Your search keyword '"Jhana O. Hendrickx"' showing total 44 results

1. Chronic Inhibition of Nitric Oxide Synthases Impairs Spatiotemporal Learning and Memory to a Similar Extent in C57BL/6 and hAPP23+/− Mice

Author

Jhana O. Hendrickx, Elke Calus, Peter Paul De Deyn, Debby Van Dam, and Guido R. Y. De Meyer

Subjects

arterial stiffness, Alzheimer’s disease, nitric oxide, learning and memory, amyloid, Computer applications to medicine. Medical informatics, R858-859.7

Abstract

Due to global population growth, age-related disorders like cardiovascular disease and dementia are anticipated to increase. Recent data suggests a connection between cardiovascular disease and neurodegeneration, especially focusing on arterial stiffness (AS) and Alzheimer’s disease (AD). In light of this, we conducted a study to explore the impact of long-term nitric oxide synthase (NOS) isoform inhibition, which leads to AS, on neurobehavioral performance. We also compared these effects in an AD model and control mice. C57BL/6 and hAPP23+/− mice (an established AD model) were given 0.5 mg/mL N(G)-Nitro-L-Arginine Methyl Ester (L-NAME) in their drinking water for 16 weeks. Our findings indicate that chronic non-selective NOS inhibition increased AS and reduced spatiotemporal learning and memory in both C57BL/6 and hAPP23+/− mice. These effects were consistent across both groups, emphasizing the role of neuronal NOS (nNOS) in cognitive aging, regardless of genetic predisposition to AD.

Published

2023

2. Progressive aortic stiffness in aging C57Bl/6 mice displays altered contractile behaviour and extracellular matrix changes

Author

Sofie De Moudt, Jhana O. Hendrickx, Cédric Neutel, Dorien De Munck, Arthur Leloup, Guido R. Y. De Meyer, Wim Martinet, and Paul Fransen

Subjects

Biology (General), QH301-705.5

Abstract

A 24-month aging study in male C57Bl/6 mice reveals that aortic aging precedes cardiovascular disease and is due to changes in the extracellular matrix and vascular smooth muscle cell signaling.

Published

2022

3. Disparate biomechanical properties of the aorta in non‐aneurysmal and aneurysmal mice treated with angiotensin II

Author

Sofie De Moudt, Jhana O. Hendrickx, Guido R. Y. De Meyer, Wim Martinet, and Paul Fransen

Subjects

abdominal aortic aneurysm, aortic stiffness, contraction, vascular smooth muscle cells, Physiology, QP1-981

Abstract

Abstract In vivo angiotensin II (AngII)‐treatment is a widely used experimental model to induce cardiovascular disease and results in a high likelihood of abdominal aorta aneurysm (AAA) formation. This involves progressive and irreversible focal dilation of the abdominal aorta and induces adverse aortic connective tissue remodeling contributing to aortic wall stiffening through inflammation, elastin degradation, and collagen restructuring. Hence, the present study aimed to investigate how AAA formation in AngII‐treated mice affects aortic function and biomechanics. To this end, C57Bl/6J mice were treated with AngII (1000 ng/[kg.min]) or PBS infusion for 28 days. Peripheral blood pressure, echocardiography, and aortic pulse wave velocity were measured in vivo. Thoracic aorta rings were studied ex vivo in organ chambers, while aortic vascular smooth muscle cell (VSMC) phenotype was investigated histologically. We confirmed peripheral hypertension, cardiac hypertrophy, aortic stiffening, and increased VSMC proliferation and migration after AngII‐treatment. Abdominal aorta aneurysm formation was observed in 8/13 AngII‐treated mice. Ex vivo thoracic aortic rings of both aneurysmal and non‐aneurysmal AngII‐treated mice showed high isobaric aortic stiffness, endothelial dysfunction, heightened α1‐adrenergic contractility, and altered VSMC contractile calcium signaling. However, aortic biomechanics were differently affected, with heightened α1‐adrenoreceptor mediated aortic stiffening in non‐aneurysmal mice, whereas contraction‐dependent stiffening was impaired in aneurysmal mice. In conclusion, although aneurysmal and non‐aneurysmal 4‐week AngII‐treated mice displayed similar changes in aortic physiology, aortic biomechanics were dissimilarly affected.

Published

2022

4. Aortic Stiffness in L-NAME Treated C57Bl/6 Mice Displays a Shift From Early Endothelial Dysfunction to Late-Term Vascular Smooth Muscle Cell Dysfunction

Author

Sofie De Moudt, Jhana O. Hendrickx, Cédric Neutel, Dorien De Munck, Arthur Leloup, Guido R.Y. De Meyer, Wim Martinet, and Paul Fransen

Subjects

aortic stiffness, hypertension, calcium, vascular smooth muscle cell, endothelial function (dysfunction), voltage-gated calcium channel, Physiology, QP1-981

Abstract

Introduction and Aims: Endothelial dysfunction is recognized as a cardiovascular aging hallmark. Administration of nitric oxide synthase blocker N-Ω-Nitro-L-arginine methyl ester hydrochloride (L-NAME) constitutes a well-known small animal model of cardiovascular aging. Despite extensive phenotypic characterization, the exact aortic function changes in L-NAME treated mice are largely unknown. Therefore, this study presents a longitudinal characterization of the aortic reactivity and biomechanical alterations in L-NAME treated C57Bl/6 mice.Methods and Results: Male C57Bl/6 mice were treated with L-NAME (0.5 mg/ml drinking water) for 1, 2, 4, 8, or 16 weeks. Peripheral blood pressure measurement (tail-cuff) and transthoracic echocardiograms were recorded, showing progressive hypertension after 4 weeks of treatment and progressive cardiac hypertrophy after 8–16 weeks of treatment. Aortic stiffness was measured in vivo as aortic pulse wave velocity (aPWV, ultrasound) and ex vivo as Peterson modulus (Ep). Aortic reactivity and biomechanics were investigated ex vivo in thoracic aortic rings, mounted isometrically or dynamically-stretched in organ bath set-ups. Aortic stiffening was heightened in L-NAME treated mice after all treatment durations, thereby preceding the development of hypertension and cardiac aging. L-NAME treatment doubled the rate of arterial stiffening compared to control mice, and displayed an attenuation of the elevated aortic stiffness at high distending pressure, possibly due to late-term reduction of medial collagen types I, III, and IV content. Remarkably, endothelial dysfunction, measured by acetylcholine concentration-response stimulation in precontracted aortic rings, was only observed after short-term (1–4 weeks) treatment, followed by restoration of endothelial function which coincided with increased phosphorylation of endothelial nitric oxide synthase (S1177). In the late-disease phase (8–16 weeks), vascular smooth muscle cell (VSMC) dysfunction developed, including increased contribution of voltage-dependent calcium channels (assessed by inhibition with diltiazem), basal VSMC cytoplasmic calcium loading (assessed by removal of extracellular calcium), and heightened intracellular contractile calcium handling (assessed by measurement of sarcoplasmic reticulum-mediated transient contractions).Conclusion: Arterial stiffness precedes peripheral hypertension and cardiac hypertrophy in chronic L-NAME treated male C57Bl/6 mice. The underlying aortic disease mechanisms underwent a distinct shift from early endothelial dysfunction to late-term VSMC dysfunction, with continued disease progression.

Published

2022

5. Basal Vascular Smooth Muscle Cell Tone in eNOS Knockout Mice Can Be Reversed by Cyclic Stretch and Is Independent of Age

Author

Sofie De Moudt, Jhana O. Hendrickx, Guido R. Y. De Meyer, Wim Martinet, and Paul Fransen

Subjects

cyclic stretch, vascular smooth muscle, calcium, arterial stiffness, endothelial nitric oxide synthase, Physiology, QP1-981

Abstract

Introduction and Aims: Endothelial nitric oxide synthase (eNOS) knockout mice develop pronounced cardiovascular disease. In the present study, we describe the alterations in aortic physiology and biomechanics of eNOS knockout and C57Bl/6 control mice at 2–12 months of age, including a thorough physiological investigation of age and cyclic stretch-dependent VSMC contractility and aortic stiffness.Methods and Results: Peripheral blood pressure and aortic pulse wave velocity were measured in vivo, and aortic biomechanical studies and isometric contractions were investigated ex vivo. Age-dependent progression of aortic stiffness, peripheral hypertension, and aortic contractility in eNOS knockout mice was absent, attenuated, or similar to C57Bl/6 control mice. Voltage-gated calcium channel (VGCC)-dependent calcium influx inversely affected isometric contraction and aortic stiffening by α1-adrenergic stimulation in eNOS knockout mice. Baseline aortic stiffness was selectively reduced in eNOS knockout mice after ex vivo cyclic stretch exposure in an amplitude-dependent manner, which prompted us to investigate cyclic stretch dependent regulation of aortic contractility and stiffness. Aortic stiffness, both in baseline conditions and after activation of vascular smooth muscle cell (VSMC) contraction, was reduced with increasing cyclic stretch amplitude. This cyclic stretch dependency was attenuated with age, although aged eNOS knockout mice displayed better preservation of cyclic stretch-dependency compared to C57Bl/6 control mice. Store operated calcium entry-medicated aortic stiffening as induced by inhibiting sarcoplasmic reticulum calcium ATPase pumps with 10 µM CPA was most pronounced in the aorta of aged mice and at low cyclic stretch amplitude, but independent of eNOS. Basal aortic tonus and VSMC depolarization were highly dependent on eNOS, and were most pronounced at low cyclic stretch, with attenuation at increasing cyclic stretch amplitude.Conclusion: eNOS knockout mice display attenuated progression of arterial disease as compared to C57Bl/6 control mice. Basal VSMC tone in eNOS knockout mice could be reduced by ex vivo exposure to cyclic stretch through stretch-dependent regulation of cytosolic calcium. Both baseline and active aortic stiffness were highly dependent on cyclic stretch regulation, which was more pronounced in young versus aged mice. Other mediators of VSMC contraction and calcium handling were dependent on cyclic stretch mechanotransduction, but independent of eNOS.

