Notch signaling is activated in cardiac myocytes and nonmyocyte cells in the adult heart. (A) Quantitative real-time RT-PCR analysis of gene expression showing the up-regulation of Notch1, Jagged1, and Hes1 in hypertrophic (H) and dilated (D) hearts of TG1306/1R transgenic mice relative to hearts of WT mice. The relative expression levels of BNP and α-skeletal actin are also shown. Asterisks denote significant difference between the groups (P < 0.05). n = 6 per group. Error bars show the mean ± SD. (B) Confocal immunofluorescence analysis of activated Notch1 in adult mouse myocardium. Tissue sections were stained with an antibody directed against the intracellular domain of proteolytically cleaved Notch1 (N1IC). Cardiomyocytes were revealed using anti–α-actinin antibody. Laminin immunostaining was used to delimit cell boundaries, and nuclei were stained with DAPI. Closed and open arrows indicate cardiomyocytes and CPCs, respectively. Bars, 10 μm.

Inhibition of Notch signaling exacerbates cardiac hypertrophy. (A) Quantitative real time RT-PCR analysis of expression of Notch1, Jagged1, and Notch target genes Hes1, Hey1, and Hey2 in the hearts of WT and TG13061/R transgenic mice treated with the γ-secretase inhibitor Ly411,575 relative to their vehicle-treated counterparts. (B) Quantitative RT-PCR analysis of expression of markers of cardiac hypertrophy and failure in the hearts of WT and transgenic mice, treated as in A, relative to vehicle-treated mice. (C) Representative transverse histological sections showing exacerbated hypertrophy in hearts from TG1306/1R transgenic mice treated with the γ-secretase inhibitor Ly411,575 compared with control mice. (D) The heart weight/body weight ratio (cardiac weight index [CWI]) of vehicle- and γ-secretase inhibitor–treated transgenic and WT mice is represented. Asterisks denote significant difference between the groups (P < 0.05). n = 6–8 mice per group. Error bars show the mean ± SD. Bar, 2 mm.

Notch1 controls the adaptive cardiac response to stress. (A) Quantitation of Notch1 activation in the adult stressed heart. Heart tissue sections from clipped (1K1C) and sham-operated (sham) mice were stained with an antibody against proteolytically activated N1IC at 8 and 20 d after clipping. The N1IC-positive nuclei were counted in representative sections and represented as percentage of total nuclei. n = 5–8 areas per section and 3 mice per group. (B and C) Quantitative RT-PCR analysis of the expression of cardiac marker genes in sham and 1K1C mice. N1^Del, mice lacking Notch1 in the heart. n = 5–7 mice per group. Error bars show the mean ± SD. (D) Development of cardiac fibrosis in mice lacking Notch1 in the heart. Heart tissue sections from sham and clipped WT and N1^Del mice were subjected to van Gieson staining to reveal fibrosis (red). (E) Mortality rate in clipped and sham-operated WT mice and mice lacking Notch1 in the heart (N1^Del). n = 20–25 mice per group. Asterisks in A, B, and C denote significant difference (P < 0.01). Bar, 2 mm.

Increased apoptosis in the heart tissue of clipped N1^Del mice. (A) Heart tissue sections were processed for detection of apoptotic nuclei using TUNEL assay and for detection of cardiac myocytes using anti-myomesin antibody. Representative photomicrographs of TUNEL-positive nuclei in α-actinin–positive cardiomyocytes and in nonmyocyte cells are shown. (B) Quantitative analysis of apoptosis in the hearts of clipped mice. Heart tissue sections cut at anatomically equivalent locations were stained as in A. The total number of TUNEL-positive nuclei per section was counted under a fluorescence microscope. The bar graph represents the mean number of nuclei in sham operated (n = 4) and clipped (n = 4) WT mice and sham (n = 3) and clipped (n = 5) N1^Del mice. The asterisk denotes significant difference (P < 0.05) between clipped WT and N1^Del mice. Error bars show the mean ± SD. Bar, 20 μm.

