Cardiomyopathy of the aging human heart. Myocyte loss and reactive cellular hypertrophy.

Olivetti, G; Melissari, M; Capasso, J. M.; Anversa, Piero

doi:10.1161/01.res.68.6.1560

Cited by 660 publications

(376 citation statements)

References 33 publications

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“…Some collagen family members were also up-regulated, including Type XV collagen alpha 1, Type VI collagen alpha 3, Type IV collagen alpha 1, and Type VI collagen alpha 2. These observations are consistent with previous findings that the aging heart undergoes ECM protein deposition (30), fibrosis (31), and cardiomyocyte hypertrophy (11).…”

Section: Aging Results In Expression Of Genes Encoding Structural Prosupporting

confidence: 93%

“…Age-related changes in human and rodent hearts include a reduction in the number of myocytes (10,11), myocyte hypertrophy (11,12), cardiac fibrosis (13), lipofuscin pigment accumulation (14), a reduction in calcium transport across sarcoplasmic reticulum membrane (15), and alterations in the response to ␤-adrenergic stimulation (16). Collectively, these alterations likely contribute to age-related heart diseases being the leading cause of mortality in the U.S. (17).…”

mentioning

confidence: 99%

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Transcriptional profiles associated with aging and middle age-onset caloric restriction in mouse hearts

Lee

Allison

Brand

et al. 2002

Proc. Natl. Acad. Sci. U.S.A.

289

218

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To provide a global analysis of gene expression in the aging heart, we monitored the expression of 9,977 genes simultaneously in 5-and 30-month-old male B6C3F1 mice by using high-density oligonucleotide microarrays and several statistical techniques. Aging was associated with transcriptional alterations consistent with a metabolic shift from fatty acid to carbohydrate metabolism, increased expression of extracellular matrix genes, and reduced protein synthesis. Caloric restriction (CR) started at 14 months of age resulted in a 19% global inhibition of age-related changes in gene expression. Interestingly, CR also resulted in alterations in gene expression consistent with preserved fatty acid metabolism, reduced endogenous DNA damage, decreased innate immune activity, apoptosis modulation, and a marked cytoskeletal reorganization. These observations provide evidence that aging of the heart is associated with specific transcriptional alterations, and that CR initiated in middle age may retard heart aging by inducing a profound transcriptional reprogramming.W hen started either early in life or at middle age, caloric restriction (CR) increases average and maximum lifespan, and reduces the incidence and delays the onset of spontaneous cancers and several other age-related diseases (1). Additionally, CR reduces the age-associated increase in reactive oxygen species (ROS)-induced molecular damage (2-5). Previously, we have used high-density oligonucleotide arrays to define aging and CR-related transcriptional alterations in mouse skeletal muscle (6) and brain (7). These reports provided evidence for an age-associated stress response characterized by the induction of heat-shock factors and other oxidative stress-induced transcripts. CR prevented these age-related alterations completely or partially. Both studies provided further support for the concept that oxidative stress may be an important, and perhaps underlying cause of the aging process of postmitotic tissues.The cardiac myocyte is the most energy demanding cell in the body, contracting constantly, 3 billion times or more in the average human lifespan (8), requiring large supplies of high-energy phosphates (9). Age-related changes in human and rodent hearts include a reduction in the number of myocytes (10, 11), myocyte hypertrophy (11, 12), cardiac fibrosis (13), lipofuscin pigment accumulation (14), a reduction in calcium transport across sarcoplasmic reticulum membrane (15), and alterations in the response to ␤-adrenergic stimulation (16). Collectively, these alterations likely contribute to age-related heart diseases being the leading cause of mortality in the U.S. (17). CR reduces the severity of spontaneous cardiomyopathy in male Sprague-Dawley rats (18) and prevents age-associated alterations in late diastolic function in B6D2F 1 mice (19). At the molecular level, CR reduces the concentration of both 8-hydroxydeoxyguanosine in DNA (20) and dityrosine cross-linking of proteins (21) in the heart of aging mice, and prevents somatic mitochondrial genomic rear...

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Section: Aging Results In Expression Of Genes Encoding Structural Prosupporting

confidence: 93%

mentioning

confidence: 99%

Transcriptional profiles associated with aging and middle age-onset caloric restriction in mouse hearts

Lee

Allison

Brand

et al. 2002

Proc. Natl. Acad. Sci. U.S.A.