Published

2022

6. G Protein-Coupled Receptor Systems and Their Role in Cellular Senescence

Author

Paula Santos-Otte, Hanne Leysen, Jaana van Gastel, Jhana O. Hendrickx, Bronwen Martin, and Stuart Maudsley

Subjects

Biotechnology, TP248.13-248.65

Abstract

Aging is a complex biological process that is inevitable for nearly all organisms. Aging is the strongest risk factor for development of multiple neurodegenerative disorders, cancer and cardiovascular disorders. Age-related disease conditions are mainly caused by the progressive degradation of the integrity of communication systems within and between organs. This is in part mediated by, i) decreased efficiency of receptor signaling systems and ii) an increasing inability to cope with stress leading to apoptosis and cellular senescence. Cellular senescence is a natural process during embryonic development, more recently it has been shown to be also involved in the development of aging disorders and is now considered one of the major hallmarks of aging. G-protein-coupled receptors (GPCRs) comprise a superfamily of integral membrane receptors that are responsible for cell signaling events involved in nearly every physiological process. Recent advances in the molecular understanding of GPCR signaling complexity have expanded their therapeutic capacity tremendously. Emerging data now suggests the involvement of GPCRs and their associated proteins in the development of cellular senescence. With the proven efficacy of therapeutic GPCR targeting, it is reasonable to now consider GPCRs as potential platforms to control cellular senescence and the consequently, age-related disorders. Keywords: G protein-coupled receptors (GPCRs), Aging, Cellular senescence, β-Arrestin, G protein-coupled receptor kinase interacting protein 2 (GIT2)

Published

2019

7. Proteomic Assessment of C57BL/6 Hippocampi after Non-Selective Pharmacological Inhibition of Nitric Oxide Synthase Activity: Implications of Seizure-like Neuronal Hyperexcitability Followed by Tauopathy

Author

Jhana O. Hendrickx, Charlotte Adams, Anne Sieben, Kris Laukens, Debby Van Dam, and Guido R. Y. De Meyer

Subjects

hippocampus, L-NAME, nitric oxide, proteomics, hyperexcitability, ribosomal dysfunction, Biology (General), QH301-705.5

Abstract

Nitric oxide (NO) is a small gaseous signaling molecule responsible for maintaining homeostasis in a myriad of tissues and molecular pathways in neurology and the cardiovasculature. In recent years, there has been increasing interest in the potential interaction between arterial stiffness (AS), an independent cardiovascular risk factor, and neurodegenerative syndromes given increasingly epidemiological study reports. For this reason, we previously investigated the mechanistic convergence between AS and neurodegeneration via the progressive non-selective inhibition of all nitric oxide synthase (NOS) isoforms with N(G)-nitro-L-arginine methyl ester (L-NAME) in C57BL/6 mice. Our previous results showed progressively increased AS in vivo and impaired visuospatial learning and memory in L-NAME-treated C57BL/6 mice. In the current study, we sought to further investigate the progressive molecular signatures in hippocampal tissue via LC–MS/MS proteomic analysis. Our data implicate mitochondrial dysfunction due to progressive L-NAME treatment. Two weeks of L-NAME treatment implicates altered G-protein-coupled-receptor signaling in the nerve synapse and associated presence of seizures and altered emotional behavior. Furthermore, molecular signatures implicate the cerebral presence of seizure-related hyperexcitability after short-term (8 weeks) treatment followed by ribosomal dysfunction and tauopathy after long-term (16 weeks) treatment.

Published

2022

8. Inflammation, Nitro-Oxidative Stress, Impaired Autophagy, and Insulin Resistance as a Mechanistic Convergence Between Arterial Stiffness and Alzheimer’s Disease

Author

Jhana O. Hendrickx, Wim Martinet, Debby Van Dam, and Guido R. Y. De Meyer

Subjects

inflammaging, metabolism, nitro-oxidative stress, autophagy, neurodegeneration, arterial stiffness, Biology (General), QH301-705.5

Abstract

The average age of the world’s elderly population is steadily increasing. This unprecedented rise in the aged world population will increase the prevalence of age-related disorders such as cardiovascular disease (CVD) and neurodegeneration. In recent years, there has been an increased interest in the potential interplay between CVDs and neurodegenerative syndromes, as several vascular risk factors have been associated with Alzheimer’s disease (AD). Along these lines, arterial stiffness is an independent risk factor for both CVD and AD. In this review, we discuss several inflammaging-related disease mechanisms including acute tissue-specific inflammation, nitro-oxidative stress, impaired autophagy, and insulin resistance which may contribute to the proposed synergism between arterial stiffness and AD.

Published

2021

9. P.17 Reduced Isometric Contractility and Isobaric Compliance of the ex vivo Thoracic Aorta of Hypertensive APP23+/− overexpressing Mice due to Serum Corticosterone Levels

Author

Jhana O. Hendrickx, Sofie De Moudt, Debby Van Dam, Guido R.Y. De Meyer, and Paul Fransen

Subjects

Dementia, stress, vascular disease, Specialties of internal medicine, RC581-951, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Objective: Alzheimer’s disease (AD) is characterized by noticeable neuropsychiatric symptoms and cognitive decline [1]. In addition, cardiovascular disease (CVD) is a known etiological hallmark of AD pathogenesis [2]. Recent epidemiological evidence suggests an interplay between arterial stiffness (AS) and AD [3]. Therefore, we aimed for an in-depth vascular characterization of the APP23+/− overexpressing AD mouse model (APP23+/−). Methods: Blood pressure (BP, CODA) and aortic pulse wave velocity (aPWV, VEVO2100) were measured in vivo, whereas isometric vascular reactivity (organ chambers), isobaric AS (Peterson modulus (Ep)) and compliance (Rodent Oscillatory Tension Set-up for Arterial Compliance) were determined ex vivo in thoracic aorta segments of APP23+/− mice (male, n = 10) vs. C57BL/6 mice (male, n = 18) at the age of 6 months. Corticosterone levels were analysed on blood serum by means of ELISA. The data are given as mean ± SEM. Results: APP23+/− mice showed elevated corticosterone levels (Figure 1A) associated with increased peripheral systolic BP (Figure 1B) and aPWV in vivo (Figure 1C), and decreased isometric adrenoreceptor-dependent contractions ex vivo upon phenylephrine stimulation (Figure 1D). Ex vivo isobaric AS measurements at baseline disclosed a smaller aortic diameter of APP23+/− mice (Figure 2A) resulting in reduced compliance (Figure 2B), with no Ep differences (Figure 2C). Upon phenylephrine treatment, a smaller effect on aortic constriction (Figure 2D), compliance (Figure 2E) and Ep (Figure 2F) was observed for APP23+/− animals, corresponding to reduced isometric contractions (Figure 1D). Figure 1Significantly increased serum corticosterone levels (A), systolic blood pressure (SBP) (B), abdominal pulse wave velocity (aPWV) (C) and decreased isometric force (D) upon phenylephrine contraction in 6 months old APP23+/− vs. C57BL/6 mice. Figure 2Significant smaller aortic diameter (A) and compliance (B) in baseline Krebs-Ringer solution for APP23+/− mice vs. C57BL/6 mice, without differences in Ep (C). Limited aortic constriction (D), compliance (E) and Ep (F) upon phenylephrine (2 μM) stimulation for APP23+/− mice vs. C57BL/6 mice. Conclusion: APP23+/− mice have increased corticosterone levels leading to increased BP, aPWV and reduced isometric contractility, resulting in decreased isobaric compliance, but with unchanged arterial wall biomechanics.

Published

2020

10. YI 2.2 Spontaneous Cardiovascular Ageing of C57bl6 Mice Results in the Development of Aortic Stiffness Prior to Periphral Blood Pressure Alterations

Author

Sofie De Moudt, Jhana O. Hendrickx, Dorien G. De Munck, Arthur J. Leloup, Wim Martinet, Guido R.Y. De Meyer, and Paul Fransen

Subjects

Arterial stiffness, ageing, aorta, Specialties of internal medicine, RC581-951, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Background: Although generally assumed to be an adaptive response to increased blood pressure (BP), arterial stiffness is now recognized as an independent predictor of cardiovascular (CV) events [1]. Moreover it precedes hypertension in at least two mouse models [2,3]. Therefore, the present study aims to investigate the temporal development of aortic stiffening and peripheral blood pressure (BP) alterations in spontaneously ageing mice. Methods: A longitudinal cardiovascular characterization of spontaneously ageing C57Bl6 mice (2, 4, 6, 9, 12 and 24- month old) (male, n > 8) was performed. This includes in vivo analysis of peripheral BP (Coda) and aortic pulse wave velocity (aPWV, Vevo2100), combined with ex vivo aortic studies of isometric reactivity (organ baths) and aortic stiffness measurements (Peterson modulus, Ep) in the Rodent Oscillatory Tension set-up for Arterial Compliance (ROTSAC). Results: In vivo and ex vivo characterisation confirms that aortic stiffness precedes peripheral BP alterations in spontaneously ageing C57Bl6 mice, with significantly increased aPWV from 6 month of age (Figure A), whereas peripheral BP measurement only shows elevated pulse pressure in 24 month old mice (30% increase vs. all other ages, Figure B). Ex vivo investigation of the thoracic aorta further reveals that the aortic stiffening is both contraction-independent (Figure C) and dependent (Figure D), since older mice display increased contractions to phenylephrine (PE) (Figure E and F). Conclusion: Spontaneously ageing C57Bl6 mice present with significant aortic stiffness by 6-months of age, which is both contraction-dependent and independent in origin. Aortic stiffness thereby precedes the development of peripheral BP alterations by 18 months.

Published

2020

11. Short-Term Pharmacological Induction of Arterial Stiffness and Hypertension with Angiotensin II Does Not Affect Learning and Memory and Cerebral Amyloid Load in Two Murine Models of Alzheimer’s Disease

Author

Jhana O. Hendrickx, Elke Calus, Peter Paul De Deyn, Debby Van Dam, and Guido R. Y. De Meyer

Subjects

arterial stiffness, hypertension, angiotensin II, Alzheimer’s disease, cognition, amyloid, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Given the unprecedented rise in the world’s population, the prevalence of prominent age-related disorders, like cardiovascular disease and dementia, will further increase. Recent experimental and epidemiological evidence suggests a mechanistic overlap between cardiovascular disease and dementia with a specific focus on the linkage between arterial stiffness, a strong independent predictor of cardiovascular disease, and/or hypertension with Alzheimer’s disease. In the present study, we investigated whether pharmacological induction of arterial stiffness and hypertension with angiotensin II (1 µg·kg−1·min−1 for 28 days via an osmotic minipump) impairs the progression of Alzheimer’s disease in two mouse models (hAPP23+/− and hAPPswe/PSEN1dE9 mice). Our results show increased arterial stiffness in vivo and hypertension in addition to cardiac hypertrophy after angiotensin II treatment. However, visuospatial learning and memory and pathological cerebral amyloid load in both Alzheimer’s disease mouse models were not further impaired. It is likely that the 28-day treatment period with angiotensin II was too short to observe additional effects on cognition and cerebral pathology.

