Myocardial Interstitial Matrix Metalloproteinase Activity Is Altered by Mechanical Changes in LV Load: Interaction With the Angiotensin Type 1 Receptor

doi:10.1161/01.RES.0000167830.12010.6b

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Circulation Research. 2005;96:1110-1118
Published online before print April 28, 2005, doi: 10.1161/01.RES.0000167830.12010.6b

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(Circulation Research. 2005;96:1110.)
© 2005 American Heart Association, Inc.

Integrative Physiology

Myocardial Interstitial Matrix Metalloproteinase Activity Is Altered by Mechanical Changes in LV Load

Interaction With the Angiotensin Type 1 Receptor

Anne M. Deschamps^*, Kimberly A. Apple^*, Amy H. Leonardi, Julie E. McLean, William M. Yarbrough, Robert E. Stroud, Leslie L. Clark, Jeffrey A. Sample, Francis G. Spinale

From the Division of Cardiothoracic Surgery (A.M.D., K.A.A., A.H.L., J.E.M., W.M.Y., R.E.S., J.A.S., F.G.S.), Department of Biostatistics, Bioinformatics and Epidemiology (L.L.C.), Medical University of South Carolina, Charleston, SC, The Ralph H. Johnson Veteran’s Affairs Medical Center

Correspondence to Dr Francis G. Spinale, Cardiothoracic Surgery, Strom Thurmond Research Building, 114 Doughty Street, Room 625, Medical University of South Carolina, Charleston, SC 29403.

LV myocardial remodeling is a structural hallmark of hypertensivehypertrophy, but molecular mechanisms driving this process arenot well understood. The matrix metalloproteinases (MMPs) cancause myocardial remodeling in chronic disease states, but howMMP activity is altered with a mechanical load remains unknown.The present study quantified interstitial MMP activity aftera discrete increase in LV load and dissected out the contributoryrole of the angiotensin II Type 1 receptor (AT₁R). Pigs (38kg)were randomized to undergo (1) increased LV load by insertionof an intra-aortic balloon pump (IABP) triggered at systolefor 3 hours, then deactivated (n=11); (2) IABP and AT₁R blockade(AT₁RB; valsartan, 3 ng/kg/hr; n=6). MMP activity was directlymeasured in the myocardial interstitium using a validated inlinedigital fluorogenic microdialysis system. IABP engagement increasedLV peak pressure from 92±3 to 113±5 and 123±7mm Hg in the vehicle and AR₁RB group, respectively, and remainedelevated throughout the IABP period (P<0.05). With IABP disengagement,segmental shortening (% change from baseline of 0) remaineddepressed in the vehicle group (-32.2±11.8%, P<0.05)but returned to baseline in the AT₁RB group (2.3±12.5%).MMP activity decreased with IABP in both groups. At IABP disengagement,a surge in MMP activity occurred in the vehicle group that wasabrogated with AT₁RB (3.03±0.85 versus 0.07±1.55MMP units/hr, P<0.05). A transient increase in LV load causeda cyclic variation in interstitial MMP activity that is regulatedin part by the AT₁R. These temporally dynamic changes in MMPactivity likely influence myocardial function and structurewith increased LV load.

Key Words: matrix metalloproteinase • extracellular matrix • angiotensin II type I receptor

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