Ontology highlight
ABSTRACT: The NHLBI "Grand Opportunity" Exome Sequencing Project (GO-ESP), a signature project of the NHLBI Recovery Act investment, was designed to identify genetic variants in coding regions (exons) of the human genome (the "exome") that are associated with heart, lung and blood diseases. These and related diseases that are of high impact to public health and individuals from diverse racial and ethnic groups will be studied. These data may help researchers understand the causes of disease, contributing to better ways to prevent, diagnose, and treat diseases, as well as determine whether to tailor prevention and treatments to specific populations. This could lead to more effective treatments and reduce the likelihood of side effects. GO-ESP is comprised of five collaborative components: 3 cohort consortia - HeartGO, LungGO, and WHISP - and 2 sequencing centers - BroadGO and SeattleGO. The Familial Interstitial Pneumonia (FIP) project seeks to identify genetic variants in coding regions of the human genome that are linked to FIP by examining the coding regions among relatives with FIP. These data will be used in conjunction with our other genetic studies to help us better understand how and why some individuals develop pulmonary fibrosis.
OTHER RELATED OMICS DATASETS IN: PRJNA106179
PROVIDER: phs000582.v1.p1 | EGA |
REPOSITORIES: EGA
Yang Ivana V IV Burch Lauranell H LH Steele Mark P MP Savov Jordan D JD Hollingsworth John W JW McElvania-Tekippe Erin E Berman Katherine G KG Speer Marcy C MC Sporn Thomas A TA Brown Kevin K KK Schwarz Marvin I MI Schwartz David A DA
American journal of respiratory and critical care medicine 20060922 1
<h4>Rationale</h4>Idiopathic interstitial pneumonia (IIP) and its familial variants are progressive and largely untreatable disorders with poorly understood molecular mechanisms. Both the genetics and the histologic type of IIP play a role in the etiology and pathogenesis of interstitial lung disease, but transcriptional signatures of these subtypes are unknown.<h4>Objectives</h4>To evaluate gene expression in the lung tissue of patients with usual interstitial pneumonia or nonspecific interstit ...[more]