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Myocyte injury along myofibers in left ventricular remodeling after myocardial infarction

^a Cardiovascular Institute, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, MA, USA
^b Department of Radiology, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, MA, USA

Received 3 March 2009; received in revised form 7 September 2009; accepted 8 September 2009

*Corresponding author. 3 Blackfan Circle, E/CLS#907, Boston, MA 02115, USA. Tel.: +1-617-735-4241; fax: +1-617-735-4207.

E-mail address: tmatsui{at}bidmc.harvard.edu (T. Matsui).

	Abstract

Top Abstract 1. Introduction 2. Materials and methods 3. Results 4. Discussion References

 
Left ventricular (LV) remodeling following myocardial infarction (MI) is considered to contribute to cardiac dysfunction. Though myofiber organization is a key component of cardiac structure, functional and anatomical features of injured myofiber during LV remodeling have not been fully defined. We investigated myocyte injury after acute MI in a mouse model. Mice were subjected to surgical coronary occlusion/reperfusion by left anterior descending coronary artery (LAD) ligation and examined at 1 week and 4 weeks post-MI. Magnetic resonance imaging (MRI) analysis demonstrated a significant decrease in systolic regional wall thickening (WT) in the border and remote zones at 4 weeks post-MI compared to that at 1 week post-MI (–86% in border zone, P<0.05, and –77% in remote zone, P<0.05). Histological assays demonstrated that a broad fibrotic scar extended from the initial infarct zone to the remote zone along mid-circumferential myofibers. Of particular note was the fact that no fibrosis was found in longitudinal myofibers in the epi- and endo-myocardium. This pattern of the scar formation coincided with the helical ventricular myocardial band (HVMB) model, introduced by Torrent-Guasp. MRI analysis demonstrated that the extension of the fibrotic scar along the band might account for the progression in cardiac dysfunction during LV remodeling.

Key Words: Muscle fibers; Ventricular function; Ventricular remodeling; Animals

	1. Introduction

Top Abstract 1. Introduction 2. Materials and methods 3. Results 4. Discussion References

 
Interstitial myocardial fibrosis is an important pathogenic feature of adverse left ventricular (LV) remodeling after myocardial infarction (MI) [1]. Since myocardium architecture, including the geometry of myofibers, accounts for efficient pump function at the global level of the heart [2], distribution of interstitial fibrosis during LV remodeling is a critical factor for prognosis in heart diseases. The helical ventricular myocardial band (HVMB) reported by Torrent-Guasp could explain the myofiber geometry and how its form as a single muscular band relates to cardiac motion [2, 3]. Recent reports, demonstrating the distribution of coronary arteries and pattern of electrophysiological mapping along the muscular band, support the HVMB model's architectural and anatomical conclusions [4, 5]. However, whether the HVMB explains pathophysiological features of LV remodeling after MI has not been explored.

In the present study with a mouse model of MI, we demonstrate that scar formation in the mid-myocardium during LV remodeling is consistent with the HVMB. Magnetic resonance imaging (MRI) analysis shows that a change in regional wall thickness during the cardiac cycle is significantly reduced at the zones possessing mid-myocardial fibrosis. Together, these data imply that the HVMB model accounts for pathological and functional features observed during LV remodeling.

	2. Materials and methods

Top Abstract 1. Introduction 2. Materials and methods 3. Results 4. Discussion References

 
2.1. Animal model of ischemia-reperfusion injury

2.2. MRI

2.3. Histological assays

2.4. Statistical analysis

	3. Results

Top Abstract 1. Introduction 2. Materials and methods 3. Results 4. Discussion References

 
3.1. MRI

View larger version (61K): [in this window] [in a new window]   Fig. 1. MRI analysis. (a) Representative MRI of sham, 1 week post-MI (week 1) and 4 weeks post-MI (week 4) mice in full diastolic (Diastole) and full systolic (Systole) phases at the mid-ventricular level. Images are representative from three sham-operated, three week 1 and six week 4 mice. (b) Measured points for wall thickness of MRI images. Front of anterior papillary muscle (Initial infarct zone), between papillary muscles (Border zone), and posterior side of posterior papillary muscle (Remote zone). (c) Systolic wall thickening. The percentage of systolic wall thickening of sham-operated (n=3), week 1 (n=3) and week 4 (n=6) mice was measured as described in the materials and methods. Data are mean±S.E.M.

View larger version (14K): [in this window] [in a new window]   Fig. 2. The ischemic are (area-at-risk). Images of fluorescent microspheres are representative from week 1 and week 4 mice (Upper). The percent of the area-at-risk of week 1 (n=3) and week 4 (n=10) mice was measured as previously described [6] (Lower). Data are mean±S.E.M.

