Overexpression of myeloid differentiation protein 88 in mice induces mild cardiac dysfunction, but no deficit in heart morphology

Cardiac remodeling involves changes in heart shape, size, structure, and function after injury to the myocardium. The proinflammatory adaptor protein myeloid differentiation protein 88 (MyD88) contributes to cardiac remodeling. To investigate whether excessive MyD88 levels initiate spontaneous cardiac remodeling at the whole-organism level, we generated a transgenic MyD88 mouse model with a cardiac-specific promoter. MyD88 mice (male, 20-30 g, n=∼80) were born at the expected Mendelian ratio and demonstrated similar morphology of the heart and cardiomyocytes with that of wild-type controls. Although heart weight was unaffected, cardiac contractility of MyD88 hearts was mildly reduced, as shown by echocardiographic examination, compared with wild-type controls. Moreover, the cardiac dysfunction phenotype was associated with elevation of ANF and BNP expression. Collectively, our data provide novel evidence of the critical role of balanced MyD88 signaling in maintaining physiological function in the adult heart.

Cardiac dysfunction; Cardiac remodeling; Transgenic mice; Myeloid differentiation protein 88

Authorship

W. Chen ^*Correspondence: X. Gao: gaoxiang@nju.edu.cn * These authors contributed equally to this study.

Institute for Cardiovascular Science & Department of Cardiovascular Surgery of the First Affiliated Hospital, Soochow University, Suzhou, Jiangsu, ChinaSoochow UniversityChinaSuzhou, Jiangsu, ChinaInstitute for Cardiovascular Science & Department of Cardiovascular Surgery of the First Affiliated Hospital, Soochow University, Suzhou, Jiangsu, China

MOE Key Laboratory of Model Animal for Disease Study, Model Animal Research Center, Nanjing University, Nanjing, Jiangsu, ChinaNanjing UniversityChinaNanjing, Jiangsu, ChinaMOE Key Laboratory of Model Animal for Disease Study, Model Animal Research Center, Nanjing University, Nanjing, Jiangsu, China

Z. Huang ^*Correspondence: X. Gao: gaoxiang@nju.edu.cn * These authors contributed equally to this study.

Jiangsu Province Key Laboratory of Gastrointestinal Nutrition and Animal Health, College of Animal Science and Technology, Nanjing Agriculture University, Nanjing, Jiangsu, ChinaNanjing Agriculture UniversityChinaNanjing, Jiangsu, ChinaJiangsu Province Key Laboratory of Gastrointestinal Nutrition and Animal Health, College of Animal Science and Technology, Nanjing Agriculture University, Nanjing, Jiangsu, China

X. Jiang ^*Correspondence: X. Gao: gaoxiang@nju.edu.cn * These authors contributed equally to this study.

C. Li

Department of Surgery, East Tennessee State University, Johnson City, TN, USAEast Tennessee State UniversityUSAJohnson City, TN, USADepartment of Surgery, East Tennessee State University, Johnson City, TN, USA

X. Gao

Correspondence: X. Gao: gaoxiang@nju.edu.cn * These authors contributed equally to this study.

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Figures

Figures (4)

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Figure 1
Generation of cardiac-specific transgenic (TG) mice overexpressing MyD88. A, Construction map of MyD88 TG mice. MHC: myosin heavy chain; MyD88: myeloid differentiation factor 88; hGH-pA: human growth hormone poly A signal; WT: wild-type. B, PCR of genomic DNA from mouse tails was performed for genotyping. A 711-bp fragment from the genomic MyD88 allele and a 308-bp fragment from the transgenic Flag-MyD88 allele was PCR-amplified with the genotyping primers. C, Tissue-specific expression of the transgene in MyD88 TG mice was performed with anti-Flag antibody. H: heart; SM: skeletal muscle; Li: liver; Sp: spleen; Lu: lungs; Ki: kidney; Br: brain.

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Figure 2
Histological analysis of MyD88 transgenic (TG) hearts. A, Gross appearance of the isolated wild-type (WT) and TG heart. B, Microscopic view of H&E-stained left ventricular sections from MyD88 TG and WT mice. Scale bar: 2 μm.

