。因此,我们研究了使用三种光合作用缺陷型质体突变体DeltapetA、Deltaycf3和DeltarpoA来开发一种表型选择系统。突变植物被用作替代野生型的转化源组织,重新引入缺失的质体序列,并使用aphA-6基因作为选择标记。转化再生植株中缺失基因的重建导致芽具有与野生型相当的明显视觉表型。这种转化/选择系统克服了与质体转化相关的常见问题,例如自发突变体或核插入的恢复。除了表型选择带来的好处外,表型重建还导致光合作用的恢复,我们认为这会促使重建植株迅速趋向同质性。因此,不再需要在抗生素选择剂存在的情况下进行重复的再生循环。

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