View larger version (45K): [in this window] [in a new window]   Fig. 3. Histological assays. (a) Representative sections of Masson's trichrome staining at week 1 and week 4. Serial cross sections were acquired from basal (Base), mid-ventricular (Mid-vent.) and apical (Apex) slice positions. (b) The percent (left) and width (right) of scar fibrosis at week 1 (black) and week 4 (white). The percent thickness of scar fibrosis was measured by the ratio to total wall thickness at the same position. Week 1 mice, n=4 and week 4 mice, n=5. Data are mean±S.E.M. (c) High magnification view of Masson's trichrome and anti-dystrophin staining. The areas indicated with a square in (a) are shown. (d) Representative nuclear staining. Cross sections from hearts of sham-operated and post-MI (week 1) mice were stained with DAPI. endo., endomyocardium; mid., mid-myocardium; epi., epimyocardium.

	4. Discussion

Top Abstract 1. Introduction 2. Materials and methods 3. Results 4. Discussion References

In post-MI patients, scarring along the mid-myocardium (called the subendocardium) has frequently been demonstrated in previous reports using a variety of examinations. Gadolinium-contrast MRI demonstrates MI scar as a late enhancement in the subendocardial layer [7]. However, further examinations of anatomical structure with mid-myocardial scar in post-MI have not been discussed. In the border and remote zones of post-MI hearts, we have observed scar extension specifically along myofibers in the mid-myocardium but not along any myofibers of either the epi- or endo-myocardium. Coronary vessels cross the whole LV wall from the epicardium to the endocardium. According to the anatomical distribution, in clinical diagnosis, the assignment of myocardial segments supplied by the three major coronary arteries are delineated with transmural lines [8]. Although total coronary ligation models (no reperfusion) in mice demonstrated transmural injury that is depicted with a radial line, ischemia-reperfusion injury has always induced myocardial injury in the mid-circumferential myofibers dominantly with survived cardiomyocytes in both the epi- and endo-myocardium. Blood flow only through transmural vessels cannot account for the injury pattern because the pressure dependent blood flow in myocardium cannot make a clear marginal line that we and other groups [9] have seen in ischemia-reperfusion injury. In addition to the scar formation, we and other groups [10] have observed that inflammatory cells were accumulated dominantly in the mid-myocardium with a clear margin. The consistent injury pattern observed in the mid-myocardium suggests that some part of the blood supply to the mid-myocardium flows along circumferential myofibers rather than along radial vessels across the myocardium. The HVMB introduced by Torrent-Guasp describes myocardial architecture in the form of a single muscular band that is spatially organized into two distinct helicoids [11]. In the HVMB concept, the LV free wall consists of three layers at the mid-ventricular level [11]. The distribution of scar in the mid-circumferential myofibers that we saw in this study appears to support aspects of the HVMB concept [11]. Recent reports demonstrated that the distribution of coronary arteries and pattern of electrophysiological mapping are observed along the HVMB [4, 5]. Taking everything together, we hypothesize that some of the coronary vessels may progress along the myocardial band in addition to transmural vessels and that tissue fibrosis during LV remodeling would extend along the coronary vessels in accord with the HVMB. In fact, recent reports have frequently discussed the fact that late enhancement of the subendocardium in gadolinium-contrast MRI is a critical indicator for subsequent heart failure [12].

Ventricular WT during systole is an essential mechanism for generating pump function within the myocardium [2]. The percent of regional WT indicated by MRI is a good indicator of regional myocardium function and often is utilized for studies of post-MI LV remodeling in patients [13] and animal models, including mice [14]. In the current study, MRI showed a significant decline in %WT in the border and remote zones at four weeks post-MI. These zones corresponded to the areas where we have seen mid-circumferential scar. In post-MI patients, there is a significant correlation between late enhanced myocardium in gadolinium-contrast MRI and WT [13], suggesting that extension of scar area in myocardium is a critical predictor for adverse LV remodeling in the chronic phase. While considerably more samples will be necessary for complete analysis of LV remodeling, we hypothesize a mechanism for the preservation of %WT in the early stage of LV remodeling (1 week post-MI). Consistent with the prior report [10], we observed a decrease on thickness of fibrotic scar in the mid-myocardium during progression of LV remodeling. As previously reported, systolic slippage of laminar sheets in the myocardium is a critical factor for generating WT [15]. Even if the mid-circumferential myofibers are dysfunctional or injured, slippage of the laminar sheet may generate enough of a longitudinal gap between the epi- and endo-myocardial surfaces during a stroke, as long as the width of the laminar sheet is kept at the same range to normal, that the rest of the myocardium (the epi- and endo-myocardium) is still functional. Although the injury pattern is a feasible mechanism for the adaptive reaction in early LV remodeling, further experiments will be necessary to address the issue.

In conclusion, the HMVB concept accounts for the localization of fibrotic scar formation that we observed in LV remodeling following acute MI. Understanding the consistent pattern of the scar formation following acute-MI may have important implications not only for cardiac exams such as MRI and echocardiography but also for interventional therapies such as surgery and cell therapy.

	References

Top Abstract 1. Introduction 2. Materials and methods 3. Results 4. Discussion References

 

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