Published

2022

12. Long-Term Pharmacological Inhibition of the Activity of All NOS Isoforms Rather Than Genetic Knock-Out of Endothelial NOS Leads to Impaired Spatial Learning and Memory in C57BL/6 Mice

Author

Jhana O. Hendrickx, Sofie De Moudt, Elke Calus, Peter Paul De Deyn, Debby Van Dam, and Guido R. Y. De Meyer

Subjects

arterial stiffness, cognitive decline, nitric oxide synthase, Biology (General), QH301-705.5

Abstract

Increasing epidemiological and experimental evidence points to a link between arterial stiffness and rapid cognitive decline. However, the underlying mechanism linking the two diseases is still unknown. The importance of nitric oxide synthases in both diseases is well-defined. In this study, we introduced arterial stiffness in both genetic (eNOS−/−, endothelial nitric oxide synthase knockout) and pharmacological (N(G)-nitro-L-arginine methyl ester (L-NAME) treatment) NO dysfunction models to study their association with cognitive decline. Our findings demonstrate that the non-selective inhibition of NOS activity with L-NAME induces cardiac dysfunction, arterial stiffness, and a decline in hippocampal-dependent learning and memory. This outcome demonstrates the importance of neuronal NOS (nNOS) in both cardiovascular and neurological pathophysiology and its potential contribution in the convergence between arterial stiffness and cognitive decline.

Published

2021

13. Serum Corticosterone and Insulin Resistance as Early Biomarkers in the hAPP23 Overexpressing Mouse Model of Alzheimer’s Disease

Author

Jhana O. Hendrickx, Sofie De Moudt, Elke Calus, Wim Martinet, Pieter-Jan D. F. Guns, Lynn Roth, Peter P. De Deyn, Debby Van Dam, and Guido R. Y. De Meyer

Subjects

hypercortisolism, insulin resistance, hypermetabolism, cognitive decline, Alzheimer’s disease, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Increasing epidemiological evidence highlights the association between systemic insulin resistance and Alzheimer’s disease (AD). As insulin resistance can be caused by high-stress hormone levels and since hypercortisolism appears to be an important risk factor of AD, we aimed to investigate the systemic insulin functionality and circulating stress hormone levels in a mutant humanized amyloid precursor protein (APP) overexpressing (hAPP23+/−) AD mouse model. Memory and spatial learning of male hAPP23+/− and C57BL/6 (wild type, WT) mice were assessed by a Morris Water Maze (MWM) test at the age of 4 and 12 months. The systemic metabolism was examined by intraperitoneal glucose and insulin tolerance tests (GTT, ITT). Insulin and corticosterone levels were determined in serum. In the hippocampus, parietal and occipital cortex of hAPP23+/− brains, amyloid-beta (Aβ) deposits were present at 12 months of age. MWM demonstrated a cognitive decline in hAPP23+/− mice at 12 but not at 4 months, evidenced by increasing total path lengths and deteriorating probe trials compared to WT mice. hAPP23+/− animals presented increased serum corticosterone levels compared to WT mice at both 4 and 12 months. hAPP23+/− mice exhibited peripheral insulin resistance compared to WT mice at 4 months, which stabilized at 12 months of age. Serum insulin levels were similar between genotypes at 4 months of age but were significantly higher in hAPP23+/− mice at 12 months of age. Peripheral glucose homeostasis remained unchanged. These results indicate that peripheral insulin resistance combined with elevated circulating stress hormone levels could be potential biomarkers of the pre-symptomatic phase of AD.

Published

2021

14. GRK5 – A Functional Bridge Between Cardiovascular and Neurodegenerative Disorders

Author

Jhana O. Hendrickx, Jaana van Gastel, Hanne Leysen, Paula Santos-Otte, Richard T. Premont, Bronwen Martin, and Stuart Maudsley

Subjects

G-protein coupled receptor kinase 5, aging, cardiovascular disease, neurodegeneration, GRK5 interactors, Therapeutics. Pharmacology, RM1-950

Abstract

Complex aging-triggered disorders are multifactorial programs that comprise a myriad of alterations in interconnected protein networks over a broad range of tissues. It is evident that rather than being randomly organized events, pathophysiologies that possess a strong aging component such as cardiovascular diseases (hypertensions, atherosclerosis, and vascular stiffening) and neurodegenerative conditions (dementia, Alzheimer’s disease, mild cognitive impairment, Parkinson’s disease), in essence represent a subtly modified version of the intricate molecular programs already in place for normal aging. To control such multidimensional activities there are layers of trophic protein control across these networks mediated by so-called “keystone” proteins. We propose that these “keystones” coordinate and interconnect multiple signaling pathways to control whole somatic activities such as aging-related disease etiology. Given its ability to control multiple receptor sensitivities and its broad protein-protein interactomic nature, we propose that G protein coupled receptor kinase 5 (GRK5) represents one of these key network controllers. Considerable data has emerged, suggesting that GRK5 acts as a bridging factor, allowing signaling regulation in pathophysiological settings to control the connectivity between both the cardiovascular and neurophysiological complications of aging.

Published

2018

15. The Protective Effects of the Autophagic and Lysosomal Machinery in Vascular and Valvular Calcification: A Systematic Review

Author

Cédric H. G. Neutel, Jhana O. Hendrickx, Wim Martinet, Guido R. Y. De Meyer, and Pieter-Jan Guns

Subjects

vascular calcification, aortic valve calcification, autophagy, lysosomes, vascular smooth muscle cell (VSMC), valvular interstitial cell (VIC), Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Background: Autophagy is a highly conserved catabolic homeostatic process, crucial for cell survival. It has been shown that autophagy can modulate different cardiovascular pathologies, including vascular calcification (VCN). Objective: To assess how modulation of autophagy, either through induction or inhibition, affects vascular and valvular calcification and to determine the therapeutic applicability of inducing autophagy. Data sources: A systematic review of English language articles using MEDLINE/PubMed, Web of Science (WoS) and the Cochrane library. The search terms included autophagy, autolysosome, mitophagy, endoplasmic reticulum (ER)-phagy, lysosomal, calcification and calcinosis. Study characteristics: Thirty-seven articles were selected based on pre-defined eligibility criteria. Thirty-three studies (89%) studied vascular smooth muscle cell (VSMC) calcification of which 27 (82%) studies investigated autophagy and six (18%) studies lysosomal function in VCN. Four studies (11%) studied aortic valve calcification (AVCN). Thirty-four studies were published in the time period 2015–2020 (92%). Conclusion: There is compelling evidence that both autophagy and lysosomal function are critical regulators of VCN, which opens new perspectives for treatment strategies. However, there are still challenges to overcome, such as the development of more selective pharmacological agents and standardization of methods to measure autophagic flux.

Published

2020

16. β-Arrestin Based Receptor Signaling Paradigms: Potential Therapeutic Targets for Complex Age-Related Disorders

Author

Jaana van Gastel, Jhana O. Hendrickx, Hanne Leysen, Paula Santos-Otte, Louis M. Luttrell, Bronwen Martin, and Stuart Maudsley

Subjects

β-arrestin signaling, ligand ‘bias’, GPCRs, age-related disorders, precision, tailored efficacy, Therapeutics. Pharmacology, RM1-950

Abstract

G protein coupled receptors (GPCRs) were first characterized as signal transducers that elicit downstream effects through modulation of guanine (G) nucleotide-binding proteins. The pharmacotherapeutic exploitation of this signaling paradigm has created a drug-based field covering nearly 50% of the current pharmacopeia. Since the groundbreaking discoveries of the late 1990s to the present day, it is now clear however that GPCRs can also generate productive signaling cascades through the modulation of β-arrestin functionality. β-Arrestins were first thought to only regulate receptor desensitization and internalization – exemplified by the action of visual arrestin with respect to rhodopsin desensitization. Nearly 20 years ago, it was found that rather than controlling GPCR signal termination, productive β-arrestin dependent GPCR signaling paradigms were highly dependent on multi-protein complex formation and generated long-lasting cellular effects, in contrast to G protein signaling which is transient and functions through soluble second messenger systems. β-Arrestin signaling was then first shown to activate mitogen activated protein kinase signaling in a G protein-independent manner and eventually initiate protein transcription – thus controlling expression patterns of downstream proteins. While the possibility of developing β-arrestin biased or functionally selective ligands is now being investigated, no additional research has been performed on its possible contextual specificity in treating age-related disorders. The ability of β-arrestin-dependent signaling to control complex and multidimensional protein expression patterns makes this therapeutic strategy feasible, as treating complex age-related disorders will likely require therapeutics that can exert network-level efficacy profiles. It is our understanding that therapeutically targeting G protein-independent effectors such as β-arrestin will aid in the development of precision medicines with tailored efficacy profiles for disease/age-specific contextualities.

Published

2018

17. Sclerostin as Regulatory Molecule in Vascular Media Calcification and the Bone–Vascular Axis

Author

Annelies De Maré, Stuart Maudsley, Abdelkrim Azmi, Jhana O. Hendrickx, Britt Opdebeeck, Ellen Neven, Patrick C D’Haese, and Anja Verhulst

Subjects

chronic kidney disease, vascular calcification, bone disease, mineral abnormalities, rat model, Medicine

Abstract

Sclerostin is a well-known inhibitor of bone formation that acts on Wnt/β-catenin signaling. This manuscript considers the possible role of sclerostin in vascular calcification, a process that shares many similarities with physiological bone formation. Rats were exposed to a warfarin-containing diet to induce vascular calcification. Vascular smooth muscle cell transdifferentiation, vascular calcification grade, and bone histomorphometry were examined. The presence and/or production of sclerostin was investigated in serum, aorta, and bone. Calcified human aortas were investigated to substantiate clinical relevance. Warfarin-exposed rats developed vascular calcifications in a time-dependent manner which went along with a progressive increase in serum sclerostin levels. Both osteogenic and adipogenic pathways were upregulated in calcifying vascular smooth muscle cells, as well as sclerostin mRNA and protein levels. Evidence for the local vascular action of sclerostin was found both in human and rat calcified aortas. Warfarin exposure led to a mildly decreased bone and mineralized areas. Osseous sclerostin production and bone turnover did not change significantly. This study showed local production of sclerostin in calcified vessels, which may indicate a negative feedback mechanism to prevent further calcification. Furthermore, increased levels of serum sclerostin, probably originating from excessive local production in calcified vessels, may contribute to the linkage between vascular pathology and impaired bone mineralization.

Published

2019

18. G Protein-Coupled Receptor Systems as Crucial Regulators of DNA Damage Response Processes

Author

Hanne Leysen, Jaana van Gastel, Jhana O. Hendrickx, Paula Santos-Otte, Bronwen Martin, and Stuart Maudsley

Subjects

G protein-coupled receptor (GPCR), aging, DNA damage, β-arrestin, G protein-coupled receptor kinase (GRK), interactome, G protein-coupled receptor kinase interacting protein 2 (GIT2), ataxia telangiectasia mutated (ATM), clock proteins, energy metabolism, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

G protein-coupled receptors (GPCRs) and their associated proteins represent one of the most diverse cellular signaling systems involved in both physiological and pathophysiological processes. Aging represents perhaps the most complex biological process in humans and involves a progressive degradation of systemic integrity and physiological resilience. This is in part mediated by age-related aberrations in energy metabolism, mitochondrial function, protein folding and sorting, inflammatory activity and genomic stability. Indeed, an increased rate of unrepaired DNA damage is considered to be one of the ‘hallmarks’ of aging. Over the last two decades our appreciation of the complexity of GPCR signaling systems has expanded their functional signaling repertoire. One such example of this is the incipient role of GPCRs and GPCR-interacting proteins in DNA damage and repair mechanisms. Emerging data now suggest that GPCRs could function as stress sensors for intracellular damage, e.g., oxidative stress. Given this role of GPCRs in the DNA damage response process, coupled to the effective history of drug targeting of these receptors, this suggests that one important future activity of GPCR therapeutics is the rational control of DNA damage repair systems.

