I have a few ideas that I hope are not completely hopeless due to cost and so on. Each of them is related to C60's likely mechanism of action (being a really bioavailable antioxidant)
Furthermore it would be possible to use this stuff as good background material for a C60-mouse study to kind of anchor it within the pre-existing free radical biological-scientific framework.
I will present them below with links to the relevant articles.
Evaluating endothelial function / dysfuntion:
J Physiol. 2014 Jun 15;592(Pt 12):2549-61. doi: 10.1113/jphysiol.2013.268680. Epub 2014 Mar 24.
Mitochondria-targeted antioxidant (MitoQ) ameliorates age-related arterial endothelial dysfunction in mice.
Abstract
Abstract
Age-related arterial endothelial dysfunction, a key antecedent of the development of cardiovascular disease (CVD), is largely caused by a reduction in nitric oxide (NO) bioavailability as a consequence of oxidative stress. Mitochondria are a major source and target of vascular oxidative stress when dysregulated. Mitochondrial dysregulation is associated with primary ageing, but its role in age-related endothelial dysfunction is unknown. Our aim was to determine the efficacy of a mitochondria-targeted antioxidant, MitoQ, in ameliorating vascular endothelial dysfunction in old mice. Ex vivo carotid artery endothelium-dependent dilation (EDD) to increasing doses of acetylcholine was impaired by ∼30% in old (∼27 months) compared with young (∼8 months) mice as a result of reduced NO bioavailability (P < 0.05). Acute (ex vivo) and chronic (4 weeks in drinking water) administration of MitoQ completely restored EDD in older mice by improving NO bioavailability. There were no effects of age or MitoQ on endothelium-independent dilation to sodium nitroprusside. The improvements in endothelial function with MitoQ supplementation were associated with the normalization of age-related increases in total and mitochondria-derived arterial superoxide production and oxidative stress (nitrotyrosine abundance), as well as with increases in markers of vascular mitochondrial health, including antioxidant status. MitoQ also reversed the age-related increase in endothelial susceptibility to acute mitochondrial damage (rotenone-induced impairment in EDD). Our results suggest that mitochondria-derived oxidative stress is an important mechanism underlying the development of endothelial dysfunction in primary ageing. Mitochondria-targeted antioxidants such as MitoQ represent a promising novel strategy for the preservation of vascular endothelial function with advancing age and the prevention of age-related CVD.
© 2014 The Authors. The Journal of Physiology © 2014 The Physiological Society.
http://onlinelibrary...268680/abstract
Looking at levels of 8-oxodG, which seems to be a fairly established biomarker:
Cruciferous vegetables contain compounds with antioxidant properties (e.g. carotenoids, vitamin C and folates) and can alter the activity of xenobiotic metabolism (i.e. isothiocyanates). These constituents may be particularly important for subjects who are exposed to free radicals and genotoxic compounds, including smokers. The aim of the study was to evaluate the effect of broccoli intake on biomarkers of DNA damage and repair. Twenty-seven young healthy smokers consumed a portion of steamed broccoli (250 g/day) or a control diet for 10 days each within a crossover design with a washout period. Blood was collected before and after each period. The level of oxidatively damaged DNA lesions (formamidopyrimidine DNA glycosylase-sensitive sites), resistance to ex vivo H2O2 treatment and repair of oxidised DNA lesions were measured in peripheral blood mononuclear cells (PBMCs). We also measured mRNA expression levels of repair and defence enzymes: 8-oxoguanine DNA glycosylase (OGG1), nucleoside diphosphate linked moiety X-type motif 1 (NUDT1) and heme oxygenase 1 (HO-1). After broccoli consumption, the level of oxidised DNA lesions decreased by 41% (95% confidence interval: 10%, 72%) and the resistance to H2O2-induced DNA strand breaks increased by 23% (95% CI: 13%, 34%). Following broccoli intake, a higher protection was observed in subjects with glutathione S-transferase (GST) M1-null genotype. The expression level and activity of repair enzymes was unaltered. In conclusion, broccoli intake was associated with increased protection against H2O2-induced DNA strand breaks and lower levels of oxidised DNA bases in PBMCs from smokers. This protective effect could be related to an overall improved antioxidant status.
