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Early Perturbations in Mitochondrial Metabolism and Bioenergetics Exerted by Trypanosoma cruzi Infection in Human Cardiomyocytes
DOI: 10.1016/j.freeradbiomed.2017.10.175
162 Combination Antiretroviral Therapy (cART) Altered Redox/Nitrosative genes,
163
Enhanced Systemic Stress and Cardiac
Early Perturbations in Mitochondrial
dysfunction in HIV-1 Transgenic (HIV-Tg)
Metabolism and Bioenergetics Exerted by
Rats: Effects of Magnesium
Trypanosoma cruzi Infection in Human
Supplementation (Mg-Supp) Ivan Tong Mak1, Jay H. Kramer1, Lama Elzohary1, Joanna J Chmielinska , Chris Spurney , and William B Weglicki 1
2
George Washington University, USA
2
Children's National Medical Center, USA determined
if
clinically
Cardiomyocytes Laura María González-Ortiz1,2, Yudy Rodríguez-Avila1,3, Sandra Milena Sanabria-Barrera1,2, Ana Doris Gomez-
1
We
1
used
Granados3, María Eugenia Cárdenas Angelone4, Diego Torres-Dueñas4, Nisha J Garg5, and Marcos Lopez1,2 cART
promoted
redox/nitrosative stress and cardiac toxicity in control and
1
Fundacion Cardiovascular de Colombia, Floridablanca,
Colombia
HIV-Tg rats and the effects of Mg. Treatment with cART
2
(Truvada+atazanavir/ritonavir) up to 18 weeks, induced
Universidad del Valle, Cali, Colombia
3
significant hypomagnesemia (-25%), elevated plasma 8-
Universidad de Santander, Bucaramanga, Colombia
4
isoprostane, and RBC GSSG 2-3 folds (at 6 wks); plasma 3-
Universidad Autónoma de Bucaramanga, Colombia
5
University of Texas Medical Branch, Galveston, Texas, USA
nitrotyrosine (NT) increased 3.5-fold in the HIV-Tg rats (at 18 wks). In association, liver Nrf2 mRNA (by real time RTPCR)
was
down-regulated
75%
along
with
altered
expression of HmOX-1 and GST; however iNOS and TNFα mRNAs were increased 2- & 4-fold. Prominent ventricular NT
staining
was
observed
in
HIV-Tg+cART
rats;
echocardiography detected time-dependent moderate, but significant
decreases
in
cardiac
systolic
(Fractional
Shortening. -17%, 18 wks) and diastolic (E/A, -26%) functions.
Mg-Supp (6X normal) in diet, substantially
prevented rises in levels of 8-isoprostane, GSSG, and plasma NT. Most strikingly, Mg-Supp restored expressions of Nrf2 and HmOX-1, GST close to controls in HIV-Tg rats; both iNOS
and
TNFα
up-regulations
were
blunted.
In
association, cardiac NT staining was substantially reduced; both cardiac systolic and diastolic functional decreases were attenuated 60-70% by Mg-supp. Conclusions:
cART
treatment
synergized
with
HIV-1
expression in down-regulating Nrf2 pathway, but upregulating iNOS and TNFα expression; elevation of systemic redox/nitrosative stress contributed to cardiac dysfunction. The cardiac protective effects of Mg-Supp might be mediated by its antioxidant actions at the genomic and systemic levels through the Nrf2 pathway Supported
by
NIH
R21-HL-125038,
Genomic Supplemental Fund.
