A: Progressive cardiac enlargement in Nf1mKO. Comparison of heart weight/body weight (left) and heart weight/tibia length (right) ratios of control and Nf1mKO mice at 4 and 12 weeks, and control, Nf1mKO, and Nf1mKO+GRD at 20 weeks. There is no significant difference in either measure at 4 weeks, with a small but statistically significant elevation of both in Nf1mKO at 12 weeks. By 20 weeks, there is a dramatic enlargement of the hearts of Nf1mKO compared to control and Nf1mKO+GRD as measured by both indices. The hearts of Nf1mKO+GRD mice are slightly, but significantly, larger than wild type.
B: Progressive myocardial fibrosis and myocyte enlargement in Nf1mKO. Trichrome stained long axis sections of control and Nf1mKO hearts at 4, 12, and 20 weeks at low power (2×) and high power (20×) are shown, along with wheat germ agglutinin (WGA) stained high power (20×) sections. At 4 weeks the overall hearts, as well as the higher-magnification sections of the myocardium appear similar. There is also no size difference in the myocytes as evidenced by WGA staining of the sarcolemma. By 12 weeks there is subtle gross enlargement of the heart in Nf1mKO. However there is no obvious increase in fibrous staining in Nf1mKO at low or high power. Myocytes appear slightly enlarged in Nf1mKO. At 20 weeks the Nf1mKO heart is clearly larger and has marked fibrosis. Myocytes in Nf1mKO are also enlarged. Vertical scale bars = 1mm, horizontal scale bars = 50µm.
C: Quantification of progressive myocyte enlargement in Nf1mKO. Measurement of the areas enclosed by the WGA staining of the sarcolemma show that the average size of myocytes in Nf1mKO is not significantly different from control at 4 weeks. There is a small but significant increase in the myocyte size in Nf1mKO by 12 weeks, which progresses further by 20 weeks.

Quantitative RT-PCR of cDNA from Nf1mKO and control hearts at 4, 12, and 20 weeks (±SEM) shows a marked, progressive increase in atrial naturetic peptide (ANP), brain-type naturetic peptide (BNP), and β-myosin heavy chain (β-MHC) mRNA in Nf1mKO relative to control at each age. Transcription of these genes is indicative of activation of a fetal gene program, as they are not abundantly found in normal adult hearts.

A: LacZ staining of e12.0 offspring of α-MCH-cre × R26R. Cre+ embryo (right) demonstrates LacZ activity in the heart (arrow). No LacZ activity is seen in the Cre-littermate (left).
B: Loss of myocardial neurofibromin in Nf1mKO. Immunoblot of neurofibromin and β-tubulin of 2 independent whole-heart homogenates from adult (12 week) control and Nf1-myocardial KO (Nf1mKO) mice. Neurofibromin is detected in control samples, but not in Nf1mKO. β-tubulin (loading control) is equivalent for all samples.
C: GRD dependant elevation of Ras-GTP/Total Ras ratio in Nf1mKO hearts. Immunoblot quantification of Ras before (“Total Ras”) and after (“Ras-GTP”) Raf-1 pulldown in 3 independent sets of whole-heart homogenates from newborn (P0) control, Nf1mKO, and Nf1mKO with Rosa-HA-GRD (Nf1mKO+GRD) mice. Ras-GTP/Total Ras ratio is significantly (p=0.031) elevated in Nf1mKO compared to wild type. This elevation of is rescued to control levels in Nf1mKO+GRD.
D: Sample immunoblot of Ras from 2 sets of whole-heart homogenates from newborn (P0) control, Nf1mKO, and Nf1mKO+GRD mice before (“Total Ras”) and after (“Ras-GTP”) Raf-1 pulldown. Total Ras is 1/10 of input of Ras-GTP after pulldown. There is increased Ras-GTP in Nf1mKO relative to control without marked changes in total Ras. Ras-GTP in Nf1mKO+GRD is reduced compared with Nf1mKO.
E: Ras-dependant activation of Erk, Akt, and mTOR in Nf1mKO. Immunoblots of total and phospho- Erk, Akt, GSK3β, and mTOR of 2 independent whole-heart homogenates from newborn (P0) control and Nf1mKO mice. There is increased phospho-Erk, Akt, and mTOR(serine 2481) consistent with hyperactivation of Ras signaling in Nf1mKO. There is also increased phospho-GSK3β in Nf1mKO, consistent with decreased activation of GSK3β. GAPDH is used as a loading control.
F: Late mortality in Nf1mKO. Kaplan-Meier survival analysis of Nf1mKO (n=20) compared with controls (n=23). There were no deaths over the first 16 weeks. However, following approximately 20 weeks, there was steady mortality of Nf1mKO with no loss among control littermates.

A: Progressive decreased fractional shortening of Nf1mKO. Echocardiographic measurement of fractional shortening (FS) in Nf1mKO and control mice at 12 and 20 weeks (±SEM) shows a small decrease in FS at 12 weeks that is markedly worsened by 20 weeks. Representative 20 week M-mode echocardiogram of control (top) and Nf1mKO (bottom), showing LV chamber dilation and reduced shortening in Nf1mKO.
B: Reduced LV contractility and impaired relaxation in Nf1mKO. Representative pressure-volume (PV) loops from Nf1mKO and control mice at 12 weeks (left) and 20 weeks (right) showing the relationship between LV pressure and volume throughout the cardiac cycle. At 12 weeks, there is a mild increase in LV end-diastolic volume in Nf1mKO, with a concomitant decrease in stroke volume (reduced PV loop width). Systolic pressure is reduced in Nf1mKO, but diastolic pressure is preserved. By 20 weeks, there is a rightward shift of the Nf1mKO PV loop, indicating LV dilation. The narrow loop indicates a reduced stroke volume, and the LV end-diastolic pressure (arrow) is elevated in Nf1mKO.
C: Impaired contractility and relaxation in Nf1mKO hearts. Representative tracings of LV pressure (top) and dp/dt (bottom) at 12 weeks. There is both reduced peak LV pressure and maximal dp/dt in Nf1mKO, indicating systolic dysfunction. Further, there is elevated LV end-diastolic pressure and minimal dp/dt in Nf1mKO, indicating diastolic dysfunction and impaired myocardial relaxation.
D: Quantification of maximal and minimal dp/dt in 12 week old Nf1mKO (n=3) and control (n=4) adult mice. The reduction in maximal and elevation in minimal dp/dt in Nf1mKO were both statistically significant and indicative of early systolic and diastolic heart failure.