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American Journal of Bioscience and Bioengineering
2014; 2(5): 60-71
Published online December 02, 2014 (http://www.sciencepublishinggroup.com/j/bio)
doi: 10.11648/j.bio.20140205.11
ISSN: 2328-5885 (Print); ISSN: 2328-5893 (Online)

Review article: Oxidative stress versus antioxidants

Said M. Al-Dalaen1, Aiman I. Al-Qtaitat2
1
Department of Pharmacology, Faculty of Medicine, Mu’tah University, Karak, Jordan
2
Department of Anatomy & Histology, Faculty of Medicine, Mu’tah University, Karak, Jordan

Email address:
[email protected] (S. M. Al-Dalaen), [email protected] (A. I. Al-Qtaitat)

To cite this article:

Said M. Al-Dalaen, Aiman I. Al-Qtaitat. Review Article: Oxidative Stress Versus Antioxidants. American Journal of Bioscience and
Bioengineering. Vol. 2, No. 5, 2014, pp. 60-71. doi: 10.11648/j.bio.20140205.11

Abstract: Oxidative stress is a phenomenon that reflects an imbalance between the production of reactive oxygen species
and so-called oxidants, and their elimination by protective mechanisms. These are referred to as antioxidative systems which
can detoxify the reactive intermediates, or repair the resulting damage causing toxic effects through the production of
peroxides and free radicals that damage all cell components. Further, some reactive oxidative species act as cellular messengers
in redox signaling that can cause disruptions in normal cellular signaling mechanisms. In humans, oxidative stress is thought to
be involved in the development of atherosclerosis, neurodegenerative diseases, such as Alzheimer’s and Parkinson’s disease,
cancer, diabetes mellitus, inflammatory diseases, as well as psychological diseases or aging processes. It is presently accepted
that the reactive oxygen species can be beneficial. Depending on the type of oxidants, intensity and time of redox imbalance, as
well as on the type of cells, oxidative stress can play a role in the regulation of other important processes. This is achieved
through modulation of signal pathways, influencing synthesis of antioxidant enzymes, repair processes, inflammation, or via
the immune system, as a way to attack and kill pathogens. This limits the potential for apoptosis and cell proliferation, and thus
affects malignant processes. Imprudent administration of antioxidants may therefore have a negative impact on the organism.

Keywords: Reactive Oxygen Species, Antioxidants, Oxidative Stress, Redox Stress, Signaling

Table 1. Nomenclature of the various O2 forms [12].

1. Summary
.
Triplet Oxygen (Ground state) O-O.
Reactive oxygen species (ROS) are chemically reactive Singlet Oxygen O-O:
molecules produced by living organisms as a result of normal Superoxide .
O-O:
.
cellular metabolism. At low to moderate concentrations, they Perhydroxyl radical O-O:H
function in physiological cell processes. However, when Hydrogen peroxide H:O-O:H
Hydrogen radical H: O.
present in high concentrations, they produce adverse Hydrogen ion H: O:
modifications to cell components, such as lipids, proteins, Water H:O:H
and DNA [1-3]. The shift in the oxidant/antioxidant balance
in favor of oxidants is termed “oxidative stress.” Oxidative
stress contributes to many pathological conditions, including
cancer, neurological disorders [4] atherosclerosis,
hypertension, ischemia/perfusion [5] diabetes, acute
respiratory distress syndrome, idiopathic pulmonary fibrosis,
chronic obstructive pulmonary disease [6] and asthma [7-10].
Aerobic organisms have integrated antioxidant systems,
which include enzymatic and nonenzymatic antioxidants that
are usually effective in blocking harmful effects of ROS.
However, in pathological conditions, the antioxidant systems
can be overcomed [11].

Figure 1. The activation states of oxygen [12].