Published

2018

19. UAS™—A Urine Preservative for Oncology Applications

Author

Vankerckhoven, Stephanie Jordaens, Amit Arora, Kyle W. MacDonald, Cameron Wood, Jhana O. Hendrickx, Karen Zwaenepoel, Christophe Deben, Wiebren Tjalma, Patrick Pauwels, Koen Beyers, and Vanessa

Subjects

oncology, liquid biopsy, first-void urine, urine collection, urine preservation, cancer, carcinoma, detection, screening, secondary prevention, treatment, response, breast, prostate, pregnancy

Abstract

Liquid biopsy is a revolutionary tool that is gaining momentum in the field of cancer research. As a body fluid, urine can be used in non-invasive diagnostics for various types of cancer. We investigated the performance of UAS™ as a preservative for urinary analytes. Firstly, the need for urine preservation was investigated using urine samples from healthy volunteers. Secondly, the performance of UAS™ was assessed for cell-free DNA (cfDNA) and host cell integrity during storage at room temperature (RT) and after freeze-thaw cycling. Finally, UAS™ was used in a clinical setting on samples from breast and prostate cancer patients. In the absence of a preservative, urinary cfDNA was degraded, and bacterial overgrowth occurred at RT. In urine samples stored in UAS™, no microbial growth was seen, and cfDNA and cellular integrity were maintained for up to 14 days at RT. After freeze-thaw cycling, the preservation of host cell integrity and cfDNA showed significant improvements when using UAS™ compared to unpreserved urine samples. Additionally, UAS™ was found to be compatible with several commercially available isolation methods.

Published

2023

20. Neuregulin-1 compensates for endothelial nitric oxide synthase deficiency

Author

Vincent F.M. Segers, Jhana O. Hendrickx, Hadis Shakeri, Jente R A Boen, Sofie De Moudt, Arthur J. A. Leloup, Pieter-Jan Guns, Griet Jacobs, Guido R.Y. De Meyer, and Gilles W. De Keulenaer

Subjects

medicine.medical_specialty, Endothelial nitric oxide synthase, biology, Physiology, business.industry, Renal Hypertrophy, medicine.disease, biology.organism_classification, Angiotensin II, Muscle hypertrophy, Endocrinology, Fibrosis, Enos, Physiology (medical), Internal medicine, mental disorders, medicine, biology.protein, Secretion, Human medicine, Neuregulin 1, Cardiology and Cardiovascular Medicine, business

Abstract

Endothelial cells (ECs) secrete different paracrine signals that modulate the function of adjacent cells; two examples of these paracrine signals are nitric oxide (NO) and neuregulin-1 (NRG1), a cardioprotective growth factor. Currently, it is undetermined whether one paracrine factor can compensate for the loss of another. Herein, we hypothesized that NRG1 can compensate for endothelial NO synthase (eNOS) deficiency. We characterized eNOS null and wild-type (WT) mice by cardiac ultrasound and histology and we determined circulating NRG1 levels. In a separate experiment, eight groups of mice were divided into four groups of eNOS null mice and WT mice; half of the mice received angiotensin II (ANG II) to induce a more severe phenotype. Mice were randomized to daily injections with NRG1 or vehicle for 28 days. eNOS deficiency increased NRG1 plasma levels, indicating that ECs increase their NRG1 expression when NO production is deleted. eNOS deficiency also increased blood pressure, lowered heart rate, induced cardiac fibrosis, and affected diastolic function. In eNOS null mice, ANG II administration not only increased cardiac fibrosis but also induced cardiac hypertrophy and renal fibrosis. NRG1 administration prevented cardiac and renal hypertrophy and fibrosis caused by ANG II infusion and eNOS deficiency. Moreover, Nrg1 expression in the myocardium is shown to be regulated by miR-134. This study indicates that administration of endothelium-derived NRG1 can compensate for eNOS deficiency in the heart and kidneys. NEW & NOTEWORTHY ECs compensate for eNOS deficiency by increasing the secretion of NRG1. NRG1 administration prevents cardiac and renal hypertrophy and fibrosis caused by ANG II infusion and eNOS deficiency. NRG1 expression is regulated by miR-134.

Published

2021

21. The RXFP3 receptor is functionally associated with cellular responses to oxidative stress and DNA damage

Author

Hanne Leysen, Stuart Maudsley, Jaana van Gastel, Paula Santos-Otte, Jhana O. Hendrickx, Abdelkrim Azmi, and Bronwen Martin

Subjects

Aging, DNA damage, medicine.disease_cause, Receptors, G-Protein-Coupled, GPCR, medicine, Humans, Gene Regulatory Networks, RNA, Messenger, Receptor, Biology, G protein-coupled receptor, Relaxin, Felodipine, Chemistry, GTPase-Activating Proteins, relaxin 3, Computational Biology, Cell Biology, Cell biology, Oxidative Stress, HEK293 Cells, Gene Expression Regulation, Phosphorylation, Camptothecin, Human medicine, Topoisomerase I Inhibitors, relaxin family peptide 3 receptor, Relaxin-3, Oxidative stress, Research Paper, medicine.drug

Abstract

DNA damage response (DDR) processes, often caused by oxidative stress, are important in aging and -related disorders. We recently showed that G protein-coupled receptor (GPCR) kinase interacting protein 2 (GIT2) plays a key role in both DNA damage and oxidative stress. Multiple tissue analyses in GIT2KO mice demonstrated that GIT2 expression affects the GPCR relaxin family peptide 3 receptor (RXFP3), and is thus a therapeutically-targetable system. RXFP3 and GIT2 play similar roles in metabolic aging processes. Gaining a detailed understanding of the RXFP3-GIT2 functional relationship could aid the development of novel anti-aging therapies. We determined the connection between RXFP3 and GIT2 by investigating the role of RXFP3 in oxidative stress and DDR. Analyzing the effects of oxidizing (H2O2) and DNA-damaging (camptothecin) stressors on the interacting partners of RXFP3 using Affinity Purification-Mass Spectrometry, we found multiple proteins linked to DDR and cell cycle control. RXFP3 expression increased in response to DNA damage, overexpression, and Relaxin 3-mediated stimulation of RXFP3 reduced phosphorylation of DNA damage marker H2AX, and repair protein BRCA1, moderating DNA damage. Our data suggests an RXFP3-GIT2 system that could regulate cellular degradation after DNA damage, and could be a novel mechanism for mitigating the rate of age-related damage accumulation.

Published

2019

22. Altered stress hormone levels affect in vivo vascular function in the hAPP23(+/-) overexpressing mouse model of Alzheimer's disease

Author

Guido R.Y. De Meyer, Jhana O. Hendrickx, Peter Paul De Deyn, Paul Fransen, Sofie De Moudt, Debby Van Dam, and Molecular Neuroscience and Ageing Research (MOLAR)

Subjects

Genetically modified mouse, medicine.medical_specialty, Physiology, BLOOD-PRESSURE VARIABILITY, PROTEIN, Disease, amyloid precursor protein, Affect (psychology), alpha-adrenergic receptor-dependent contraction, AGE, In vivo, DEFICITS, Physiology (medical), Internal medicine, Amyloid precursor protein, medicine, Pulse wave velocity, ANTIHYPERTENSIVE DRUG-THERAPY, biology, hypercortisolism, Chemistry, AMYLOID-BETA, Stress hormone, CORTICOTROPIN-RELEASING-FACTOR, MICE, Endocrinology, Blood pressure, pulse-wave velocity, stress hormone, biology.protein, Human medicine, Cardiology and Cardiovascular Medicine, ARTERIAL STIFFNESS

Abstract

Alzheimer's disease (AD) has long been considered a brain-specific dementia syndrome. However, in recent decades, the occurrence of cardiovascular (CV) disease in the progression of AD has been confirmed by increasing epidemiological evidence. In this study, we conducted an in-depth cardiovascular characterization of a humanized amyloid precursor protein (APP) overexpressing mouse model (hAPP23(+/-)), which overexpresses the Swedish mutation (KM670/671NL). At the age of 6 mo, hAPP23(+/-) mice had a lower survival, lower body weight, and increased corticosterone and VMA levels compared with C57BL/6 littermates. Systolic blood pressure was increased in hAPP23(+/-) animals compared with C57BU6 littermates, but diastolic blood pressure was not statistically different. Pulse pressure remained unchanged but abdominal and carotid pulse-wave velocity (aPWV and cPWV) were increased in hAPP23(+/-) compared with C57BL/6 mice. Echocardiography showed no differences in systolic or diastolic cardiac function. Ex vivo evaluation of vascular function showed decreased adreno receptor dependent vasoconstriction of hAPP23(+/-) aortic segments, although the isobaric biomechanics of the aortic wall were similar to C57BL/6 aortic segments. In conclusion, hAPP23(+/-) mice exhibited high serum corticosterone levels, elevated systolic blood pressure, and increased arterial stiffness in vivo. However, ex vivo aortic stiffness of hAPP23(+/-) aortic segments was not changed and vascular reactivity to alpha(1)-drenoceptor stimulation was attenuated. These findings highlight the need for more frequent assessment of circulating stress hormone levels and PWV measurements in daily clinical practice for people at risk of AD.NEW & NOTEWORTHY We showed that male amyloid precursor protein (APP) transgenic mice have higher circulating stress hormone levels. As a result, higher systolic blood pressure and pulse-wave velocity were measured in vivo in addition to a smaller alpha-adrenergic receptor-dependent contraction upon ex vivo stimulation with phenylephrine. Our findings highlight the need for more frequent assessment of circulating stress hormone levels and PWV measurements in daily clinical practice for people at risk of Alzheimer's disease.