and
McCormick
Chagas’ disease is a zoonotic disease caused by Trypanosoma cruzi infection that is endemic in Mexico, Central and South America. Usually, the disease is transmitted by a triatomine vector and domestic and wild mammals that serve as reservoirs for this parasitic protozoan. However, due to increased immigration, individuals with the disease have been identified in developed countries like the USA, Canada and
Europe,
increasing
the
possibility
of
secondary
transmission routes of T. cruzi via organ transplantation, blood transfusions and maternal-fetal transmission. The clinical course of the disease is divided into the acute and chronic phases. While the acute infection is mildly asymptomatic and often misdiagnosed, the chronic phase usually manifests as cardiomyopathy with a wide spectrum of
manifestations,
ranging
from
minor
myocardium
involvement to left ventricular (LV) systolic dysfunction, dilated
cardiomyopathy,
arrhythmias,
thromboembolic
events, and terminal cardiac failure. Interestingly, because chagasic hearts are virtually free of parasites, and the etiology of chronic Chagas disease remains under heavy discussion. The B and T cell immunity in combination with mitochondrial
dysfunction,
inflammatory
cytokines/chemokines, and oxidative stress are the hallmark of the disease. In this work, we aimed to elucidate the early metabolic perturbations exerted by T. cruzi (Sylvio X10) infection in AC16 human cardiomyocytes. In addition, we
SfRBM 2017
117
also examined the role of innate immunity by co-treating
reductase activity were analyzed in blood samples. In black
cells with pro-inflammatory proteins and cytokines known
men, ambulatory pulse pressure was negatively associated
to have a role in the infection process like IFN-γ, TNF-α and
with glutathione peroxidase activity (R2 = 0.19; β = -0.25;
IL-6. Early changes in metabolism and mitochondrial
p = 0.026). Black and white women displayed positive
bioenergetics were assessed in real time with a Seahorse
associations of ambulatory systolic blood pressure and
XFe24 Extracellular Flux Analyzer. We found that T. cruzi
ambulatory
infection alone, was not enough to induce significant
reductase activity while white men displayed a positive
mean
arterial
pressure
with
glutathione
changes in mitochondrial metabolism and bioenergetics and
association of ambulatory pulse pressure with glutathione
to increase ROS generation in human cardiomyocytes.
reductase activity. The lower glutathione peroxidase activity
However, T. cruzi infection in combination with IFN-γ, TNF-
and total antioxidant status, the higher reactive oxygen
α and IL-6 exerted a drastic effect in cardiomyocyte
species as well as the negative association between
mitochondrial bioenergetics and ROS production, suggesting
ambulatory pulse pressure and glutathione peroxidase
that innate immunity plays a key role in Chagas-induced
activity in the black men suggest that oxidative stress is
cardiomyopathy.
associated with early vascular changes in this group. In the other three groups, the positive associations of blood pressure with glutathione reductase activity suggest a
DOI: 10.1016/j.freeradbiomed.2017.10.176
possible role for adequate glutathione reductase activity in preventing or delaying the development of hypertension. DOI: 10.1016/j.freeradbiomed.2017.10.177
164 The Relation of blood pressure and carotid intima-media
thickness
with
the
glutathione cycle in a young bi-ethnic population: The African-PREDICT study
Effect of Nitrite and N-acetylcysteine
Caitlynd Myburgh1,2, Catharina MC Mels1,3, and Hugo W Huisman1,3 1
Hypertension in Africa Research Team (HART), South
Africa
Treatment on Blood Pressure, Arterial Stiffness and Vascular Function in Spontaneously Hypertensive Rats Enika Nagababu1, Jochen Steppan1, Lakshmi Santhanam1,
2
University of South Africa (UNISA), South Africa
3
MRC Research Unit for Hypertension and Cardiovascular
Disease, North-West University, South Africa Oxidative stress has been implicated in the development of hypertension, arterial stiffness and atherosclerosis. Optimal functioning of the enzymatic antioxidant system is central to prevent increased oxidative stress and its consequences. We aimed to investigate the relationships of ambulatory blood pressure and carotid intima-media thickness with enzyme activities of the glutathione cycle in young, healthy black and white South Africans. This study included 396 participants (black men (N = 89), white men (N = 78), black women (N = 105) and white women (N = 124)) of the African-PREDICT study aged 20-30 years. Ambulatory blood pressure and carotid intima-media thickness were measured, while glutathione peroxidase and glutathione
118
165
Steven M Frank1, and Dan E Berkowitz1 1
Johns Hopkins Medical Institutions, USA
Introduction: Reduced nitric oxide (NO) bioavailability and increased generation of reactive oxygen species and inflammation with advancing age play a major role in the development of cardiovascular disease (CVD) risk factors of hypertension, endothelial dysfunction and arterial stiffness. Therefore, increase in NO bioavailability by supplementing inorganic nitrite and improve in antioxidant defense system by supplementing N-acetylcysteine (NAC) could protect against the CVD. Hypertension is highly prevalent in a population and cause endothelial dysfunction and arterial stiffness. Hence spontaneously hypertensive rats (SHR) were used in this study as a model for hypertension-mediated endothelial dysfunction and arterial stiffness.