289

218

View full text Add to dashboard Cite

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“…Both phenomena decrease the reserve of the myocardium to sustain increases in mechanical load generated by myocardial infarction, systemic hypertension, or their combination. Diabetic cardiomyopathy resembles the aged heart in men, in which tissue damage is not apparent in spite of an agedependent loss of myocytes and reactive hypertrophy of the viable cells (Olivetti et al, 1991(Olivetti et al, , 1995. Similar findings have been obtained in aging Sprague-Dawley rats (Anversa et al, 1986).…”

Section: Figuresupporting

confidence: 78%

Myocyte Death in Streptozotocin-Induced Diabetes in Rats Is Angiotensin II- Dependent

Fiordaliso

Latini

et al. 2000

Laboratory Investigation

275

217

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SUMMARY:To determine whether myocyte death and angiotensin II (AT II) formation are implicated in the development of diabetic cardiomyopathy, rats were injected with streptozotocin, and apoptosis and necrosis were measured at 3, 10, and 28 days. Expression of the components of the renin-angiotensin system (RAS) and AT II levels were assessed at 3 days. The percentage of AT II-labeled myocytes and the number and distribution of AT II sites in myocytes were measured at 3 and 10 days. The effects of AT 1 blockade on local RAS and cell death were examined at 3 days. Diabetes was characterized by myocyte apoptosis that peaked at 3 days and decreased at 10 and 28 days, in spite of high concentrations of blood glucose. Cell necrosis was absent throughout. Angiotensinogen, renin, and AT 1 receptor increased in myocytes from diabetic rat hearts, while angiotensin-converting enzyme and AT 2 remained constant. AT II quantity increased severalfold, as did the fraction of AT II positive cells and the number of AT II sites per myocyte. However, AT II labeling decreased at 10 days, which paralleled the reduction in myocyte death. AT 1 antagonist inhibited upregulation of this receptor and angiotensinogen, which prevented AT II synthesis and myocyte death at their peaks with diabetes. An aggregate 30% myocyte loss and a 14% increase in the volume of viable cells were found in diabetic rats at 28 days. Thus diabetic cardiomyopathy may be viewed as an AT II-dependent process in which that peptide plays a critical role in myocyte death and hypertrophy. (Lab Invest 2000, 80:513-527).

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“…20 Standard published human ECG results consist of an HR of 60-100 beats/min, a mean PR interval of 120-200 ms, a mean QRS interval of <120 ms, and a mean QT interval of 420 ms. 21,22 In an earlier National Health Statistics Report, the mean weight of female adults over 20 years of age in the United States from 2003 to 2006 was 74.7 kg and that of males was 88.3 kg. 23 Additionally, a study evaluating the diseasefree aging heart reported BW from adults over 20 years of age ranging from 51 to 99 kg and HW of 123 to 306 g. 24 …”

Section: Sinclairmentioning

confidence: 99%

Comparative cardiovascular physiology and pathology in selected lineages of minipigs

Stricker–Krongrad

Shoemake

Brocksmith

et al. 2017

Toxicology Research and Application

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The minipig has been increasingly recognized as a valid alternative to canines and nonhuman primates in regulatory toxicity. This article presents the results of cardiovascular assessments in the Yucatan, Hanford, Sinclair, and Göttingen minipigs conducted during nonclinical investigations and control toxicity testing. Cardiac electrophysiology was obtained using clinical electrocardiogram and surgical monitor units. Peripheral vessel diameter, velocity, and flow were obtained by Doppler ultrasonography, and cardiac vessel diameter was obtained postmortem. Anatomic parameters were obtained at necropsy. Histopathology assessments were conducted on heart, blood vessels, and kidneys. Collected data were compared to published cardiovascular measurements of adult humans to illustrate similarities and differences. Each lineage of minipigs was found to have specific anatomic and physiologic characteristics that may accurately reflect response of human cardiovascular systems in clinical investigations and toxicity testing. In conclusion, the interspecies similarities between the cardiovascular systems make these lineages of minipigs suitable as models for the human counterpart. In addition, these reported differences between lineages will aid investigators in selecting a relevant lineage of minipigs if specific cardiovascular parameters are required during drug safety evaluation.

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Cardiomyopathy of the aging human heart. Myocyte loss and reactive cellular hypertrophy.

Cited by 660 publications

References 33 publications

Transcriptional profiles associated with aging and middle age-onset caloric restriction in mouse hearts

Transcriptional profiles associated with aging and middle age-onset caloric restriction in mouse hearts

Myocyte Death in Streptozotocin-Induced Diabetes in Rats Is Angiotensin II- Dependent

Comparative cardiovascular physiology and pathology in selected lineages of minipigs

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