Published

2021

23. Altered stress hormone levels affect in vivo vascular function in the hAPP23

Author

Jhana O, Hendrickx, Sofie, De Moudt, Debby, Van Dam, Peter Paul, De Deyn, Paul, Fransen, and Guido R Y, De Meyer

Subjects

Male, Aorta, Thoracic, Mice, Transgenic, Up-Regulation, Mice, Inbred C57BL, Amyloid beta-Protein Precursor, Disease Models, Animal, Vascular Stiffness, Alzheimer Disease, Vasoconstriction, Receptors, Adrenergic, alpha-1, Mutation, Animals, Arterial Pressure, Adrenergic alpha-1 Receptor Agonists, Corticosterone

Abstract

Alzheimer's disease (AD) has long been considered a brain-specific dementia syndrome. However, in recent decades, the occurrence of cardiovascular (CV) disease in the progression of AD has been confirmed by increasing epidemiological evidence. In this study, we conducted an in-depth cardiovascular characterization of a humanized amyloid precursor protein (APP) overexpressing mouse model (hAPP23

Published

2021

24. Age-related cognitive decline in spatial learning and memory of C57BL/6J mice

Author

Guido R.Y. De Meyer, Peter Paul De Deyn, Sofie De Moudt, Elke Calus, Debby Van Dam, Jhana O. Hendrickx, and Molecular Neuroscience and Ageing Research (MOLAR)

Subjects

Male, Aging, Novel object recognition, Spatial Learning, Morris water navigation task, C57bl 6j, Hippocampus, Behavioral Neuroscience, Mice, MOUSE MODELS, Memory, Morris Water Maze Test, Medicine, Dementia, 6J, Psychology, Animals, Cognitive Dysfunction, Cognitive decline, Pathological, Biology, business.industry, Cognition, Spontaneous cognitive decline, medicine.disease, Mice, Inbred C57BL, C57BL, Disease Models, Animal, Spatial learning, Human medicine, business, Neuroscience, Morris water maze, Open Field Test

Abstract

During the last decades, most of the preclinical neurodegenerative research was performed in mouse models of amyloidosis, tauopathies or alpha-synucleinopathies preferentially maintained on a C57BL/6J background. However, comprehensive neurobehavioural data from C57BL/6J mice outlining the critical point of spontaneous cognitive decline are incomplete. In this study, we aimed for the neurobehavioural phenotyping of hippocampusdependent spatial learning and memory of aging C57BL/6J mice. Neurobehavioural phenotyping was performed by means of a Morris Water Maze (MWM) and a Novel Object Recognition (NOR) test. MWM measurements revealed signs of age-related memory loss in C57BL/6J animals from the age of 6 months onward. The NOR assessment strengthened latter finding by decreasing discrimination indexes (DI) and recognition indexes (RI) starting from the age of 6 months. Taken together, these findings contribute to the current knowledge of spontaneous cognitive behaviours of this perhaps most widely used mouse strain and serve as a benchmark for dementia mouse models to distinguish spontaneous from pathological neurodegenerative behaviour.

Published

2021

25. G Protein-Coupled Receptor Systems and Their Role in Cellular Senescence

Author

Hanne Leysen, Jhana O. Hendrickx, Paula Santos-Otte, Stuart Maudsley, Jaana van Gastel, and Bronwen Martin

Subjects

Aging, Review Article, Disease, Aging disorders, Biochemistry, vascular smooth muscle cells, (VSMC), cyclin-dependent kinase inhibitor 1, (cdkn1A/p21), 0302 clinical medicine, Structural Biology, Hutchinson–Gilford progeria syndrome, (HGPS), purinergic receptors family, (P2Y), protein kinases, (PK), beta2-adrenergic receptor, (β2AR), Receptor, endothelial cell differentiation gene, (Edg), nuclear factor kappa-light-chain-enhancer of activated B cells, (NF- κβ), senescence associated secretory phenotype, (SASP), 0303 health sciences, Relaxin family receptor 3, (RXFP3), tumor suppressor gene PTEN, (PTEN), transcription factor E2F3, (E2F3), Computer Science Applications, Cell biology, retinoblastoma, (RB), Chemistry, 030220 oncology & carcinogenesis, G protein-coupled receptor kinase, (GRK), latent semantic indexing, (LSI), Lysophosphatidic acid, (LPA), G protein-coupled receptors (GPCRs), G protein-coupled receptor kinase interacting protein 2 (GIT2), mitogen-activated protein kinase, (MAPK), Regulator of G-protein signaling, (RGS), Engineering sciences. Technology, AT1R blockers, (ARB), Biotechnology, Cell signaling, lcsh:Biotechnology, renin-angiotensin system, (RAS), Biophysics, Cellular senescence, tumor suppressor protein 53, (p53), Biology, 03 medical and health sciences, Cell surface receptor, lcsh:TP248.13-248.65, angiotensin type 2 receptor, (AT2R), Genetics, G protein-coupled receptor kinase interacting protein 2, (GIT2), Ataxia telangiectasia mutated, (ATM), Angiotensin II, (Ang II), 030304 developmental biology, G protein-coupled receptor, inactive state, (R), angiotensin type 1 receptor, (AT1R), G protein-coupled receptors, (GPCRs), β-Arrestin, ADP-ribosylation factor GTPase-activating protein, (Arf-GAP), cyclin-dependent kinase 2, (CDK2), Apoptosis, transmembrane, (TM), stress-induced premature senescence, (SIPS), active state, (R*)

Abstract

Aging is a complex biological process that is inevitable for nearly all organisms. Aging is the strongest risk factor for development of multiple neurodegenerative disorders, cancer and cardiovascular disorders. Age-related disease conditions are mainly caused by the progressive degradation of the integrity of communication systems within and between organs. This is in part mediated by, i) decreased efficiency of receptor signaling systems and ii) an increasing inability to cope with stress leading to apoptosis and cellular senescence. Cellular senescence is a natural process during embryonic development, more recently it has been shown to be also involved in the development of aging disorders and is now considered one of the major hallmarks of aging. G-protein-coupled receptors (GPCRs) comprise a superfamily of integral membrane receptors that are responsible for cell signaling events involved in nearly every physiological process. Recent advances in the molecular understanding of GPCR signaling complexity have expanded their therapeutic capacity tremendously. Emerging data now suggests the involvement of GPCRs and their associated proteins in the development of cellular senescence. With the proven efficacy of therapeutic GPCR targeting, it is reasonable to now consider GPCRs as potential platforms to control cellular senescence and the consequently, age-related disorders., Graphical Abstract Unlabelled Image

Published

2019

26. Serum Corticosterone and Insulin Resistance as Early Biomarkers in the hAPP23 Overexpressing Mouse Model of Alzheimer's Disease

Author

Guido R.Y. De Meyer, Jhana O. Hendrickx, Debby Van Dam, Peter Paul De Deyn, Lynn Roth, Sofie De Moudt, Wim Martinet, Pieter-Jan Guns, Elke Calus, and Molecular Neuroscience and Ageing Research (MOLAR)

Subjects

0301 basic medicine, Male, medicine.medical_treatment, Morris water navigation task, chemistry.chemical_compound, Amyloid beta-Protein Precursor, Mice, 0302 clinical medicine, Corticosterone, insulin resistance, hypermetabolism, Medicine, Glucose homeostasis, Insulin, Biology (General), Cognitive decline, BRAIN, Cushing Syndrome, Spectroscopy, RISK, DEMENTIA, General Medicine, Alzheimer's disease, Computer Science Applications, Chemistry, Hypermetabolism, CUSHINGS-SYNDROME, Alzheimer’s disease, APP23, medicine.medical_specialty, AMYLOID-PRECURSOR-PROTEIN, QH301-705.5, Mice, Transgenic, Catalysis, Article, Inorganic Chemistry, 03 medical and health sciences, Insulin resistance, Alzheimer Disease, Internal medicine, Animals, Cognitive Dysfunction, Physical and Theoretical Chemistry, QD1-999, Biology, Molecular Biology, hypercortisolism, business.industry, CORTISOL, Organic Chemistry, medicine.disease, COGNITIVE IMPAIRMENT, cognitive decline, DYSFUNCTION, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Endocrinology, chemistry, A-BETA-DEPOSITION, Human medicine, business, 030217 neurology & neurosurgery, Biomarkers, Hormone

Abstract

Increasing epidemiological evidence highlights the association between systemic insulin resistance and Alzheimer’s disease (AD). As insulin resistance can be caused by high-stress hormone levels and since hypercortisolism appears to be an important risk factor of AD, we aimed to investigate the systemic insulin functionality and circulating stress hormone levels in a mutant humanized amyloid precursor protein (APP) overexpressing (hAPP23+/−) AD mouse model. Memory and spatial learning of male hAPP23+/− and C57BL/6 (wild type, WT) mice were assessed by a Morris Water Maze (MWM) test at the age of 4 and 12 months. The systemic metabolism was examined by intraperitoneal glucose and insulin tolerance tests (GTT, ITT). Insulin and corticosterone levels were determined in serum. In the hippocampus, parietal and occipital cortex of hAPP23+/− brains, amyloid-beta (Aβ) deposits were present at 12 months of age. MWM demonstrated a cognitive decline in hAPP23+/− mice at 12 but not at 4 months, evidenced by increasing total path lengths and deteriorating probe trials compared to WT mice. hAPP23+/− animals presented increased serum corticosterone levels compared to WT mice at both 4 and 12 months. hAPP23+/− mice exhibited peripheral insulin resistance compared to WT mice at 4 months, which stabilized at 12 months of age. Serum insulin levels were similar between genotypes at 4 months of age but were significantly higher in hAPP23+/− mice at 12 months of age. Peripheral glucose homeostasis remained unchanged. These results indicate that peripheral insulin resistance combined with elevated circulating stress hormone levels could be potential biomarkers of the pre-symptomatic phase of AD.

Published

2021

27. Inflammation, Nitro-Oxidative Stress, Impaired Autophagy, and Insulin Resistance as a Mechanistic Convergence Between Arterial Stiffness and Alzheimer’s Disease

Author

Guido R.Y. De Meyer, Jhana O. Hendrickx, Wim Martinet, and Debby Van Dam

Subjects

0301 basic medicine, autophagy, Inflammation, Review, Disease, Bioinformatics, medicine.disease_cause, Biochemistry, Genetics and Molecular Biology (miscellaneous), Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Insulin resistance, medicine, Molecular Biosciences, Risk factor, Molecular Biology, Biology, lcsh:QH301-705.5, business.industry, Neurodegeneration, Autophagy, neurodegeneration, medicine.disease, Chemistry, 030104 developmental biology, arterial stiffness, lcsh:Biology (General), Arterial stiffness, inflammaging, Human medicine, medicine.symptom, nitro-oxidative stress, business, metabolism, 030217 neurology & neurosurgery, Oxidative stress

Abstract

The average age of the world’s elderly population is steadily increasing. This unprecedented rise in the aged world population will increase the prevalence of age-related disorders such as cardiovascular disease (CVD) and neurodegeneration. In recent years, there has been an increased interest in the potential interplay between CVDs and neurodegenerative syndromes, as several vascular risk factors have been associated with Alzheimer’s disease (AD). Along these lines, arterial stiffness is an independent risk factor for both CVD and AD. In this review, we discuss several inflammaging-related disease mechanisms including acute tissue-specific inflammation, nitro-oxidative stress, impaired autophagy, and insulin resistance which may contribute to the proposed synergism between arterial stiffness and AD.