Mutagenesis. 2010 Nov;25(6):595-602. doi: 10.1093/mutage/geq045. Epub 2010 Aug 16.
DNA damage and repair activity after broccoli intake in young healthy smokers.
Abstract
Cruciferous vegetables contain compounds with antioxidant properties (e.g. carotenoids, vitamin C and folates) and can alter the activity of xenobiotic metabolism (i.e. isothiocyanates). These constituents may be particularly important for subjects who are exposed to free radicals and genotoxic compounds, including smokers. The aim of the study was to evaluate the effect of broccoli intake on biomarkers of DNA damage and repair. Twenty-seven young healthy smokers consumed a portion of steamed broccoli (250 g/day) or a control diet for 10 days each within a crossover design with a washout period. Blood was collected before and after each period. The level of oxidatively damaged DNA lesions (formamidopyrimidine DNA glycosylase-sensitive sites), resistance to ex vivo H(2)O(2) treatment and repair of oxidised DNA lesions were measured in peripheral blood mononuclear cells (PBMCs). We also measured mRNA expression levels of repair and defence enzymes: 8-oxoguanine DNA glycosylase (OGG1), nucleoside diphosphate linked moiety X-type motif 1 (NUDT1) and heme oxygenase 1 (HO-1). After broccoli consumption, the level of oxidised DNA lesions decreased by 41% (95% confidence interval: 10%, 72%) and the resistance to H(2)O(2)-induced DNA strand breaks increased by 23% (95% CI: 13%, 34%). Following broccoli intake, a higher protection was observed in subjects with glutathione S-transferase (GST) M1-null genotype. The expression level and activity of repair enzymes was unaltered. In conclusion, broccoli intake was associated with increased protection against H(2)O(2)-induced DNA strand breaks and lower levels of oxidised DNA bases in PBMCs from smokers. This protective effect could be related to an overall improved antioxidant status.
http://www.ncbi.nlm....pubmed/20713433
Ischemia-Reperfusion injury:
Protective effects of superoxide dismutase against ischemia-reperfusion injury: development and application of a transgenic animal model.
Abstract
Reperfusion of ischemic tissues can be associated with structural and functional injury, which is referred to as ischemia-reperfusion injury. Superoxide dismutase is an endogenous free radical scavenger that converts toxic oxygen derived free radicals to hydrogen peroxide. With the development of gene cloning technology, the potential of manipulating cells to overexpress endogenous proteins has been realized. Transgenic mice capable of overexpressing superoxide dismutase, and knockout mice in which the gene responsible for its production has been deleted, were used as a model to examine the protective effects of superoxide dismutase against ischemia-reperfusion injury. Epigastric island flaps were elevated in wild-type (control), transgenic superoxide dismutase 1, and knockout superoxide dismutase 1 mice and subjected to ischemic intervals of 0, 3, 6, 9, or 12 hours. Five animals were studied at each time point in each study group. Flap viability was assessed on postoperative day 7. Baseline wild-type flap survival was 100 percent after 3 hours of ischemia and subsequent reperfusion; survival decreased to 21 percent after 9 hours of ischemia. Transgenic mice had significantly higher flap survival than wild-type animals after 6 hours of ischemia and subsequent reperfusion (97.0 versus 85.2 percent) and after 9 hours of ischemia (82 versus 21 percent, p < 0.01). In knockout mice, there was complete flap necrosis after as little as 3 hours of ischemia. This study confirms the protective effects of superoxide dismutase against ischemia-reperfusion injury. In addition, its deficiency results in a dramatic susceptibility to ischemic injury.
http://www.ncbi.nlm....pubmed/12496586
Highly efficient conversion of superoxide to oxygen using hydrophilic carbon clusters.
