(4) The chromosome locations of DEGs.
(5) Functional annotation of DEGs.
(6) Exon expression level analysis.
(7) Identification of novel DE exon-exon junctions.
The key study results:
(1) For the first time the RNA-seq analysis of HBV-related HCC.
(2) 1,378 significantly DEGs and 24, 338 DEEs were identified.
(3) 54 bio-function terms and 41 canonical pathways related to HCC.
(4) Many of chromosomal aberrations were identified, especially 8q24.
(5) Some splicing patterns were identified.
(6) A novel-splicing variant in ATAD2 was identified.
Conclusion:
Overall, by RNA-seq our study represents the most comprehensive
characterization of the HBV-related HCC transcriptome including gene
level expression changes, exon level expression changes and novel splicing
variants, which provided important clues for understanding the molecular
mechanisms of HCC pathogenesis at system-wide levels.
Key words:next-generation sequencing; liver cancer; transcriptome,
Hepatitis B virus; exon
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