Published

2021

28. YI 2.2 Spontaneous Cardiovascular Ageing of C57bl6 Mice Results in the Development of Aortic Stiffness Prior to Periphral Blood Pressure Alterations

Author

Paul Fransen, Guido R.Y. De Meyer, Sofie De Moudt, Arthur J. A. Leloup, Wim Martinet, Dorien G. De Munck, and Jhana O. Hendrickx

Subjects

Aorta, medicine.medical_specialty, business.industry, Specialties of internal medicine, General Medicine, medicine.disease, Arterial stiffness, aorta, Blood pressure, RC581-951, Ageing, ageing, medicine.artery, Internal medicine, RC666-701, Cardiology, Medicine, Diseases of the circulatory (Cardiovascular) system, Aortic stiffness, business

Abstract

Background: Although generally assumed to be an adaptive response to increased blood pressure (BP), arterial stiffness is now recognized as an independent predictor of cardiovascular (CV) events [1]. Moreover it precedes hypertension in at least two mouse models [2,3]. Therefore, the present study aims to investigate the temporal development of aortic stiffening and peripheral blood pressure (BP) alterations in spontaneously ageing mice. Methods: A longitudinal cardiovascular characterization of spontaneously ageing C57Bl6 mice (2, 4, 6, 9, 12 and 24- month old) (male, n > 8) was performed. This includes in vivo analysis of peripheral BP (Coda) and aortic pulse wave velocity (aPWV, Vevo2100), combined with ex vivo aortic studies of isometric reactivity (organ baths) and aortic stiffness measurements (Peterson modulus, Ep) in the Rodent Oscillatory Tension set-up for Arterial Compliance (ROTSAC). Results: In vivo and ex vivo characterisation confirms that aortic stiffness precedes peripheral BP alterations in spontaneously ageing C57Bl6 mice, with significantly increased aPWV from 6 month of age (Figure A), whereas peripheral BP measurement only shows elevated pulse pressure in 24 month old mice (30% increase vs. all other ages, Figure B). Ex vivo investigation of the thoracic aorta further reveals that the aortic stiffening is both contraction-independent (Figure C) and dependent (Figure D), since older mice display increased contractions to phenylephrine (PE) (Figure E and F). Conclusion: Spontaneously ageing C57Bl6 mice present with significant aortic stiffness by 6-months of age, which is both contraction-dependent and independent in origin. Aortic stiffness thereby precedes the development of peripheral BP alterations by 18 months.

Published

2020

29. Abstract 15505: Aortic Stiffening in L-NAME Treated C57bl6 Mice Precedes Peripheral Hypertension and Cardiac Hypertrophy: Early Endothelial Dysfunction Shifts to Late-term Vascular Smooth Muscle Cell Disease

Author

Guido R.Y. De Meyer, Jhana O. Hendrickx, Sofie De Moudt, Arthur J. A. Leloup, Dorien G. De Munck, Wim Martinet, and Paul Fransen

Subjects

Aorta, medicine.medical_specialty, Vascular smooth muscle, business.industry, Disease, medicine.disease, Peripheral, Nitric oxide, chemistry.chemical_compound, Blood pressure, chemistry, Ageing, Physiology (medical), medicine.artery, Internal medicine, medicine, Cardiology, Endothelial dysfunction, Cardiology and Cardiovascular Medicine, business

Abstract

Introduction: Endothelial dysfunction (ED) acts as a common player in most cardiovascular (CV) risk factors (e.g. hypertension, smoking) underlining its importance in CV ageing. Therefore, this study aims to characterize ex vivo aortic function changes in Nω-Nitro-L-arginine methyl ester hydrochloride (L-NAME) treated mice. Methods: C57Bl6 mice (male, n=10) received 0.5 mg/mL L-NAME through the drinking water for 1, 2, 4, 8, and 16 weeks, followed by in-depth ex vivo thoracic aorta isometric reactivity studies and arterial stiffness (Peterson modulus, Ep) measurements in the Rodent Oscillatory Tension set-up for Arterial Compliance (ROTSAC). In addition, peripheral blood pressure (BP, Coda), aortic pulse wave velocity (aPWV, Vevo2100), and echocardiography (Vevo2100) were measured in vivo . (Data are represented as mean±SEM) Results: L-NAME treated mice display fast-onset aortic stiffening after 1-week L-NAME (Fig. A, B), followed by the development of peripheral hypertension (Fig. C) and cardiac disease (Fig. D-F) after 4-weeks L-NAME. Ex vivo aorta studies reveal different stages of disease. Early on (1-4 weeks), mice show elevated phenylephrine (PE) contractions (Fig. G) and impaired acetylcholine (ACh) relaxations (Fig. H), consistent with L-NAME related ED. After 8 weeks, endothelial function and PE contractions normalize. Relaxations to exogenous NO remain unaltered (Fig. I). In contrast to the recovery of ACh relaxations, stiffness analysis in the ROTSAC reveals constantly reduced basal NO levels (Fig. J), and a late-term shift (16 weeks) towards vascular smooth muscle cell (VSMC) disease. This involves basal cytoplasmic calcium loading (Fig. K) and a sharply increasing contribution of voltage-gated calcium channels (Fig. L). Conclusions: NOS inhibition by L-NAME treatment causes a distinct time-dependent aortic disease phenotype, underlying fast-onset arterial stiffening which precedes peripheral hypertension and cardiac disease.

Published

2020

30. Abstract 15515: Cardiovascular Phenotyping of the APP23 Overexpressing Mouse Model of Alzheimer’s Disease Reveals Decreased Vascular Contractility

Author

Jhana O. Hendrickx, Guido R.Y. De Meyer, Paul Fransen, Debby Van Dam, and Sofie De Moudt

Subjects

Vascular contractility, medicine.medical_specialty, business.industry, Disease, medicine.disease, Contractility, Physiology (medical), Internal medicine, Epidemiology, Cardiology, Medicine, Dementia, Cognitive decline, Cardiology and Cardiovascular Medicine, business

Abstract

Background and Aim: Alzheimer’s disease (AD), the most common form of dementia, is characterized by noticeable neuropsychiatric symptoms and cognitive decline. Increasing epidemiological and experimental evidence highlights the occurrence of cardiovascular (CV) disease in the progression of AD. Therefore, we aimed to investigate the cardiovascular phenotype of the APP23 +/- overexpressing mouse model (APP23 +/- ). Methods: The current study presents the CV characterization of APP23 +/- mice (male, n=10) compared to C57BL/6 (male, n=24) at 6 months of age, including in vivo analysis of blood pressure (BP, CODA), aortic pulse wave velocity (aPWV), and echocardiography (high-frequency echocardiography, VEVO2100). Serum corticosterone levels and vascular smooth muscle cell (VSMC) phenotypic markers were ascertained via ELISA and qPCR. Data are presented as mean ± SEM. Results: At 6 month of age, APP23 +/- mice experience a lower survival rate compared to C57BL/6 littermates (39% vs. 100%, p=0.001) and APP23 +/- mice showed increased corticosterone levels compared to C57BL/6 mice (13.39 ± 5.15 vs. 2.30 ± 2.52 μg/mL, p=0.0025). Peripheral BP was increased (systolic BP: 110 ± 5 vs. 99 ± 3 mmHg, p=0.045; diastolic BP: 81 ± 5 vs. 71 ± 3 mmHg, p=0.09) with unaltered pulse pressure. Echocardiography revealed no differences in systolic and diastolic heart function. In vivo arterial stiffness was elevated in APP23 +/- mice (aPWV: 4.08 ± 0.3 vs. 2.94 ± 0.1 m/s, p=0.0004). Vascular reactivity studies showed decreased (32 %) adrenoreceptor-dependent contractions of the thoracic aorta from APP23 +/- mice. Endothelial-dependent (acetylcholine) and -independent (diethylamine nonoate) relaxations were unaffected. Contractile VSMC markers remained unchanged. Conclusion: In conclusion, APP23 +/- mice present with high serum corticosterone levels, elevated pulse wave velocity and decreased vascular contractility.

Published

2020

31. High-dimensionality Data Analysis of Pharmacological Systems Associated with Complex Diseases

Author

Bronwen Martin, Hanne Leysen, Jhana O. Hendrickx, Stuart Maudsley, and Jaana van Gastel

Subjects

0301 basic medicine, Computer science, Process (engineering), Disease, Computational biology, 03 medical and health sciences, 0302 clinical medicine, Metabolomics, Animals, Humans, Repurposing, Metabolic Syndrome, Pharmacology, Principal Component Analysis, Mechanism (biology), Data stream mining, business.industry, Pharmacology. Therapy, Computational Biology, Neurodegenerative Diseases, 030104 developmental biology, Analytics, Cardiovascular Diseases, Informatics, Data Interpretation, Statistical, Molecular Medicine, business, 030217 neurology & neurosurgery

Abstract

It is widely accepted that molecular reductionist views of highly complex human physiologic activity, e.g., the aging process, as well as therapeutic drug efficacy are largely oversimplifications. Currently some of the most effective appreciation of biologic disease and drug response complexity is achieved using high-dimensionality (H-D) data streams from transcriptomic, proteomic, metabolomics, or epigenomic pipelines. Multiple H-D data sets are now common and freely accessible for complex diseases such asmetabolic syndrome, cardiovascular disease, and neurodegenerative conditions such as Alzheimer's disease. Over the last decade our ability to interrogate these high-dimensionality data streams has been profoundly enhanced through the development and implementation of highly effective bioinformatic platforms. Employing these computational approaches to understand the complexity of age-related diseases provides a facile mechanism to then synergize this pathologic appreciation with a similar level of understanding of therapeutic-mediated signaling. For informative pathology and drug-based analytics that are able to generate meaningful therapeutic insight across diverse data streams, novel informatics processes such as latent semantic indexing and topological data analyses will likely be important. Elucidation of H-D molecular disease signatures from diverse data streams will likely generate and refine new therapeutic strategies that will be designed with a cognizance of a realistic appreciation of the complexity of human age-related disease and drug effects. We contend that informatic platforms should be synergistic with more advanced chemical/drug and phenotypic cellular/tissue-based analytical predictive models to assist in either de novo drug prioritization or effective repurposing for the intervention of aging-related diseases. Significance Statement-All diseases, as well as pharmacological mechanisms, are far more complex than previously thought a decade ago. With the advent of commonplace access to technologies that produce large volumes of high-dimensionality data (e.g., transcriptomics, proteomics, metabolomics), it is now imperative that effective tools to appreciate this highly nuanced data are developed. Being able to appreciate the subtleties of high-dimensionality data will allow molecular pharmacologists to develop the most effective multidimensional therapeutics with effectively engineered efficacy profiles.