61 Said M. Al-Dalaen and Aiman I. Al-Qtaitat: Review Article: Oxidative Stress Versus Antioxidants
2. Oxidants
2.1. Endogenous Sources of Oxidants
ROS (shown in Figure 1 and table 1) are produced from
the activation of molecular oxygen, intracellularly through
multiple mechanisms, as a result of normal cellular
metabolism. Their major sources are mitochondria,
peroxisomes, endoplasmic reticulum, and the NADPH
oxidase (NOX) complex in cell membranes (Figure 2) [13,
14]. ROS can be classified as either free radicals or
nonradicals.
Molecules containing one or more unpaired electrons and
thus giving reactivity to the molecule are called free radicals.
When two free radicals share their unpaired electrons,
nonradical forms are created. The three major ROS that are
of physiological significance are superoxide anion (O2-.),
hydroxyl radical (.OH), and hydrogen peroxide (H2O2) [11].
Mitochondria convert energy into ATP—a form that can be
utilized by the cell. The ATP production process, known as
oxidative phosphorylation, involves the transport of protons
(hydrogen ions) across the inner mitochondrial membrane by
means of the electron transport chain. In the electron
transport chain, electrons are passed through a series of
proteins via oxidation-reduction reactions, with each acceptor
Figure 2. Different ROS sources [13].
protein along the chain having a greater reduction potential
than the previous one. The final destination for an electron
along this chain is an oxygen molecule. In normal conditions,
oxygen is reduced to produce water. However, in about 1–3%
[11] of electrons passing through the chain, oxygen is
prematurely and incompletely reduced, resulting in the
superoxide radical (·O2-). While superoxide is not
particularly reactive, it can inactivate specific enzymes or
initiate lipids peroxidation in its protonated form,
hydroperoxyl HO2· [15], O2- itself can also react with H2O2
and generate OH- [16]. Hydroxyl radical is the most reactive
ROS and can damage proteins, lipids, carbohydrates and
DNA. It can also initiate lipid peroxidation by taking an
electron from polyunsaturated fatty acids. Hydrogen peroxide
is also produced by xanthine oxidase, amino acid oxidase,
and NADPH oxidase [17] and in peroxisomes by
consumption of molecular oxygen in metabolic reactions. In
a succession of reactions, called Haber–Weiss and Fenton
reactions (Figure 3), H2O2 can break down to OH- in the
presence of transmission metals, such as Fe2+ or Cu2+ [18].
Fe3 + + .O2 → Fe2++ O2 Haber-Weiss
Fe2+ + H2O2→ Fe3 + + OH- + .OH Fenton reaction
 American Journal of Bioscience and Bioengineering 2014; 2(5): 60-71
Figure 3. Fenton reaction [18].
Granulocytic enzymes further expand the reactivity of
H2O2 via eosinophil peroxidase and myeloperoxidase (MPO).
In activated neutrophils, H2O2 is consumed by MPO. In the
presence of chloride ion, H2O2 is converted to hypochlorous
acid (HOCl), which is highly oxidative and plays an
important role in killing of the pathogens in the airways [19].
However, HOCl can also react with DNA, induce DNA–
protein interactions, produce pyrimidine oxidation products
and add chloride to DNA bases [20]. Eosinophil peroxidase
and MPO also contribute to the oxidative stress through
modification of proteins by halogenations, nitration, and
protein cross-links via tyrosyl radicals [21].
The peroxyl radicals (ROO..) are another type of oxygen-
derived free radicals, the simplest of which is hydroperoxyl
radical (ROO..) that plays a role in fatty acid peroxidation.
Free radicals can trigger lipid peroxidation chain reactions by
abstracting a hydrogen atom from a side chain methylene
carbon. The lipid radical then reacts with oxygen to produce
peroxyl radical. Peroxyl radical initiates a chain reaction and
transforms polyunsaturated fatty acids into lipid
hydroperoxides, which are very unstable and easily
decompose to secondary products, such as aldehydes and
malondialdehydes. Isoprostanes are another group of lipid
peroxidation products that are generated via the peroxidation
of arachidonic acid and have also been found to be elevated
in plasma and breath condensates of asthmatics [22].
2.2. Exogenous Sources of Oxidants
Exogenous ROS can be produced as a result of smoking
[23] as well as exposure to pollutants, ozone [24], hyperoxia
[25], heavy metals [26] or radiation [27]. Cigarette smoke
contains many oxidants, free radicals and organic compounds,
such as superoxide and nitric oxide [24]. Ozone exposure can
cause lipid peroxidation and induce influx of neutrophils into
the airway epithelium.
Short-term exposure to ozone also causes the release of
inflammatory mediators, such as MPO, eosinophil cationic
proteins, lactate dehydrogenase and albumin [28].
Hyperoxia refers to conditions characterized by oxygen
levels that are higher than normal partial pressure of oxygen
in the lungs or other body tissues. This leads to greater