Samuel EL1,
Marcano DC2,
Berka V3,
Bitner BR4,
Wu G3,
Potter A1,
Fabian RH5,
Pautler RG4,
Kent TA6,
Tsai AL7,
Tour JM8.
Abstract
Many diseases are associated with oxidative stress, which occurs when the production of reactive oxygen species (ROS) overwhelms the scavenging ability of an organism. Here, we evaluated the carbon nanoparticle antioxidant properties of poly(ethylene glycolated) hydrophilic carbon clusters (PEG-HCCs) by electron paramagnetic resonance (EPR) spectroscopy, oxygen electrode, and spectrophotometric assays. These carbon nanoparticles have 1 equivalent of stable radical and showed superoxide (O2 (•-)) dismutase-like properties yet were inert to nitric oxide (NO(•)) as well as peroxynitrite (ONOO(-)). Thus, PEG-HCCs can act as selective antioxidants that do not require regeneration by enzymes. Our steady-state kinetic assay using KO2 and direct freeze-trap EPR to follow its decay removed the rate-limiting substrate provision, thus enabling determination of the remarkable intrinsic turnover numbers of O2 (•-) to O2 by PEG-HCCs at >20,000 s(-1). The major products of this catalytic turnover are O2 and H2O2, making the PEG-HCCs a biomimetic superoxide dismutase.
Nanoparticles reboot blood flow in brain
Nanoantioxidants reboot brain blood-flow
Rice University, Baylor College of Medicine discovery might aid emergency care of traumatic brain-injury victims
A nanoparticle developed at Rice University and tested in collaboration with Baylor College of Medicine (BCM) may bring great benefits to the emergency treatment of brain-injury victims, even those with mild injuries.
Combined polyethylene glycol-hydrophilic carbon clusters (PEG-HCC), already being tested to enhance cancer treatment, are also adept antioxidants. In animal studies, injections of PEG-HCC during initial treatment after an injury helped restore balance to the brain’s vascular system.
The results were reported this month in the American Chemical Society journal ACS Nano.
A PEG-HCC infusion that quickly stabilizes blood flow in the brain would be a significant advance for emergency care workers and battlefield medics, said Rice chemist and co-author James Tour.
“This might be a first line of defense against reactive oxygen species (ROS) that are always overstimulated during a medical trauma, whether that be to an accident victim or an injured soldier,” said Tour, Rice’s T.T. and W.F. Chao Chair in Chemistry as well as a professor of mechanical engineering and materials science and of computer science. “They’re certainly exacerbated when there’s trauma with massive blood loss.”
In a traumatic brain injury, cells release an excessive amount of an ROS known as superoxide (SO) into the blood. Superoxides are toxic free radicals, molecules with one unpaired electron, that the immune system normally uses to kill invading microorganisms. Healthy organisms balance SO with superoxide dismutase (SOD), an enzyme that neutralizes it. But even mild brain trauma can release superoxides at levels that overwhelm the brain’s natural defenses.
“Superoxide is the most deleterious of the reactive oxygen species, as it’s the progenitor of many of the others,” Tour said. “If you don’t deal with SO, it forms peroxynitrite and hydrogen peroxide. SO is the upstream precursor to many of the downstream problems.”
SO affects the autoregulatory mechanism that manages the sensitive circulation system in the brain. Normally, vessels dilate when blood pressure is low and constrict when high to maintain an equilibrium, but a lack of regulation can lead to brain damage beyond what may have been caused by the initial trauma.
“There are many facets of brain injury that ultimately determine how much damage there will be,” said Thomas Kent, the paper’s co-author, a BCM professor of neurology and chief of neurology at the Michael E. DeBakey Veterans Affairs Medical Center in Houston. “One is the initial injury, and that’s pretty much done in minutes. But a number of things that happen later often make things worse, and that’s when we can intervene.”
Kent cited as an example the second burst of free radicals that can occur after post-injury resuscitation. “That’s what we can treat: the further injury that happens because of the necessity of restoring somebody’s blood pressure, which provides oxygen that leads to more damaging free radicals.”