Published

2019

32. Enhanced Molecular Appreciation of Psychiatric Disorders Through High-Dimensionality Data Acquisition and Analytics

Author

Jaana, van Gastel, Jhana O, Hendrickx, Hanne, Leysen, Bronwen, Martin, Len, Veenker, Sophie, Beuning, Violette, Coppens, Manuel, Morrens, and Stuart, Maudsley

Subjects

Proteomics, Phenotype, Proteome, Data Interpretation, Statistical, Gene Expression Profiling, Mental Disorders, Animals, Computational Biology, Humans, Metabolomics, Disease Susceptibility, Transcriptome, Biomarkers

Abstract

The initial diagnosis, molecular investigation, treatment, and posttreatment care of major psychiatric disorders (schizophrenia and bipolar depression) are all still significantly hindered by the current inability to define these disorders in an explicit molecular signaling manner. High-dimensionality data analytics, using large datastreams from transcriptomic, proteomic, or metabolomic investigations, will likely advance both the appreciation of the molecular nature of major psychiatric disorders and simultaneously enhance our ability to more efficiently diagnose and treat these debilitating conditions. High-dimensionality data analysis in psychiatric research has been heterogeneous in aims and methods and limited by insufficient sample sizes, poorly defined case definitions, methodological inhomogeneity, and confounding results. All of these issues combine to constrain the conclusions that can be extracted from them. Here, we discuss possibilities for overcoming methodological challenges through the implementation of transcriptomic, proteomic, or metabolomics signatures in psychiatric diagnosis and offer an outlook for future investigations. To fulfill the promise of intelligent high-dimensionality data-based differential diagnosis in mental disease diagnosis and treatment, future research will need large, well-defined cohorts in combination with state-of-the-art technologies.

Published

2019

33. Sclerostin as Regulatory Molecule in Vascular Media Calcification and the Bone–Vascular Axis

Author

Anja Verhulst, Patrick C. D'Haese, Jhana O. Hendrickx, Annelies De Maré, Britt Opdebeeck, Ellen Neven, Abdelkrim Azmi, and Stuart Maudsley

Subjects

Male, Vascular smooth muscle, Bone disease, Health, Toxicology and Mutagenesis, lcsh:Medicine, 030204 cardiovascular system & hematology, Toxicology, Bone remodeling, chemistry.chemical_compound, 0302 clinical medicine, Osteogenesis, 0303 health sciences, Adipogenesis, Pharmacology. Therapy, Wnt signaling pathway, mineral abnormalities, Cell Differentiation, Arteries, vascular calcification, Bone Morphogenetic Proteins, Genetic Markers, medicine.medical_specialty, education, Myocytes, Smooth Muscle, Bone and Bones, Article, 03 medical and health sciences, Downregulation and upregulation, Internal medicine, medicine, Animals, Humans, RNA, Messenger, Rats, Wistar, Biology, Adaptor Proteins, Signal Transducing, 030304 developmental biology, business.industry, rat model, lcsh:R, medicine.disease, stomatognathic diseases, Endocrinology, chemistry, Sclerostin, bone disease, Calcium, Warfarin, Human medicine, business, chronic kidney disease, Calcification

Abstract

Sclerostin is a well-known inhibitor of bone formation that acts on Wnt/&beta, catenin signaling. This manuscript considers the possible role of sclerostin in vascular calcification, a process that shares many similarities with physiological bone formation. Rats were exposed to a warfarin-containing diet to induce vascular calcification. Vascular smooth muscle cell transdifferentiation, vascular calcification grade, and bone histomorphometry were examined. The presence and/or production of sclerostin was investigated in serum, aorta, and bone. Calcified human aortas were investigated to substantiate clinical relevance. Warfarin-exposed rats developed vascular calcifications in a time-dependent manner which went along with a progressive increase in serum sclerostin levels. Both osteogenic and adipogenic pathways were upregulated in calcifying vascular smooth muscle cells, as well as sclerostin mRNA and protein levels. Evidence for the local vascular action of sclerostin was found both in human and rat calcified aortas. Warfarin exposure led to a mildly decreased bone and mineralized areas. Osseous sclerostin production and bone turnover did not change significantly. This study showed local production of sclerostin in calcified vessels, which may indicate a negative feedback mechanism to prevent further calcification. Furthermore, increased levels of serum sclerostin, probably originating from excessive local production in calcified vessels, may contribute to the linkage between vascular pathology and impaired bone mineralization.

Published

2019

34. The human RXFP3 receptor regulates the conserved DNA damage response process

Author

Abdelkrim Azmi, Hanne Leysen, Jhana O. Hendrickx, Stuart Maudsley, Jaana van Gastel, and Paula Santos-Otte

Subjects

Response process, Chemistry, DNA damage, Genetics, Receptor, Molecular Biology, Biochemistry, Biotechnology, Cell biology

Published

2019

35. Multidimensional informatic deconvolution defines gender-specific roles of hypothalamic GIT2 in aging trajectories

Author

Huan Cai, Wayne Chadwick, Elin Lehrmann, Stuart Maudsley, Jaana van Gastel, Caitlin M. Daimon, Bronwen Martin, Laura Vangenechten, Jens Van Turnhout, Hanne Leysen, Jasper Verswyvel, Yongqing Zhang, Robin De Schepper, Wei-na Cong, William H. Wood, Kevin G. Becker, and Jhana O. Hendrickx

Subjects

Male, 0301 basic medicine, Aging, Somatic cell, media_common.quotation_subject, Longevity, Hypothalamus, Biology, Transcriptome, Loss of heterozygosity, Mice, 03 medical and health sciences, 0302 clinical medicine, Animals, Cluster Analysis, media_common, Sex Characteristics, GTPase-Activating Proteins, Computational Biology, Mice, Inbred C57BL, 030104 developmental biology, Functional annotation, Evolutionary biology, Informatics, RNA, Female, Human medicine, Metabolic activity, 030217 neurology & neurosurgery, Signal Transduction, Developmental Biology

Abstract

In most species, females live longer than males. An understanding of this female longevity advantage will likely uncover novel anti-aging therapeutic targets. Here we investigated the transcriptomic responses in the hypothalamus - a key organ for somatic aging control - to the introduction of a simple aging-related molecular perturbation, i.e. GIT2 heterozygosity. Our previous work has demonstrated that GIT2 acts as a network controller of aging. A similar number of both total (1079-female, 1006-male) and gender-unique (577-female, 527-male) transcripts were significantly altered in response to GIT2 heterozygosity in early life-stage (2 month-old) mice. Despite a similar volume of transcriptomic disruption in females and males, a considerably stronger dataset coherency and functional annotation representation was observed for females. It was also evident that female mice possessed a greater resilience to pro-aging signaling pathways compared to males. Using a highly data-dependent natural language processing informatics pipeline, we identified novel functional data clusters that were connected by a coherent group of multifunctional transcripts. From these it was clear that females prioritized metabolic activity preservation compared to males to mitigate this pro-aging perturbation. These findings were corroborated by somatic metabolism analyses of living animals, demonstrating the efficacy of our new informatics pipeline.

Published

2019

36. Enhanced Molecular Appreciation of Psychiatric Disorders Through High-Dimensionality Data Acquisition and Analytics

Author

Bronwen Martin, Len Veenker, Manuel Morrens, Jaana van Gastel, Sophie Beuning, Jhana O. Hendrickx, Violette Coppens, Hanne Leysen, and Stuart Maudsley

Subjects

0301 basic medicine, medicine.medical_specialty, Insufficient Sample, Molecular signaling, business.industry, Schizophrenia (object-oriented programming), Mental disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Analytics, Psychiatric diagnosis, medicine, Human medicine, High dimensionality, Psychology, business, Psychiatry, 030217 neurology & neurosurgery

Abstract

The initial diagnosis, molecular investigation, treatment, and posttreatment care of major psychiatric disorders (schizophrenia and bipolar depression) are all still significantly hindered by the current inability to define these disorders in an explicit molecular signaling manner. High-dimensionality data analytics, using large datastreams from transcriptomic, proteomic, or metabolomic investigations, will likely advance both the appreciation of the molecular nature of major psychiatric disorders and simultaneously enhance our ability to more efficiently diagnose and treat these debilitating conditions. High-dimensionality data analysis in psychiatric research has been heterogeneous in aims and methods and limited by insufficient sample sizes, poorly defined case definitions, methodological inhomogeneity, and confounding results. All of these issues combine to constrain the conclusions that can be extracted from them. Here, we discuss possibilities for overcoming methodological challenges through the implementation of transcriptomic, proteomic, or metabolomics signatures in psychiatric diagnosis and offer an outlook for future investigations. To fulfill the promise of intelligent high-dimensionality data-based differential diagnosis in mental disease diagnosis and treatment, future research will need large, well-defined cohorts in combination with state-of-the-art technologies.

Published

2019

37. GRK5 – A Functional Bridge Between Cardiovascular and Neurodegenerative Disorders

Author

Hanne Leysen, Bronwen Martin, Paula Santos-Otte, Stuart Maudsley, Richard T. Premont, Jaana van Gastel, and Jhana O. Hendrickx

Subjects

0301 basic medicine, Normal aging, Disease, Review, 03 medical and health sciences, G-Protein-Coupled Receptor Kinase 5, cardiovascular disease, GRK5 interactors, G-protein coupled receptor kinase 5, Medicine, Dementia, Pharmacology (medical), Receptor, Pharmacology, business.industry, Pharmacology. Therapy, Neurodegeneration, lcsh:RM1-950, aging, neurodegeneration, medicine.disease, 030104 developmental biology, lcsh:Therapeutics. Pharmacology, Signal transduction, business, Protein network, Neuroscience

Abstract

Complex aging-triggered disorders are multifactorial programs that comprise a myriad of alterations in interconnected protein networks over a broad range of tissues. It is evident that rather than being randomly organized events, pathophysiologies that possess a strong aging component such as cardiovascular diseases (hypertensions, atherosclerosis, and vascular stiffening) and neurodegenerative conditions (dementia, Alzheimer's disease, mild cognitive impairment, Parkinson's disease), in essence represent a subtly modified version of the intricate molecular programs already in place for normal aging. To control such multidimensional activities there are layers of trophic protein control across these networks mediated by so-called "keystone" proteins. We propose that these "keystones" coordinate and interconnect multiple signaling pathways to control whole somatic activities such as aging-related disease etiology. Given its ability to control multiple receptor sensitivities and its broad protein-protein interactomic nature, we propose that G protein coupled receptor kinase 5 (GRK5) represents one of these key network controllers. Considerable data has emerged, suggesting that GRK5 acts as a bridging factor, allowing signaling regulation in pathophysiological settings to control the connectivity between both the cardiovascular and neurophysiological complications of aging.