production of reactive oxygen and nitrogen species [29].
Heavy metal ions—such as iron, copper, cadmium,
62
mercury, nickel, lead, and arsenic—can induce generation of
reactive radicals. This can cause cellular damage via
depletion of enzyme activities through lipid peroxidation and
reaction with nuclear proteins and DNA, where ROS
generated by metal-catalyzed reactions can modify DNA
bases. Three base substitutions, G → C, G → T, and C → T,
can occur as a result of oxidative damage by metal ions, such
as Fe2+, Cu2+, and Ni2+. Previous studies have shown that G
→ C can be predominantly produced by Fe2+, while C → T
substitution is typically achieved by Cu2+ and Ni2+ [30].
In the presence of O2, ionizing radiation converts hydroxyl
radical, superoxide, and organic radicals to hydrogen
peroxide and organic hydroperoxide, which can react with
redox active metal ions, such as Fe and Cu, via Fenton
reactions, and thus induce oxidative stress [31]. In addition, it
can generate damaging intermediates through interaction
with water, a process termed radiolysis. Since water
comprises 55-60% of the human body, the probability of
radiolysis is quite high under the presence of ionizing
radiation. The outcome is conversion of water into hydroxyl
radical (-OH), hydrogen peroxide (H2O2), superoxide radical
(O2-) and ultimately oxygen (O2) [32]. Moreover, according
to the findings of extant studies, various signal transduction
molecules—such as extracellular signal-regulated kinase 1
and 2 (ERK1/2), c-Jun N-terminal kinase (JNK), and p38—
and transcription factors—such as activator protein-1 (AP-1),
nuclear factor-κB (NF-κB), and p53—are activated under
effect of ionizing radiation. This results in the expression of
radiation response-related genes [33, 34].
3. Oxidative Stress-Induced Cellular
Damage
The targets of ROS damage include all major biomolecular
groups, as discussed below.
3.1. Proteins
It is well known that ROS can target almost all cellular
compounds. According to the findings of several studies,
ROS can react with several amino acid residues in vitro,
generating a wide range of products—from modified and less
active enzymes to denatured, non-functioning proteins [35].
63 Said M. Al-Dalaen and Aiman I. Al-Qtaitat: Review Article: Oxidative Stress Versus Antioxidants
Fragmentation of the peptide chain and aggregation of
cross-linked reaction products result in an altered electrical
charge and increased susceptibility to proteolysis by
degradation by specific proteases. Here, the amino acids in a
peptide differ in their susceptibility to attack, while the
various forms of activated oxygen differ in their potential
reactivity [36].
Cysteine and methionine residues in proteins are
particularly susceptible to oxidation [37]. For example,
oxidation of sulfhydryl groups or methionine residues of
proteins causes conformational changes, protein unfolding,
and degradation [38, 39]. Enzymes that have metals at or
close to their active sites are especially more sensitive to
metal catalyzed oxidation, which can inhibit their activities
[40].
3.2. Lipids
Oxidative stress can induce lipid peroxidation, causing
different arrangement in the membrane lipid bilayer. This
results in inactivation of the membrane-bound receptors and
enzymes and causes an increase in tissue permeability [41].
Products of lipid peroxidation, such as malodialdehyde and
unsaturated aldehydes, are capable of inactivating many
cellular proteins by forming protein cross-linkages [42]. This
causes depletion of intracellular GSH, induces peroxide
production [43] activates epidermal growth factor receptor
[44] and induces fibronectin production [45].
3.3. DNA
Most of the long-term effects of oxidative stress are
inflicted by modifications of DNA [46] which involves
degradation of bases, single- or double-stranded DNA breaks,
purine, pyrimidine or sugar-bound modifications, mutations,
deletions or translocations, and cross-linking with proteins.
Most of these DNA modifications are highly relevant to
carcinogenesis, aging, and neurodegenerative, cardiovascular,
and autoimmune diseases. DNA damage similar to that
induced by oxidative stress can also be induced by ionizing
radiation. Promoter regions of genes contain transcription
factor-binding sites that have consensus sequences. These
contain GC-rich sequences are susceptible for oxidant attacks,
which can change the expression of the related gene [47].
Single-base damage by radiation or oxidation, such as 8-
oxoguanine and thymine glycol, is well known. However, the
research focus has recently shifted to some of the more
complex lesions, such as tandem DNA lesions, formed at
substantial frequency by ionizing radiation and metal-
catalyzed H2O2 reactions.
Under anoxic conditions, the predominant double-base
lesion is a species in which C8 of guanine is linked to the 5-
methyl group of an adjacent 3'-thymine (G [8, 5- Me] T) [48].