SfRBM 2017
162 Combination Antiretroviral Therapy (cART) Altered Redox/Nitrosative genes,
163
Enhanced Systemic Stress and Cardiac
Early Perturbations in Mitochondrial
dysfunction in HIV-1 Transgenic (HIV-Tg)
Metabolism and Bioenergetics Exerted by
Rats: Effects of Magnesium
Trypanosoma cruzi Infection in Human
Supplementation (Mg-Supp) Ivan Tong Mak1, Jay H. Kramer1, Lama Elzohary1, Joanna J Chmielinska , Chris Spurney , and William B Weglicki 1
2
George Washington University, USA
2
Children's National Medical Center, USA determined
if
clinically
Cardiomyocytes Laura María González-Ortiz1,2, Yudy Rodríguez-Avila1,3, Sandra Milena Sanabria-Barrera1,2, Ana Doris Gomez-
1
We
1
used
Granados3, María Eugenia Cárdenas Angelone4, Diego Torres-Dueñas4, Nisha J Garg5, and Marcos Lopez1,2 cART
promoted
redox/nitrosative stress and cardiac toxicity in control and
1
Fundacion Cardiovascular de Colombia, Floridablanca,
Colombia
HIV-Tg rats and the effects of Mg. Treatment with cART
2
(Truvada+atazanavir/ritonavir) up to 18 weeks, induced
Universidad del Valle, Cali, Colombia
3
significant hypomagnesemia (-25%), elevated plasma 8-
Universidad de Santander, Bucaramanga, Colombia
4
isoprostane, and RBC GSSG 2-3 folds (at 6 wks); plasma 3-
Universidad Autónoma de Bucaramanga, Colombia
5
University of Texas Medical Branch, Galveston, Texas, USA
nitrotyrosine (NT) increased 3.5-fold in the HIV-Tg rats (at 18 wks). In association, liver Nrf2 mRNA (by real time RTPCR)
was
down-regulated
75%
along
with
altered
expression of HmOX-1 and GST; however iNOS and TNFα mRNAs were increased 2- & 4-fold. Prominent ventricular NT
staining
was
observed
in
HIV-Tg+cART
rats;
echocardiography detected time-dependent moderate, but significant
decreases
in
cardiac
systolic
(Fractional
Shortening. -17%, 18 wks) and diastolic (E/A, -26%) functions.
Mg-Supp (6X normal) in diet, substantially
prevented rises in levels of 8-isoprostane, GSSG, and plasma NT. Most strikingly, Mg-Supp restored expressions of Nrf2 and HmOX-1, GST close to controls in HIV-Tg rats; both iNOS
and
TNFα
up-regulations
were
blunted.
In
association, cardiac NT staining was substantially reduced; both cardiac systolic and diastolic functional decreases were attenuated 60-70% by Mg-supp. Conclusions:
cART
treatment
synergized
with
HIV-1
expression in down-regulating Nrf2 pathway, but upregulating iNOS and TNFα expression; elevation of systemic redox/nitrosative stress contributed to cardiac dysfunction. The cardiac protective effects of Mg-Supp might be mediated by its antioxidant actions at the genomic and systemic levels through the Nrf2 pathway Supported
by
NIH
R21-HL-125038,
Genomic Supplemental Fund.