In tests, the researchers found PEG-HCC nanoparticles immediately and completely quenched superoxide activity and allowed the autoregulatory system to quickly regain its balance. Tour said ROS molecules readily combine with PEG-HCCs, generating “an innocuous carbon double bond, so it’s really radical annihilation. There’s no such mechanism in biology.” While an SOD enzyme can alter only one superoxide molecule at a time, a single PEG-HCC about the size of a large protein at 2-3 nanometers wide and 30-40 nanometers long can quench hundreds or thousands. “This is an occasion where a nano-sized package is doing something that no small drug or protein could do, underscoring the efficacy of active nano-based drugs.”
“This is the most remarkably effective thing I’ve ever seen,” Kent said. “Literally within minutes of injecting it, the cerebral blood flow is back to normal, and we can keep it there with just a simple second injection. In the end, we’ve normalized the free radicals while preserving nitric oxide (which is essential to autoregulation). These particles showed the antioxidant mechanism we had previously identified as predictive of effectiveness.”
The first clues to PEG-HCC’s antioxidant powers came during nanoparticle toxicity studies with the MD Anderson Cancer Center. “We noticed they lowered alkaline phosphatase in the liver,” Tour said. “One of our Baylor colleagues saw this and said, ‘Hey, this looks like it’s actually causing the liver cells to live longer than normal.’
“Oxidative destruction of liver cells is normal, so that got us to thinking these might be really good radical scavengers,” Tour said.
Kent said the nanoparticles as tested showed no signs of toxicity, but any remaining concerns should be answered by further tests. The researchers found the half-life of PEG-HCCs in the blood – the amount of time it takes for half the particles to leave the body – to be between two and three hours. Tests with different cell types in vitro showed no toxicity, he said.
The research has implications for stroke victims and organ transplant patients as well, Tour said.
Next, the team hopes to have another lab replicate its positive results. “We’ve repeated it now three times, and we got the same results, so we’re sure this works in our hands,” Kent said.
First authors of the paper are BCM graduate student Brittany Bitner, Rice graduate student Daniela Marcano and former Rice postdoctoral researcher Jacob Berlin, now an assistant professor of molecular medicine at the Beckman Research Institute of the City of Hope, Duarte, Calif. Co-authors are all at BCM: Roderic Fabian, associate professor of neurology; Claudia Robertson, professor of neurosurgery; Leela Cherian, research instructor of neurosurgery; Mary Dickinson, associate professor of molecular physiology; Robia Pautler, associate professor of molecular physiology; and James Culver, a graduate student in molecular physiology.
The research was funded by the Department of Defense’s Mission Connect Mild Traumatic Brain Injury Consortium, the National Science Foundation, the National Institutes of Health and the National Heart, Lung and Blood Institute.
- See more at:
http://www.ncbi.nlm....pubmed/25675492
Nanoparticles reboot blood flow in brain
Rice University, Baylor College of Medicine discovery might aid emergency care of traumatic brain-injury victims
A nanoparticle developed at Rice University and tested in collaboration with Baylor College of Medicine (BCM) may bring great benefits to the emergency treatment of brain-injury victims, even those with mild injuries.
Combined polyethylene glycol-hydrophilic carbon clusters (PEG-HCC), already being tested to enhance cancer treatment, are also adept antioxidants. In animal studies, injections of PEG-HCC during initial treatment after an injury helped restore balance to the brain’s vascular system.
- See more at:
http://news.rice.edu...h.KknZLtJN.dpuf
Nano-antioxidants prove their potential Rice-led study shows how particles quench damaging superoxides
Injectable nanoparticles that could protect an injured person from further damage due to oxidative stress have proven to be astoundingly effective in tests to study their mechanism.
Scientists at Rice University, Baylor College of Medicine and the University of Texas Health Science Center at Houston (UTHealth) Medical School designed methods to validate their 2012 discovery that combined polyethylene glycol-hydrophilic carbon clusters — known as PEG-HCCs — could quickly stem the process of overoxidation that can cause damage in the minutes and hours after an injury.