Most of these oxygen-derived species are produced at a low
level by normal aerobic metabolism. As a result of oxidation,
5-methyl cytosine is converted into 5-hydroxy methyl uracil,
due to a deamination/oxidation reaction, affecting DNA
organization and repair activity [49]. Normal cellular defense
mechanisms destroy most of these and any damage to the
cells is constantly repaired. However, under the severe levels
of oxidative stress that cause necrosis, the damage causes
ATP depletion, preventing the control of cell death by
apoptosis and causing cell disintegration [50].
4. Effects of Oxidative Stress on Signal
Transduction
Oxidative stress can cause disruption of the GSH/GSSG
ratio, leading to activation of redox sensitive transcription
factors, such as the nuclear factor of activated T cells (NF-κB)
and hypoxia-inducible factor 1 (AP-1). Owing to their
involvement in inflammatory responses, these factors can
facilitate the transmission of information into the cell.
Tyrosine kinase receptors, most of the growth factor
receptors—such as epidermal growth factor receptor,
vascular endothelial growth factor receptor, and receptor for
platelet-derived growth factor—as well as protein tyrosine
phosphatases and serine/threonine kinases are targets of ROS
[51]. Moreover, oxidants can regulate many of the
extracellular signal regulated kinases, such as p38, which are
the members of mitogen-activated protein kinase family. As
such, they are involved in several processes in the cell,
including proliferation, differentiation, and apoptosis. ROS
can activate NF-κB by phosphorylating IκBs at serine
residues, which frees NF-κB to enter the nucleus to activate
gene transcription [52]. A number of kinases have been
reported to phosphorylate IκBs; these kinases are targets for
oxidative signals to activate NF-κB [53]. As a result of NF-
κB activation via oxidation, several antioxidant defense-
related genes that can participate in immune response are
activated. These include IL-1b, IL-6, tumor necrosis factor-α,
IL-8, and several adhesion molecules. NF-κB also regulates
angiogenesis, proliferation and cell differentiation [54].
5. Oxidative Stress and Diseases
5.1. Aging
In an attempt to explain the aging process, many theories
have been put forward [55, 56]. However, only the “free
radical theory of aging” [57] has gained universal acceptance,
as it is supported by the fact that the production of free
radicals and the free radical damage increases with age [58].
This theory postulates that free radicals in the body cause
oxidative damage to cellular components—a process that
results in altered cellular function, compromised tissue and
organ function, ultimately leading to death. The free radial
theory is also supported by the “rate of living” hypothesis,
which inversely links metabolic rate with the longevity of the
organisms [59]. This is supported by empirical evidence
proved by indicating that oxidative damage to proteins, DNA
and lipids increases with age [58]. As free radical-mediated
oxidative stress increases with age, it may overwhelm the
natural repair systems in the elderly [60]. Thus, it is a major
contributor to diseases associated with aging [61].
 American Journal of Bioscience and Bioengineering 2014; 2(5): 60-71
5.2. Cardiovascular Disease
Vascular proliferation and inflammation are closely linked
[62] and excessive proliferation of vascular cells plays an
important role in the pathology of vascular occlusive disease.
Free radicals are considered to play a causal role in this
process [63]. ROS lead to the oxidation of low density
lipoprotein, which accumulates within plaques. It thus
contributes to the inflammatory state of atherosclerosis and
plays a key role in its pathogenesis [64]. Oxidized-LDL leads
to endothelial dysfunction, and can result in either cell
growth or apoptotic cell death, causing vasoconstriction. Free
radicals have also been implicated in congestive heart failure
[65].
5.3. Diabetes
Findings of pertinent studies indicate that free radical-
induced damage also plays a role in the development of
insulin resistance, β-cell dysfunction, impaired glucose
tolerance, and type II diabetes mellitus [66]. Hyperglycemia
can induce oxidative stress through several mechanisms,
including glucose autoxidation, the formation of advanced
glycation end-products (AGEs), and activation of the polyol
pathway [67]. In diabetics, a significant increase in protein
glycation (AGE) has been noted. Moreover, evidence
suggests that, owing to their accumulation, prevalence of
microvascular lesions increases. These are present in diabetic
retinopathy, and are also responsible for cardiovascular
complications in diabetic patients [67, 68]. The damage
caused by ROS has also been implicated in primary open
angle glaucoma (POGA), which is the leading cause of
irreversible blindness [69].
5.4. Cancer
ROS can activate the initiation, promotion and progression