and
McCormick
Chagas’ disease is a zoonotic disease caused by Trypanosoma cruzi infection that is endemic in Mexico, Central and South America. Usually, the disease is transmitted by a triatomine vector and domestic and wild mammals that serve as reservoirs for this parasitic protozoan. However, due to increased immigration, individuals with the disease have been identified in developed countries like the USA, Canada and
Europe,
increasing
the
possibility
of
secondary
transmission routes of T. cruzi via organ transplantation, blood transfusions and maternal-fetal transmission. The clinical course of the disease is divided into the acute and chronic phases. While the acute infection is mildly asymptomatic and often misdiagnosed, the chronic phase usually manifests as cardiomyopathy with a wide spectrum of
manifestations,
ranging
from
minor
myocardium
involvement to left ventricular (LV) systolic dysfunction, dilated
cardiomyopathy,
arrhythmias,
thromboembolic
events, and terminal cardiac failure. Interestingly, because chagasic hearts are virtually free of parasites, and the etiology of chronic Chagas disease remains under heavy discussion. The B and T cell immunity in combination with mitochondrial
dysfunction,
inflammatory
cytokines/chemokines, and oxidative stress are the hallmark of the disease. In this work, we aimed to elucidate the early metabolic perturbations exerted by T. cruzi (Sylvio X10) infection in AC16 human cardiomyocytes. In addition, we
SfRBM 2017
117
also examined the role of innate immunity by co-treating
reductase activity were analyzed in blood samples. In black
cells with pro-inflammatory proteins and cytokines known
men, ambulatory pulse pressure was negatively associated
to have a role in the infection process like IFN-γ, TNF-α and
with glutathione peroxidase activity (R2 = 0.19; β = -0.25;
IL-6. Early changes in metabolism and mitochondrial
p = 0.026). Black and white women displayed positive
bioenergetics were assessed in real time with a Seahorse
associations of ambulatory systolic blood pressure and
XFe24 Extracellular Flux Analyzer. We found that T. cruzi
ambulatory
infection alone, was not enough to induce significant
reductase activity while white men displayed a positive
mean
arterial
pressure
with
glutathione
changes in mitochondrial metabolism and bioenergetics and
association of ambulatory pulse pressure with glutathione
to increase ROS generation in human cardiomyocytes.
reductase activity. The lower glutathione peroxidase activity
However, T. cruzi infection in combination with IFN-γ, TNF-
and total antioxidant status, the higher reactive oxygen
α and IL-6 exerted a drastic effect in cardiomyocyte
species as well as the negative association between
mitochondrial bioenergetics and ROS production, suggesting
ambulatory pulse pressure and glutathione peroxidase
that innate immunity plays a key role in Chagas-induced
activity in the black men suggest that oxidative stress is
cardiomyopathy.
associated with early vascular changes in this group. In the other three groups, the positive associations of blood pressure with glutathione reductase activity suggest a
DOI: 10.1016/j.freeradbiomed.2017.10.176
possible role for adequate glutathione reductase activity in preventing or delaying the development of hypertension. DOI: 10.1016/j.freeradbiomed.2017.10.177
164 The Relation of blood pressure and carotid intima-media
thickness
with
the
glutathione cycle in a young bi-ethnic population: The African-PREDICT study
Effect of Nitrite and N-acetylcysteine
Caitlynd Myburgh1,2, Catharina MC Mels1,3, and Hugo W Huisman1,3 1
Hypertension in Africa Research Team (HART), South
Africa
Treatment on Blood Pressure, Arterial Stiffness and Vascular Function in Spontaneously Hypertensive Rats Enika Nagababu1, Jochen Steppan1, Lakshmi Santhanam1,
2
University of South Africa (UNISA), South Africa
3
MRC Research Unit for Hypertension and Cardiovascular
Disease, North-West University, South Africa Oxidative stress has been implicated in the development of hypertension, arterial stiffness and atherosclerosis. Optimal functioning of the enzymatic antioxidant system is central to prevent increased oxidative stress and its consequences. We aimed to investigate the relationships of ambulatory blood pressure and carotid intima-media thickness with enzyme activities of the glutathione cycle in young, healthy black and white South Africans. This study included 396 participants (black men (N = 89), white men (N = 78), black women (N = 105) and white women (N = 124)) of the African-PREDICT study aged 20-30 years. Ambulatory blood pressure and carotid intima-media thickness were measured, while glutathione peroxidase and glutathione
118
165
Steven M Frank1, and Dan E Berkowitz1 1
Johns Hopkins Medical Institutions, USA
Introduction: Reduced nitric oxide (NO) bioavailability and increased generation of reactive oxygen species and inflammation with advancing age play a major role in the development of cardiovascular disease (CVD) risk factors of hypertension, endothelial dysfunction and arterial stiffness. Therefore, increase in NO bioavailability by supplementing inorganic nitrite and improve in antioxidant defense system by supplementing N-acetylcysteine (NAC) could protect against the CVD. Hypertension is highly prevalent in a population and cause endothelial dysfunction and arterial stiffness. Hence spontaneously hypertensive rats (SHR) were used in this study as a model for hypertension-mediated endothelial dysfunction and arterial stiffness.
SfRBM 2017