Demonstration of altered fibroblast contractile activity in hypertensive heart disease

doi:10.1016/j.cardiores.2003.09.021

Cardiovascular Research 2003 60(3):547-556; doi:10.1016/j.cardiores.2003.09.021
© 2003 by European Society of Cardiology

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Demonstration of altered fibroblast contractile activity in hypertensive heart disease

William A Marganski^a, Vanessa M De Biase^a, Maria L Burgess^b and Micah Dembo^*^,a

^aDepartment of Biomedical Engineering, Boston University, 44 Cummington Street, Boston, MA 02215, USA
^bDepartment of Health Sciences, Boston University, Boston, MA, USA

*Corresponding author. Tel.: +1-617-353-1671; fax: +1-617-353-6766. Email address: mxd{at}bu.edu

Objective: The aim of this study is to investigate the ideathat altered fibroblast contractile activity is involved inthe pathogenesis of hypertensive heart disease (HHD). Methods:Cell area and contraction are quantified using the tractionforce microscopy technique for cardiac fibroblasts isolatedfrom both normotensive Wistar–Kyoto (WKY) and spontaneouslyhypertensive (SHR) rats. Results: The data indicate that thereare marked phenotypic differences between the two cell types.For instance, WKY fibroblasts exert an average traction stressof $~$ 3.3 kPa and have an area of $~$ 2640 µm². Under identicalconditions the SHR fibroblasts have an area $~$ 1.45 times larger(p<0.01) and exert an average stress $~$ 1.86 times higher (p<0.01).Challenging WKY fibroblasts with 1 µmol/l angiotensinII (Ang II) gradually causes a $~$ 2-fold increase in traction after1 h while simultaneously causing a $~$ 28% decrease in area. Incontrast, Ang II has no effect on SHR fibroblasts. The dataalso show that WKY and SHR cells respond in different ways whenchallenged with irbesartan (Irb). The addition of 1 µmol/lIrb initially causes WKY cells to decrease their average tractionoutput by $~$ 50% after $~$ 10 min. Subsequently, contractile activitybegins to recover and returns to normal after 1 h. The SHR cellsalso decrease their tractions by $~$ 50%, but this decrease requires30 min for completion and there is no recovery to the initialcontractile state. For both cell types, Irb produces no significanteffect on area and the combined effect of equimolar Irb andAng II is the same as Irb alone. Conclusion: These in vitrodata suggest that among the many factors producing hypertensiveheart disease in SHR's are excessive contraction of their cardiacfibroblasts and defective control of fibroblast contractionby Ang II.

KEYWORDS Hypertension; Heart failure; Ventricular function; Angiotensin; Remodeling

Time for primary review 30 days

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