1. HMGA1 drives stem cell, inflammatory pathway, and cell cycle progression genes during lymphoid tumorigenesis
- Author
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C. Conover Talbot, Francescopaolo Di Cello, Jeanne Kowalski, Sandeep N. Shah, Linda M.S. Resar, Amy Belton, Weijie Poh, David L. Huso, Hua Ling Tsai, Tait Huso, and Andrew Schuldenfrei
- Subjects
Leukemia, T-Cell ,lcsh:QH426-470 ,Lymphoid Tissue ,lcsh:Biotechnology ,Mice, Transgenic ,Biology ,medicine.disease_cause ,Chromatin remodeling ,Malignant transformation ,Transcriptome ,Mice ,03 medical and health sciences ,0302 clinical medicine ,lcsh:TP248.13-248.65 ,Genetics ,medicine ,Animals ,Humans ,HMGA1a Protein ,RNA, Neoplasm ,Oligonucleotide Array Sequence Analysis ,030304 developmental biology ,Inflammation ,Regulation of gene expression ,0303 health sciences ,Microarray analysis techniques ,Stem Cells ,Gene Expression Regulation, Neoplastic ,Genes, cdc ,lcsh:Genetics ,Haematopoiesis ,Cell Transformation, Neoplastic ,030220 oncology & carcinogenesis ,Cancer research ,Stem cell ,Carcinogenesis ,Research Article ,Biotechnology - Abstract
Background Although the high mobility group A1 (HMGA1) gene is widely overexpressed in diverse cancers and portends a poor prognosis in some tumors, the molecular mechanisms that mediate its role in transformation have remained elusive. HMGA1 functions as a potent oncogene in cultured cells and induces aggressive lymphoid tumors in transgenic mice. Because HMGA1 chromatin remodeling proteins regulate transcription, HMGA1 is thought to drive malignant transformation by modulating expression of specific genes. Genome-wide studies to define HMGA1 transcriptional networks during tumorigenesis, however, are lacking. To define the HMGA1 transcriptome, we analyzed gene expression profiles in lymphoid cells from HMGA1a transgenic mice at different stages in tumorigenesis. Results RNA from lymphoid samples at 2 months (before tumors develop) and 12 months (after tumors are well-established) was screened for differential expression of > 20,000 unique genes by microarray analysis (Affymetrix) using a parametric and nonparametric approach. Differential expression was confirmed by quantitative RT-PCR in a subset of genes. Differentially expressed genes were analyzed for cellular pathways and functions using Ingenuity Pathway Analysis. Early in tumorigenesis, HMGA1 induced inflammatory pathways with NFkappaB identified as a major node. In established tumors, HMGA1 induced pathways involved in cell cycle progression, cell-mediated immune response, and cancer. At both stages in tumorigenesis, HMGA1 induced pathways involved in cellular development, hematopoiesis, and hematologic development. Gene set enrichment analysis showed that stem cell and immature T cell genes are enriched in the established tumors. To determine if these results are relevant to human tumors, we knocked-down HMGA1 in human T-cell leukemia cells and identified a subset of genes dysregulated in both the transgenic and human lymphoid tumors. Conclusions We found that HMGA1 induces inflammatory pathways early in lymphoid tumorigenesis and pathways involved in stem cells, cell cycle progression, and cancer in established tumors. HMGA1 also dyregulates genes and pathways involved in stem cells, cellular development and hematopoiesis at both early and late stages of tumorigenesis. These results provide insight into HMGA1 function during tumor development and point to cellular pathways that could serve as therapeutic targets in lymphoid and other human cancers with aberrant HMGA1 expression.
- Published
- 2011