Blood Pressure, Artery Size, and Artery Compliance Parallel Bone Size and Strength in Mice With Differing Ece1 Expression

Wang, Zhijie; Kristianto, Jasmin; Ooi, Chen Yen; Johnson, Michael G.; Litscher, Suzanne J.; Pugh, Thomas D.; Sandhu, Gurpreet S.; Chesler, Naomi C.; Blank, Robert D.

doi:10.1115/1.4024161

Cited by 5 publications

(6 citation statements)

References 40 publications

(52 reference statements)

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“…Previous work in our laboratory using the recombinant congenic mice HcB-8 and HcB-23 identified ECE-1, the gene encoding ECE-1, as a positional candidate for a pleiotropic quantitative trait locus influencing bone strength and size in skeletally mature mice (Saless et al 2009(Saless et al , 2010(Saless et al , 2011aKristianto et al 2016). In these mice, higher expression of ECE-1 is associated with the presence of larger, stronger, and denser bones (Wang et al 2013). We hypothesized that big ET-1 signaling promotes osteoblast differentiation and mineralization in normal physiology.…”

Section: Introductionmentioning

confidence: 99%

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Endothelin signaling regulates mineralization and posttranscriptionally regulates SOST in TMOb cells via miR 126-3p

et al. 2017

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Previously, our laboratory identified ECE‐1, encoding endothelin‐converting enzyme‐1 (ECE‐1), as a positional candidate for a pleiotropic quantitative trait locus affecting femoral size, shape, and biomechanical performance. We hypothesized that endothelin‐1 (ET‐1) signaling promotes osteogenesis. Exposure of immortalized mouse osteoblast (TMOb) cells to big ET‐1 increased mineralization. Following big ET‐1 treatment, we measured the secretion of insulin‐like‐growth factor‐1 (IGF1), dickkopf‐homolog‐1 protein 1 (DKK1), and sclerostin (SOST). In each case, big ET‐1 signaling changed secretion in a manner that favored increased osteogenic activity. Treatment with ECE‐1, endothelin receptor A (EDNRA), or WNT receptor antagonists inhibited the big ET‐1‐mediated increase in mineralization. In the presence of big ET‐1, message levels of Runx2, Igf1, Dkk1, and Sost are uncoupled from protein production, suggesting posttranscriptional regulation. To evaluate the role of big ET‐1 in normal bone physiology, we inhibited EDNRA signaling during mineralization in the absence of exogenous ET‐1. EDNRA blockade reduced mineralization, decreased IGF1, and increased DKK1 and SOST secretion, responses opposite to those induced by exogenous big ET‐1. Pharmacological and siRNA knockdown to inhibit ECE‐1 reduced mineralization and IGF1 secretion with decreasing DKK1 and decreasing or stable SOST secretion, suggesting a further, unknown role of ECE‐1 in osteoblast maturation. Previously we identified miR 126‐3p as a potential ET‐1‐responsive regulator of SOST in murine cells. Overexpression of miR126‐3p increased mineralization in TMOb cells and decreased SOST secretion. Osteoblasts express the ET‐1 signaling pathway and ET‐1 signaling is necessary for normal osteoblast differentiation and mineralization, acting through regulation of miRs that target osteogenic molecules.

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Section: Introductionmentioning

confidence: 99%

“…In these mice, higher expression of ECE‐1 is associated with the presence of larger, stronger, and denser bones (Wang et al. ). We hypothesized that big ET‐1 signaling promotes osteoblast differentiation and mineralization in normal physiology.…”

Section: Introductionmentioning

confidence: 99%

Endothelin signaling regulates mineralization and posttranscriptionally regulates SOST in TMOb cells via miR 126-3p

et al. 2017

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“…Endothelial cells are the primary source of ET1 and have a high density of EDNRB, so autocrine signaling favors vasodilation and hypotensive responses, while paracrine signaling leads to hypertensive responses. In experiments we performed using the same mice in which we identified Ece1 as a candidate gene for bone biomechanical performance, we found that mice harboring a high-expressing Ece1 allele had larger femoral and arterial cross-sections, greater arterial compliance, and lower BP than mice harboring a low-expressing Ece1 allele 52 .…”

Section: Future Considerationsmentioning

confidence: 89%

Endothelin Signaling in Bone

Kristianto

Johnson

Afzal

et al. 2017

Endocrinology and Metabolism Clinics of North America

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“…The LCCA was stretched 150% axially to mimic in vivo length (Tian et al, 2013; Wang et al, 2013a), pressurized to 90 mmHg, and allowed to equilibrate at 37°C for 30 minutes. Sinusoidal pressure cycles of 90-120 mmHg at 1 Hz were applied for pre-conditioning to achieve a consistent mechanical response (Fung et al, 1979).…”

Section: Methodsmentioning

confidence: 99%

Mitochondria DNA mutations cause sex-dependent development of hypertension and alterations in cardiovascular function

Golob¹,

Tian²,

Wang³

et al. 2015

Journal of Biomechanics

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Aging is associated with conduit artery stiffening that is a risk factor for and can precede hypertension and ventricular dysfunction. Increases in mitochondria DNA (mtDNA) frequency have been correlated with aging. Mice with a mutation in the encoding domain (D257A) of a proof-reading deficient version of mtDNA polymerase-γ (POLG) have musculoskeletal features of premature aging and a shortened lifespan. However, few studies using these mice have investigated the effects of mtDNA mutations on cardiovascular function. We hypothesized that the proof-reading deficient mtDNA POLG leads to arterial stiffening, hypertension, and ventricular hypertrophy. Ten to twelve month-old D257A mice (n=13) and age- and sex-matched wild-type controls (n=13) were catheterized for hemodynamic and ventricular function measurements. Left common carotid arteries (LCCA) were harvested for mechanical tests followed by histology. Male D257A mice had pulmonary and systemic hypertension, arterial stiffening, larger LCCA diameter (701 ± 45 vs. 597 ± 60 μm), shorter LCCA axial length (8.96 ± 0.56 vs. 10.10 ± 0.80 mm), and reduced hematocrit (29.1 ± 6.1 vs. 41.3 ± 8.1; all p<0.05). Male and female D257A mice had biventricular hypertrophy (p<0.05). Female D257A mice did not have significant increases in pressure or arterial stiffening, suggesting that the mechanisms of hypertension or arterial stiffening from mtDNA mutations differ based on sex. Our results lend insight into the mechanisms of age-related cardiovascular disease and may point to novel treatment strategies to address cardiovascular mortality in the elderly.

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Blood Pressure, Artery Size, and Artery Compliance Parallel Bone Size and Strength in Mice With Differing Ece1 Expression

Cited by 5 publications

References 40 publications

Endothelin signaling regulates mineralization and posttranscriptionally regulates SOST in TMOb cells via miR 126-3p

Endothelin signaling regulates mineralization and posttranscriptionally regulates SOST in TMOb cells via miR 126-3p

Endothelin Signaling in Bone

Mitochondria DNA mutations cause sex-dependent development of hypertension and alterations in cardiovascular function

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