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Figure 3
MyD88 transgenic (TG) mice did not show an increased heart size. Data are reported as means ± SE. A, Relative heart weights (HW/BW and HW/TL) of wild-type (WT) and TG mice at 5 months of age. HW: heart weight (mg); BW: body weight (g); TL: tibia length (mm); LW: liver weight (g) (n=3-6). The heart and liver were removed, weighed, and normalized to body weight or tibia length. B, Echocardiographic analysis of WT and TG hearts at 5 months of age (n=5-11). LVEDD: left ventricular end-diastolic dimension; LVESD: left ventricular end-systolic dimension; IVSTD: interventricular septal thickness in diastole; PWTD: posterior wall thickness in diastole; *P<0.05 (two-tailed Student’s t-test).

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Figure 4
MyD88 transgenic (TG) mice showed reduced cardiac contractility and elevated heart failure marker expression. A, Representative M-mode echocardiographic views of wild-type (WT) and TG hearts at 5 months (M) of age. Scale bar, 20 μm. B, Statistical analysis of echocardiographic parameters of WT and TG mice (n=5-11). FS%: fractional shortening, FS% = (LVEDD−LVESD)/LVEDD×100; EF%: ejection fraction, EF% = (LVEDD³−LVESD³)/LVEDD³×100. *P<0.05, **P<0.01 compared to WT (two-tailed Student’s t-test). C, Measurement of atrial natriuretic factor (ANF) and brain natriuretic peptide (BNP) mRNA levels in WT and TG hearts at 2 and 5 months of age.

Figure 1 Generation of cardiac-specific transgenic (TG) mice overexpressing MyD88. A, Construction map of MyD88 TG mice. MHC: myosin heavy chain; MyD88: myeloid differentiation factor 88; hGH-pA: human growth hormone poly A signal; WT: wild-type. B, PCR of genomic DNA from mouse tails was performed for genotyping. A 711-bp fragment from the genomic MyD88 allele and a 308-bp fragment from the transgenic Flag-MyD88 allele was PCR-amplified with the genotyping primers. C, Tissue-specific expression of the transgene in MyD88 TG mice was performed with anti-Flag antibody. H: heart; SM: skeletal muscle; Li: liver; Sp: spleen; Lu: lungs; Ki: kidney; Br: brain.

Figure 2 Histological analysis of MyD88 transgenic (TG) hearts. A, Gross appearance of the isolated wild-type (WT) and TG heart. B, Microscopic view of H&E-stained left ventricular sections from MyD88 TG and WT mice. Scale bar: 2 μm.

Figure 3 MyD88 transgenic (TG) mice did not show an increased heart size. Data are reported as means ± SE. A, Relative heart weights (HW/BW and HW/TL) of wild-type (WT) and TG mice at 5 months of age. HW: heart weight (mg); BW: body weight (g); TL: tibia length (mm); LW: liver weight (g) (n=3-6). The heart and liver were removed, weighed, and normalized to body weight or tibia length. B, Echocardiographic analysis of WT and TG hearts at 5 months of age (n=5-11). LVEDD: left ventricular end-diastolic dimension; LVESD: left ventricular end-systolic dimension; IVSTD: interventricular septal thickness in diastole; PWTD: posterior wall thickness in diastole; *P<0.05 (two-tailed Student’s t-test).

Figure 4 MyD88 transgenic (TG) mice showed reduced cardiac contractility and elevated heart failure marker expression. A, Representative M-mode echocardiographic views of wild-type (WT) and TG hearts at 5 months (M) of age. Scale bar, 20 μm. B, Statistical analysis of echocardiographic parameters of WT and TG mice (n=5-11). FS%: fractional shortening, FS% = (LVEDD−LVESD)/LVEDD×100; EF%: ejection fraction, EF% = (LVEDD³−LVESD³)/LVEDD³×100. *P<0.05, **P<0.01 compared to WT (two-tailed Student’s t-test). C, Measurement of atrial natriuretic factor (ANF) and brain natriuretic peptide (BNP) mRNA levels in WT and TG hearts at 2 and 5 months of age.

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Overexpression of myeloid differentiation protein 88 in mice induces mild cardiac dysfunction, but no deficit in heart morphology

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[1] Correspondence: X. Gao: gaoxiang@nju.edu.cn * These authors contributed equally to this study.