Published

2018

38. G Protein-Coupled Receptor Systems as Crucial Regulators of DNA Damage Response Processes

Author

Jaana van Gastel, Stuart Maudsley, Paula Santos-Otte, Bronwen Martin, Jhana O. Hendrickx, and Hanne Leysen

Subjects

0301 basic medicine, Aging, DNA Repair, interactome, Review, medicine.disease_cause, Interactome, Receptors, G-Protein-Coupled, lcsh:Chemistry, energy metabolism, Protein Interaction Maps, lcsh:QH301-705.5, Spectroscopy, General Medicine, Computer Science Applications, Cell biology, Chemistry, G protein-coupled receptor kinase interacting protein 2 (GIT2), Signal Transduction, Cell signaling, DNA damage, G protein-coupled receptor kinase (GRK), G protein-coupled receptor (GPCR), 570 Biologie, Biology, Catalysis, Inorganic Chemistry, 03 medical and health sciences, ataxia telangiectasia mutated (ATM), ddc:570, medicine, Animals, Humans, CLOCK Proteins, Physical and Theoretical Chemistry, Molecular Biology, G protein-coupled receptor, β-arrestin, Organic Chemistry, aging, clock proteins, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, Targeted drug delivery, Human medicine, Oxidative stress, Function (biology)

Abstract

G protein-coupled receptors (GPCRs) and their associated proteins represent one of the most diverse cellular signaling systems involved in both physiological and pathophysiological processes. Aging represents perhaps the most complex biological process in humans and involves a progressive degradation of systemic integrity and physiological resilience. This is in part mediated by age-related aberrations in energy metabolism, mitochondrial function, protein folding and sorting, inflammatory activity and genomic stability. Indeed, an increased rate of unrepaired DNA damage is considered to be one of the hallmarks of aging. Over the last two decades our appreciation of the complexity of GPCR signaling systems has expanded their functional signaling repertoire. One such example of this is the incipient role of GPCRs and GPCR-interacting proteins in DNA damage and repair mechanisms. Emerging data now suggest that GPCRs could function as stress sensors for intracellular damage, e.g., oxidative stress. Given this role of GPCRs in the DNA damage response process, coupled to the effective history of drug targeting of these receptors, this suggests that one important future activity of GPCR therapeutics is the rational control of DNA damage repair systems. View Full-Text Keywords: G protein-coupled receptor (GPCR); aging; DNA damage; β-arrestin; G protein-coupled receptor kinase (GRK); interactome; G protein-coupled receptor kinase interacting protein 2 (GIT2); ataxia telangiectasia mutated (ATM); clock proteins; energy metabolism

Published

2018

39. Author response: Transition between fermentation and respiration determines history-dependent behavior in fluctuating carbon sources

Author

Pieter Berden, Maarten Coomans, Maria C Dzialo, Lieselotte Vermeersch, Jhana O Hendrickx, Sara Verbandt, Sander K. Govers, Gemma Perez-Samper, Kevin J. Verstrepen, Julian M. J. Pietsch, Eva Galle, Bram Cerulus, Peter S. Swain, Miguel Roncoroni, Abbas Jariani, Brigida Gallone, Aaron M. New, and Matthew M. Crane

Subjects

Chemistry, Respiration, chemistry.chemical_element, Thermodynamics, Fermentation, Carbon

Published

2018

40. The RXFP3‐GIT2 signaling system represents a potential multidimensional therapeutic target in age‐related disorders

Author

Abdelkrim Azmi, Mi‐Hye M. Lee, Stuart Maudsley, Jonathan Janssens, Jhana O. Hendrickx, Jaana van Gastel, Hanne Leysen, and Louis M. Luttrell

Subjects

0301 basic medicine, 03 medical and health sciences, 030104 developmental biology, Age related, Genetics, Biology, Molecular Biology, Biochemistry, Neuroscience, Biotechnology, Signaling system

Published

2018

41. Transition between fermentation and respiration determines history-dependent behavior in fluctuating carbon sources

Author

Jhana O Hendrickx, Maarten Coomans, Sara Verbandt, Maria C Dzialo, Sander K. Govers, Pieter Berden, Kevin J. Verstrepen, Lieselotte Vermeersch, Aaron M. New, Abbas Jariani, Brigida Gallone, Matthew M. Crane, Peter S. Swain, Gemma Perez-Samper, Julian M. J. Pietsch, Eva Galle, Bram Cerulus, and Miguel Roncoroni

Subjects

0301 basic medicine, Life Sciences & Biomedicine - Other Topics, Time Factors, Cell division, S. cerevisiae, Cell Count, YEAST SACCHAROMYCES-CEREVISIAE, CATABOLITE INACTIVATION, GLUCOSE, chemistry.chemical_compound, Gene Expression Regulation, Fungal, single-cell analysis, Gene Regulatory Networks, Biology (General), Microbiology and Infectious Disease, biology, General Neuroscience, General Medicine, ENVIRONMENTAL-CHANGES, Aerobiosis, lag phase, Medicine, glucose repression, Life Sciences & Biomedicine, metabolic shift, Research Article, Computational and Systems Biology, Saccharomyces cerevisiae Proteins, QH301-705.5, Systems biology, Science, Genes, Fungal, Saccharomyces cerevisiae, Carbohydrates, NUCLEAR-PORE COMPLEX, SIGNAL-TRANSDUCTION, cellular memory, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Oxygen Consumption, Respiration, RNA, Messenger, Biology, GAL GENES, Cell Nucleus, Science & Technology, General Immunology and Microbiology, Gene Expression Profiling, Metabolism, Maltose, biology.organism_classification, Carbon, Yeast, TRANSCRIPTIONAL MEMORY, CELLULAR MEMORY, 030104 developmental biology, chemistry, Fermentation, Mutation, Biophysics, gene regulation, MALTOSE TRANSPORTER

Abstract

Cells constantly adapt to environmental fluctuations. These physiological changes require time and therefore cause a lag phase during which the cells do not function optimally. Interestingly, past exposure to an environmental condition can shorten the time needed to adapt when the condition re-occurs, even in daughter cells that never directly encountered the initial condition. Here, we use the molecular toolbox of Saccharomyces cerevisiae to systematically unravel the molecular mechanism underlying such history-dependent behavior in transitions between glucose and maltose. In contrast to previous hypotheses, the behavior does not depend on persistence of proteins involved in metabolism of a specific sugar. Instead, presence of glucose induces a gradual decline in the cells' ability to activate respiration, which is needed to metabolize alternative carbon sources. These results reveal how trans-generational transitions in central carbon metabolism generate history-dependent behavior in yeast, and provide a mechanistic framework for similar phenomena in other cell types. ispartof: ELIFE vol:7 ispartof: location:England status: published

Published

2018

42. <tex>\beta$</tex>-Arrestin based receptor signaling paradigms : potential therapeutic targets for complex age-related disorders

Author

Jaana van Gastel, Jhana O. Hendrickx, Hanne Leysen, Paula Santos-Otte, Louis M. Luttrell, Bronwen Martin, and Stuart Maudsley

Subjects

0301 basic medicine, G protein, media_common.quotation_subject, Review, GPCRs, ligand ‘bias’, 03 medical and health sciences, Arrestin, Pharmacology (medical), ddc:610, Internalization, β-arrestin signaling, G protein-coupled receptor, media_common, Pharmacology, biology, Effector, Pharmacology. Therapy, lcsh:RM1-950, tailored efficacy, 030104 developmental biology, lcsh:Therapeutics. Pharmacology, Rhodopsin, Mitogen-activated protein kinase, Second messenger system, biology.protein, precision, age-related disorders, 610 Medizin und Gesundheit, Neuroscience

Abstract

G protein coupled receptors (GPCRs) were first characterized as signal transducers that elicit downstream effects through modulation of guanine (G) nucleotide-binding proteins. The pharmacotherapeutic exploitation of this signaling paradigm has created a drug-based field covering nearly 50% of the current pharmacopeia. Since the groundbreaking discoveries of the late 1990s to the present day, it is now clear however that GPCRs can also generate productive signaling cascades through the modulation of beta-arrestin functionality. beta-Arrestins were first thought to only regulate receptor desensitization and internalization - exemplified by the action of visual arrestin with respect to rhodopsin desensitization. Nearly 20 years ago, it was found that rather than controlling GPCR signal termination, productive beta-arrestin dependent GPCR signaling paradigms were highly dependent on multi-protein complex formation and generated long-lasting cellular effects, in contrast to G protein signaling which is transient and functions through soluble second messenger systems. beta-Arrestin signaling was then first shown to activate mitogen activated protein kinase signaling in a G protein-independent manner and eventually initiate protein transcription - thus controlling expression patterns of downstream proteins. While the possibility of developing beta-arrestin biased or functionally selective ligands is now being investigated, no additional research has been performed on its possible contextual specificity in treating age-related disorders. The ability of beta-arrestin-dependent signaling to control complex and multidimensional protein expression patterns makes this therapeutic strategy feasible, as treating complex age-related disorders will likely require therapeutics that can exert network-level efficacy profiles. It is our understanding that therapeutically targeting G protein-independent effectors such as beta-arrestin will aid in the development of precision medicines with tailored efficacy profiles for disease/age-specific contextualities.

Published

2018

43. 680 Neuregulin stimulates nitric oxide production in cardiomyocytes

Author

Katrien Lemmens, G.W. De Keulenaer, Jhana O. Hendrickx, Stanislas U. Sys, D. L. Brutsaert, and Paul Fransen

Subjects

chemistry.chemical_compound, chemistry, business.industry, Medicine, Neuregulin, Cardiology and Cardiovascular Medicine, business, Nitric oxide, Cell biology

Published

2003

44. Transition between fermentation and respiration determines history-dependent behavior in fluctuating carbon sources

Author

Bram Cerulus, Abbas Jariani, Gemma Perez-Samper, Lieselotte Vermeersch, Julian MJ Pietsch, Matthew M Crane, Aaron M New, Brigida Gallone, Miguel Roncoroni, Maria C Dzialo, Sander K Govers, Jhana O Hendrickx, Eva Galle, Maarten Coomans, Pieter Berden, Sara Verbandt, Peter S Swain, and Kevin J Verstrepen

Subjects

cellular memory, lag phase, metabolic shift, glucose repression, gene regulation, single-cell analysis, Medicine, Science, Biology (General), QH301-705.5

Abstract

Cells constantly adapt to environmental fluctuations. These physiological changes require time and therefore cause a lag phase during which the cells do not function optimally. Interestingly, past exposure to an environmental condition can shorten the time needed to adapt when the condition re-occurs, even in daughter cells that never directly encountered the initial condition. Here, we use the molecular toolbox of Saccharomyces cerevisiae to systematically unravel the molecular mechanism underlying such history-dependent behavior in transitions between glucose and maltose. In contrast to previous hypotheses, the behavior does not depend on persistence of proteins involved in metabolism of a specific sugar. Instead, presence of glucose induces a gradual decline in the cells’ ability to activate respiration, which is needed to metabolize alternative carbon sources. These results reveal how trans-generational transitions in central carbon metabolism generate history-dependent behavior in yeast, and provide a mechanistic framework for similar phenomena in other cell types.

Published

2018