stages of carcinogenesis [70] due to the interaction between
free radicals and DNA components. By damaging its bases
and the deoxyribose backbone, it causes mutations in crucial
genes, thus leading to cancer [71]. In support of this free
radical-mediated damage to DNA, either through arrest or
induction of transcription, induction of signal transduction
pathways, replication errors, and genomic instability occurs.
All these phenomena are associated with carcinogenesis [49]
which has been found in various cancer tissues. Moreover,
there is a direct link between the size of benign tumors and
the amount of DNA oxidized product, 8-hydroxyguanine (8-
OH-G) adduct formation. Understanding this process may be
important in explaining the transformation of benign to
malignant tumors [72]. In cancer cells, the high level of
oxidative stress can induce apoptosis or even necrosis, while,
its low level can stimulate cell division and thus promote
tumor growth [73].
5.5. Neurodegenerative Diseases
A growing body of evidence indicates that free radicals are
involved in the initiation of cellular injury observed in
64
neurodegenerative diseases [74] which are characterized by
loss of specific neuronal populations. This is often
accompanied by intraneuronal damage, as well as
extracellular accumulation of fibrillary materials.
5.6. Parkinson’s Disease
This progressive neurodegenerative movement disorder is
considered the most common form of motor system
degeneration, affecting approximately 1% of the population
over the age of 65 [75]. Empirical evidence suggests the
involvement of free radicals in the pathogenesis of this
disease. It has been observed that that oxidation of dopamine
yields potentially toxic semiquinones. Moreover, the
accelerated metabolism of dopamine by monoamine-oxidase-
B may induce an excessive formation of hydrogen peroxide,
superoxide anions, and hydroxyl radicals, which not only
maintain the oxidative stress level, but also initiate/propagate
apoptosis of the dopaminergic neurons [76]. According to the
reports in the pertinent literature, Parkinson's disease is
associated with increased oxidative damage to DNA [77],
proteins [78] and lipids [79].
5.7. Huntington’s Disease
This inherited autosomal dominant neurodegenerative
disease is characterized by uncontrollable movements,
irritability and depression [80]. There is a direct evidence to
support the involvement of free radicals in the pathogenesis
of Huntington’s disease, in that increased levels of F2-
isoprostanes have been detected in the cerebrospinal fluid of
the patients compared to those measured in the healthy
persons [81].
5.8. Alzheimer’s Disease
This neurodegenerative disorder is characterized by
cognitive impairment and a gradual loss of memory,
language skills, and dementia. It eventually leads to death
due to the loss of neurons and synapses [82]. Oxidative
damage may play a role in amyloid deposition in Alzheimer’s
disease, and oxidizing conditions can cause protein cross-
linking and aggregation of β-amyloid protein, tau and other
cytoskeletal proteins [83]. The accumulated β-amyloid can
cause oxidation of the nonsaturated carbohydrate side chains
of membrane lipids, which leads to the disintegration of the
neural membrane. The outcome of this process is cell lysis
due to lipid peroxidation [84] which is associated with DNA
damage and oxidative modification of proteins in the frontal
cortex of brain affected by Alzheimer’s disease [85].
5.9. Stroke
In the patients that have suffered stroke, neuronal death is
caused by the free radicals arising from various sources, such
as xanthine oxidase, cyclooxygenase, inflammatory cells and
mitochondria [86]. The mitochondrial electron transport
chain is altered during ischemia and reperfusion and is also a
likely source of free radicals. This can result in increased
formation of superoxide radical anions [87].
65 Said M. Al-Dalaen and Aiman I. Al-Qtaitat: Review Article: Oxidative Stress Versus Antioxidants
The accumulation of blood borne inflammatory cells, such
as neutrophils and monocytes/macrophages, which can occur
during reperfusion, can also promote further oxidative stress.
This can cause lipid peroxidation and oxidative damage to
DNA in ischemic stroke patients [88]. In addition; increased
ROS levels can make the brain more susceptible to oxidative
stress due to a variety of reasons. For example, the brain
could consume a significant amount of the body’s oxygen
supply, or have a relatively poor antioxidant defense system.
Alternatively, it could be enriched in pro-oxidant molecules
or contain high concentration of readily peroxidizable lipids
[89].
6. Antioxidants
Humans have evolved complex antioxidants strategies
against prooxidant conditions. The antioxidant defensive
system has many components, and a deficiency of any of
these components can cause destruction in the overall