- See more at:
http://news.rice.edu...h.pqtaFsJj.dpuf
http://news.rice.edu...low-in-brain-2/
http://news.rice.edu...ir-potential-2/
Inhibition of Metastasis by interfering with Mito-superoxide production:
Tumors are highly heterogeneous in all phenotypic features including glucose metabolism. Although glycolysis is coupled to oxidative phosphorylation (OXPHOS) in oxygenated tumor cells, some malignant cells are subject to fluctuations in oxygen availability and, therefore, rely on glycolysis uncoupled from OXPHOS for energy production (Dewhirst, 2009). From an energetic standpoint, it is surprising that some cancer cells also perform aerobic glycolysis (known as the Warburg effect), characterized by an increased normoxic flux of glucose to lactate (Warburg, 1956). However, this particular metabolic phenotype is shared with nonmalignant proliferating cells and is therefore thought to reflect increased biosynthetic plasticity (Vander Heiden et al., 2009, Ward and Thompson, 2012). Although it sometimes results from mutations (Frezza et al., 2011), there is evidence that mitochondria generally retain full oxidative capacities in solid tumors and that aerobic glycolysis can often be reverted (Faubert et al., 2013, Vaupel and Mayer, 2012), suggesting that this metabolic activity generally results from reversible changes that could be targeted pharmacologically. Thus, mitochondria actively contribute to aerobic glycolysis by producing cataplerotic intermediates and reducing equivalents to sustain cell growth and cell cycling (Anastasiou et al., 2011, Vander Heiden et al., 2009).
Tumor metastasis is a leading cause of cancer death. The metastatic switch marking the onset of metastatic dissemination corresponds to the acquisition of specific traits by tumor cells, including migration, invasion, and survival in the blood stream (Gupta and Massagué, 2006, Roussos et al., 2011). Three main lines of evidence led us to hypothesize that metastasis is under metabolic control. First, PET with the glucose analog tracer [18]-F-fluorodeoxyglucose (FDG) is routinely used for the clinical detection and imaging of tumor metastasis (Gambhir et al., 2001). This application is based on the observation that the vast majority of metastases trap far more glucose than normal tissues (with the exception of the brain), which has often been related to metabolic characteristics already acquired at the primary tumor site (Vander Heiden et al., 2009). Second, aerobic glycolysis could offer protection against oxidative damage and cell death when tumor cells transit in oxygenated blood (Porporato et al., 2011). Third, a mitochondrial defect corresponding to an inactivating mutation of respiratory chain complex I has been found in a metastatic mouse Lewis lung carcinoma cell line and was absent in weakly metastatic parental cells (Ishikawa et al., 2008a). Experimentally, the transfer of mtDNA from highly to weakly metastatic cells increased their metastatic potential in mice.
It is estimated that on average 106 tumor cells per gram of tumor are shed in the circulation daily (Chang et al., 2000). Of these cells, only a few, termed metastatic progenitors, are able to generate metastases in distant organs. In this study, we tested whether Warburg-phenotype tumor cells constitute a population of metastatic progenitors. We observed that tumor cell migration, invasion, clonogenicity, metastatic take, and spontaneous metastasis in mice are promoted by the natural selection of a mitochondrial phenotype associated with superoxide production, which was phenocopied by experimentally targeting the electron transport chain (ETC). We also report that pharmacological scavenging of mitochondrial superoxide prevents metastatic dissemination from primary orthotopic tumors in mice.
http://www.cell.com/...1247(14)00527-0
Good luck and thank you for the hard work Kmoody!
Edited by Cosmicalstorm, 01 April 2015 - 02:49 PM.
I agree with your thoughts on replication of Baati's study. I am 100% skeptical of anyone who claims such profound life extension effects until it has been confirmed many times over, preferably in my own hands. If my mice live longer on C60, well, then I will have a difficult time not believing those results won't I? I have infrastructure for a limited tox study. We don't have the pathology expertise in house to assess histology but I might be able to find a collaborator for that. But CBC, chemistry profiles, etc. are all easy to do on a regular basis.
