"Correction: Molecular Subsets in the Gene Expression Signatures of Scl" by Ausra Milano, Sarah A. Pendergrass et al.

Dartmouth Scholarship

Title

Correction: Molecular Subsets in the Gene Expression Signatures of Scleroderma Skin

Authors

Ausra Milano, Dartmouth College
Sarah A. Pendergrass, Dartmouth College
Jennifer L. Sargent, Dartmouth College
Lacy K. George, Dartmouth CollegeFollow
Timothy H. McCalmont, University of California, San Francisco
M. Kari Connolly, University of California, San Francisco
Michael L. Whitfield, Dartmouth College

Document Type

Article

Publication Date

7-16-2008

Publication Title

PloS One

Department

Geisel School of Medicine

Abstract

Background: Scleroderma is a clinically heterogeneous disease with a complex phenotype. The disease is characterized by vascular dysfunction, tissue fibrosis, internal organ dysfunction, and immune dysfunction resulting in autoantibody production. Methodology and Findings: We analyzed the genome-wide patterns of gene expression with DNA microarrays in skin biopsies from distinct scleroderma subsets including 17 patients with systemic sclerosis (SSc) with diffuse scleroderma (dSSc), 7 patients with SSc with limited scleroderma (lSSc), 3 patients with morphea, and 6 healthy controls. 61 skin biopsies were analyzed in a total of 75 microarray hybridizations. Analysis by hierarchical clustering demonstrates nearly identical patterns of gene expression in 17 out of 22 of the forearm and back skin pairs of SSc patients. Using this property of the gene expression, we selected a set of ‘intrinsic’ genes and analyzed the inherent data-driven groupings. Distinct patterns of gene expression separate patients with dSSc from those with lSSc and both are easily distinguished from normal controls. Our data show three distinct patient groups among the patients with dSSc and two groups among patients with lSSc. Each group can be distinguished by unique gene expression signatures indicative of proliferating cells, immune infiltrates and a fibrotic program. The intrinsic groups are statistically significant (p , 0.001) and each has been mapped to clinical covariates of modified Rodnan skin score, interstitial lung disease, gastrointestinal involvement, digital ulcers, Raynaud’s phenomenon and disease duration. We report a 177-gene signature that is associated with severity of skin disease in dSSc. Conclusions and Significance: Genome-wide gene expression profiling of skin biopsies demonstrates that the heterogeneity in scleroderma can be measured quantitatively with DNA microarrays. The diversity in gene expression demonstrates multiple distinct gene expression programs in the skin of patients with scleroderma.

DOI

10.1371/annotation/05bed72c-c6f6-4685-a732-02c78e5f66c2

Original Citation

Milano A, Pendergrass SA, Sargent JL, George LK, McCalmont TH, Connolly MK, Whitfield ML. Molecular subsets in the gene expression signatures of scleroderma skin. PLoS One. 2008 Jul 16;3(7):e2696. doi: 10.1371/journal.pone.0002696. Erratum in: PLoS ONE. 2008;3(10). doi: 10.1371/annotation/05bed72c-c6f6-4685-a732-02c78e5f66c2. PMID: 18648520; PMCID: PMC2481301.

Dartmouth Digital Commons Citation

Milano, Ausra; Pendergrass, Sarah A.; Sargent, Jennifer L.; George, Lacy K.; McCalmont, Timothy H.; Connolly, M. Kari; and Whitfield, Michael L., "Correction: Molecular Subsets in the Gene Expression Signatures of Scleroderma Skin" (2008). Dartmouth Scholarship. 2613.
https://digitalcommons.dartmouth.edu/facoa/2613

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