Notch1 activation controls maturation and cardiac gene expression in cardiomyocytes. (A) Analysis of Notch1 activation in cultured cardiomyocytes isolated from neonatal mice carrying floxed Notch1 allele (Notch1^lox/lox) without (Cre⁻) or with (Cre⁺) Cre recombinase expression under the control of the MLC2v promoter. The cultures were stained for activated Notch1 (N1IC) and myomesin. The Cre⁻ (WT) cardiomyocytes demonstrate either high (N1IC^hi) or low (N1IC^low) N1IC staining concomitant with poor or elaborate myofibrillar structure, respectively. (B) Quantitative RT-PCR analysis demonstrating the up-regulation of cardiac-specific gene expression in cultures of Cre⁺ (Notch1 deleted) cardiac myocytes relative to Cre⁻ myocyte cultures. Error bars represent the means ± SD. Bar, 20 μm.

Notch1 activation in proliferating undifferentiated cardiac-committed cells in the adult myocardium. (A) Confocal microscopy of normal heart tissue sections showing activation of Notch1 (N1IC) in GATA4-positive α-actinin–negative cells. Nuclei are stained with DAPI. (B) Staining of cardiac tissue sections, as in A, showing N1IC staining in Nkx2.5-positive nuclei of undifferentiated α-actinin–negative cells. (C) Activation of Notch1 (N1IC) in proliferating Ki67-positive α-actinin–negative cells. (D) Analysis of BrdU incorporation in hearts of clipped (1K1C) and sham-operated (sham) WT mice and mice lacking Notch1 in the heart (N1^del). Tissue sections of hearts from mice administered with BrdU for 96 h in drinking water were stained with anti-BrdU antibody. The BrdU⁺ nuclei are red. (E) Quantitation of BrdU incorporation represented as percentage of BrdU⁺ nuclei. * and † denote significance at P < 0.01 within groups and between groups, respectively. Error bars show the mean ± SD. Bars: (A, B, and C) 10 μm; (D) 100 μm.

Notch signaling controls differentiation of CPCs into mature cardiomyocytes. (A) Analysis of Notch1 activation in growing and differentiating cardiac-committed nonmyocyte cells in vitro. Cultures of nonmyocyte cells isolated from neonatal hearts were maintained in expansion conditions and stained for activated Notch1 (N1IC, green) and Nkx2.5 (red). The cultures were shifted to differentiation conditions and stained either for N1IC (green) and Nkx2.5 (red) in the middle column or for N1IC (green) and α-actinin (red) in the right column. Arrows indicate cardiac-committed or differentiated cardiomyocyte nuclei lacking N1IC staining. (B) Quantitative RT-PCR analysis of expression of markers of cardiac differentiation. Nonmyocyte cells were maintained in differentiation medium or control medium and analyzed by quantitative RT-PCR for the expression of the indicated genes. Down-regulation of Jagged1 and Hes1 expression during nonmyocyte differentiation in vitro is also presented. The expression levels are relative to controls maintained in expansion medium. Results are presented as the mean of three independent experiments. (C) Pharmacological and genetic inhibition of Notch accelerates differentiation in vitro. On the left, nonmyocyte cultures were established from WT neonatal mouse hearts and placed in differentiation medium in presence of vehicle alone (DMSO) or the γ-secretase inhibitor DAPT. On the right, nonmyocyte cultures were established from WT or Notch1lox/lox MLC2vCre⁺ (N1^del) newborn mice and placed in differentiation medium. RNA was isolated from the differentiated cultures and analyzed by semiquantitative RT-PCR for the expression of the indicated genes. Representative results of three independent experiments are shown. Bar, 20 μm.

Up-regulation of Jagged1 expression in the stressed heart. (A) Immunofluorescence analysis of Jagged1 expression in the heart. The micrograph shows Jagged1 expression on the surface of α-actinin–positive cardiomyocytes with an enlarged area shown in the inset. Nuclei are stained with DAPI. (B) Confocal micrograph showing Jagged1 expression on the surface of α-actinin–positive cardiomyocytes. Arrows in the inset indicate undifferentiated Nkx2.5-positive α-actinin–negative CPCs lying between Jagged1-expressing fibers. The nuclei are stained with DAPI. (C) Heart tissue sections from sham-operated (sham) and clipped (1K1C) mice were subjected to alkaline phosphatase immunohistochemistry using an antibody directed against Jagged1. The representative micrographs show Jagged1 expression in the myocardium at 4, 8, and 12 d after surgery. (D) Jagged1 immunostaining in WT and TG1306/1R transgenic mice as in C. Bars: (A and B) 20 μm; (C and D) 100 μm.