The draft genome of sweet orange (Citrus sinensis)

Qiang Xu,Juan Xu,Niranjan Nagarajan,Xianhong Ge,Chunli Chen,Yijun Ruan,Zhonghui Tang,Dijun Chen,Wenfang Zeng,Denis Bertrand,Shixin Xiao,Manosh Kumar Biswas,Song Gao,Wen-Biao Jiao,Xiaoan Ruan,Yang Lei,Hanhui Kuang,Xiaoming Yang,Qun Hu,Fei Guo,Jiongjiong Chen,Lun Wang,Oscar Junhong Luo,Andan Zhu,Feng Xing,Yin Miao,Guo Wen ,Matthew P Lyon ,Xi Wen Xu ,Ji Wei Chang ,Hong Yu Zhang ,Bao Hai Hao ,Yun Cheng ,Hongrui Cao ,Hong Li ,Jihong Liu ,Mikeal L Roose ,Ling Ling Chen ,X X Deng

doi:10.1038/ng.2472

Abstract

Oranges are an important nutritional source for human health and have immense economic value. Here we present a comprehensive analysis of the draft genome of sweet orange (Citrus sinensis). The assembled sequence covers 87.3% of the estimated orange genome, which is relatively compact, as 20% is composed of repetitive elements. We predicted 29,445 protein-coding genes, half of which are in the heterozygous state. With additional sequencing of two more citrus species and comparative analyses of seven citrus genomes, we present evidence to suggest that sweet orange originated from a backcross hybrid between pummelo and mandarin. Focused analysis on genes involved in vitamin C metabolism showed that GalUR, encoding the rate-limiting enzyme of the galacturonate pathway, is significantly upregulated in orange fruit, and the recent expansion of this gene family may provide a genomic basis. This draft genome represents a valuable resource for understanding and improving many important citrus traits in the future.

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