Virus Dataset Sample Info

> Dataset: 22634756 Search Result


Summary
Item Summary
Project 22634756
Virus Name HBV
Sample Number 25
Disease Hepatocellular carcinoma (HCC)
Country United States
Data Link https://www.ncbi.nlm.nih.gov/geo/query/acc.cgi?acc=GSE36390

Sample
ID Sample ID Age Gender Origin Detail
1 HB1 56 M United States View
2 HB2 46 M United States View
3 HB3 74 M United States View
4 HB4 61 M United States View
5 HB5 38 M United States View
6 HB6 57 M United States View
7 HB7 58 M United States View
8 HB8 68 F United States View
9 HB9 60 M United States View
10 HB10 56 M United States View
11 HB11 41 F United States View
12 HC1 62 M United States View
13 HC2 71 M United States View
14 HC3 69 M United States View
15 HC3 69 M United States View
16 HC4 61 M United States View
17 HC5 58 M United States View
18 HC6 61 M United States View
19 HC7 64 M United States View
20 HC7 64 M United States View
21 HC8 73 F United States View
22 HC9 66 M United States View
23 HC10 62 F United States View
24 HC11 71 F United States View
25 HC12 57 M United States View
26 NBNC1 81 F United States View
27 NBNC2 73 M United States View

Literature
Item Summary
PMID 22634756
Title Whole-genome Sequencing of Liver Cancers Identifies Etiological Influences on Mutation Patterns and Recurrent Mutations in Chromatin Regulators
Abstract Hepatocellular carcinoma (HCC) is the third leading cause of cancer-related death worldwide. We sequenced and analyzed the whole genomes of 27 HCCs, 25 of which were associated with hepatitis B or C virus infections, including two sets of multicentric tumors. Although no common somatic mutations were identified in the multicentric tumor pairs, their whole-genome substitution patterns were similar, suggesting that these tumors developed from independent mutations, although their shared etiological backgrounds may have strongly influenced their somatic mutation patterns. Statistical and functional analyses yielded a list of recurrently mutated genes. Multiple chromatin regulators, including ARID1A, ARID1B, ARID2, MLL and MLL3, were mutated in _50% of the tumors. Hepatitis B virus genome integration in the TERT locus was frequently observed in a high clonal proportion. Our whole-genome sequencing analysis of HCCs identified the influence of etiological background on somatic mutation patterns and subsequent carcinogenesis, as well as recurrent mutations in chromatin regulators in HCCs.