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Series GSE130372 Query DataSets for GSE130372
Status Public on Dec 27, 2019
Title Replication timing alterations in leukemia reflect stable clinically-relevant changes in genome architecture [Repli-Chip]
Organism Homo sapiens
Experiment type Other
Third-party reanalysis
Genome variation profiling by genome tiling array
Summary Human B-lineage precursor acute lymphoid leukemias (BCP-ALLs) comprise a group of genetically and clinically distinct disease entities with features of differentiation arrest at known stages of normal B-lineage differentiation. We previously showed BCP-ALL cells display unique and clonally heritable DNA-replication timing (RT) programs; i.e., programs describing the variable order of replication and sub-nuclear 3D architecture of megabase-scale chromosomal units of DNA in different cell types. To determine the extent to which BCP-ALL RT programs mirror or deviate from specific stages of normal human B-cell differentiation, we transplanted immunodeficient mice with quiescent normal human CD34+ cord blood cells and obtained RT signatures of the regenerating B-lineage populations. We then compared these with RT signatures for leukemic cells from a large cohort of BCP-ALL patients of varied genetic subtype and outcome. The results identify BCP-ALL subtype-specific features that resemble specific stages of B-cell differentiation and features that appear associated with relapse. These results suggest the genesis of BCP-ALL involves alterations in RT that reflect biologically significant and clinically relevant leukemia-specific epigenetic changes that have potential as a novel genre of prognostic biomarkers.
 
Overall design Genome-wide replication timing profiles were constructed from leukemia patients cells and normal differentiation stages of B-cell differentiation

Please note that the processed data 'BALLanBlood_Alldata.txt' was generated from both array and HTS data (GSE130372 and GSE130373).
 
Citation(s) 31698451
Submission date Apr 26, 2019
Last update date Dec 27, 2019
Contact name David M Gilbert
Organization name Florida State University
Department Biology
Lab Gilbert
Street address 319 Stadium Drive
City Tallahassee
State/province FL
ZIP/Postal code 32306-4295
Country USA
 
Platforms (3)
GPL14120 NimbleGen Human CGH 385K Whole-Genome Tiling Array [80101_HG18_WG_CGH_v2_X1]
GPL14965 NimbleGen Human 3x720k Whole Genome CGH [100718_HG18_WG_CGH_v3.1_HX3]
GPL18318 NimbleGen Human 6x630K CGH Whole Genome tiling array [100710_HG19_WG_CGH_PERF_UX6]
Samples (63)
GSM3736943 xenograft from bone marrow case 1 passage 1 [Case1P1R1]
GSM3736944 xenograft from bone marrow case 1 passage 1 [Case1P1R2]
GSM3736945 xenograft from bone marrow case 1 passage 1 [Case1P1R3]
This SubSeries is part of SuperSeries:
GSE130374 Replication timing alterations in leukemia reflect stable clinically-relevant changes in genome architecture
Relations
Reanalysis of GSM931321
Reanalysis of GSM931322
Reanalysis of GSM931323
Reanalysis of GSM931324
Reanalysis of GSM931325
Reanalysis of GSM931335
Reanalysis of GSM931327
Reanalysis of GSM931332
Reanalysis of GSM931333
Reanalysis of GSM931334
Reanalysis of GSM931330
Reanalysis of GSM931331
Reanalysis of GSM931329
Reanalysis of GSM931337
Reanalysis of GSM931338
Reanalysis of GSM931339
Reanalysis of GSM931341
Reanalysis of GSM931342
Reanalysis of GSM931343
Reanalysis of GSM931344
Reanalysis of GSM931345
Reanalysis of GSM931346
Reanalysis of GSM931347
Reanalysis of GSM931348
Reanalysis of GSM931349
Reanalysis of GSM931352
Reanalysis of GSM931354
Reanalysis of GSM931355
Reanalysis of GSM931358
Reanalysis of GSM931359
Reanalysis of GSM931360
BioProject PRJNA539935

Download family Format
SOFT formatted family file(s) SOFTHelp
MINiML formatted family file(s) MINiMLHelp
Series Matrix File(s) TXTHelp

Supplementary file Size Download File type/resource
GSE130372_BALLanBlood_Alldata.txt.gz 36.3 Mb (ftp)(http) TXT
GSE130372_RAW.tar 1.7 Gb (http)(custom) TAR (of PAIR)
Processed data are available on Series record

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