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Am J Physiol Lung Cell Mol Physiol (April 27, 2007). doi:10.1152/ajplung.00481.2006
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Submitted on December 18, 2006
Accepted on April 25, 2007

Use of Consomic Rats for Genomic Insights into Ventilator-Associated Lung Injury

Stephanie A Nonas1, Liliana Moreno Vinasco2, Shwu F Ma2, Jeffrey R Jacobson2, Ankit Ajit Desai2, Steven Dudek2, Carlos Flores2, Paul M Hassoun1, Lee Sam2, Shui Q Ye2, Jaideep Moitra2, Joe Barnard1, Dmitry N Grigoryev1, Yves A Lussier2, and Joe G.N. Garcia2*

1 Medicine, Johns Hopkins University, Baltimore, Maryland, United States
2 Medicine, University of Chicago, Chicago, Illinois, United States

* To whom correspondence should be addressed. E-mail: jgarcia{at}medicine.bsd.uchicago.edu.

Increasing evidence supports the contribution of genetic influences on susceptibility/severity in acute lung injury (ALI), a devastating syndrome requiring mechanical ventilation with subsequent risk for ventilator-associated lung injury (VALI). To identify VALI candidate genes, we determined that Brown Norway (BN) and Dahl Salt Sensitive (SS) rat strains were differentially sensitive to VALI (tidal volume of 20 ml/kg, 85 breaths/min, 2 hrs) defined by BAL protein and leukocytes. We next exploited differential sensitivities and phenotyped both the VALI-sensitive BN and the VALI-resistant SS rat strains by expression profiling coupled to a bioinformatic-intense candidate gene approach (Significance Analysis of Microarrays). We identified 106 differentially expressed VALI genes representing gene ontologies such as "transcription" and "chemotaxis/cell motility". We mapped the chromosomal location of the differentially expressed probe sets and selected consomic SS rats with single BN introgressions of chromosomes 2, 13, and 16 (based on the highest density of probe sets) while also choosing chromosome 20 (low probe sets density). VALI exposure of consomic rats with introgressions of BN chromosomes 13 and 16 resulted in significant increases in both BAL cells and protein (compared to parental SS strain) while introgression of BN chromosome 2 displayed a large increase only in BAL protein. Introgression of BN chromosome 20 had a minimal effect. These results suggest that genes residing on BN chromosomes 2, 13 and 16 confer increased sensitivity to high tidal volume ventilation. We speculate that the consomic-microarray-SAM approach is a time- and resource-efficient tool for the genetic dissection of complex diseases including VALI.




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