antioxidant status of an individual [90]. Antioxidants are the
molecules that have the ability to counterbalance the effects
Figure 4. Mutual association between oxidants and antioxidants [92].
6.1. Enzymatic Antioxidants
The major enzymatic antioxidants found in the lungs are
superoxide dismutases (SODs) (EC 1.15.1.11), catalase (EC
1.11.1.6), glutathione peroxidases (GSH-Pxs) (EC 1.11.1.9)
and glutathione-S-transferase (GSTs) (EC 2.5.1.18) [93]. In
addition to these major enzymes, other antioxidants,
including heme oxygenase-1 (EC 1.14.99.3), and redox
proteins, such as thioredoxins (TRXs, EC 1.8.4.10),
peroxiredoxins (PRXs, EC 1.11.1.15), and glutaredoxins,
have been found to play crucial roles in the pulmonary
antioxidant defenses.
Since superoxide is the primary ROS produced in a variety
of sources, its dismutation by SOD is of primary importance
for each cell. All three forms of SOD—CuZn-SOD, Mn-SOD,
and EC-SOD—are widely expressed in human tissues [94].
Mn-SOD is localized in the mitochondria matrix. EC-SOD is
primarily localized in the extracellular matrix, especially in
of oxidants before these attacks the cells (Figure 4). There are
highly complex antioxidant systems (enzymatic and
nonenzymatic) in human cells, working in collaboration in
other to protect the body against free radical damage.
Antioxidants can be endogenous or obtained exogenously,
as a part of a diet or through dietary supplements. They can
also be consumed as compounds that do not neutralize free
radicals, but rather enhance endogenous activity.
An ideal antioxidant should be readily absorbed, quench
free radicals, and chelate redox metals. It should also work in
both aqueous and/or membrane domains, positively affecting
gene expression.
Endogenous antioxidants play a crucial role in maintaining
optimal cellular functions. However, under conditions that
promote oxidative stress, endogenous antioxidants may not
be sufficient. In such cases, dietary antioxidants should be
supplied to maintain optimal cellular functions. Some
antioxidants can interact with other antioxidants,
regenerating their original properties. This process is referred
to as the “antioxidant network.” [91].
areas containing high amounts of type I collagen fibers and
around pulmonary and systemic vessels. It has also been
detected in the bronchial epithelium, alveolar epithelium, and
alveolar macrophages [95]. Overall, CuZn-SOD and Mn-
SOD are generally thought to act as bulk scavengers of
superoxide radicals. The relatively high EC-SOD level in the
lung with its specific binding to the extracellular matrix
components may represent a fundamental component of lung
matrix protection [96].
Cu, Zn-SOD has two identical subunits, with a molecular
weight of 32 kDa. Each subunit contains a dinulcear metal
cluster, comprising of copper and zinc ions as the active site,
and it specifically catalyzes the dismutation of the superoxide
anion to oxygen and water [97]. The mitochondrial Mn-SOD
is a homotetramer with a molecular weight of 96 kDa and
contains one manganese atom per subunit. It vacillates from
Mn (III) to Mn (II) and back to Mn (III) during the two-step
 American Journal of Bioscience and Bioengineering 2014; 2(5): 60-71
dismutation of superoxide [97]. Extra-cellular superoxide
dismutase contains copper and zinc. It is a tetrameric
secretary glycoprotein, characterized by a high affinity for
certain glycosaminoglycans, such as heparin and heparin
sulphate. However, its regulation in mammalian tissues
occurs primarily in a manner coordinated by cytokines, rather
than as a response to oxidative stress [97].
H2O2 produced by the action of SODs or oxidases, such as
xanthine oxidase, is reduced to water by catalase and the
GSH-Px. Catalase exists as a tetramer composed of four
identical monomers, each of which contains a heme group at
the active site. Degradation of H2O2 is accomplished via the
conversion between two conformations of catalase-
ferricatalase (iron coordinated to water) and compound I
(iron complexed with an oxygen atom). Catalase also binds
NADPH as a reducing equivalent to prevent oxidative
inactivation of the enzyme (formation of compound II) by
H2O2 as it is reduced to water [98]. Catalase has one of the
highest turnover rates of all enzymes; one molecule of
catalase can convert approximately 6 million molecules of
hydrogen peroxide to water and oxygen each minute [97].
The GSH-Pxs are a family of tetrameric enzymes that contain
the unique amino acid selenocysteine within the active sites
and use glutathione (GSH) to reduce H2O2 and lipid
peroxides to their corresponding alcohols. While four
GSHPxs have been described, encoded by different genes,
GSHPx-1 (cellular GSH-Px) is ubiquitous. It reduces H2O2
and fatty acid peroxides, but not esterified peroxyl lipids [99].
Esterified lipids are reduced by membrane-bound GSH-Px-4
using several different thiols as reducing equivalents. GSH-
Px-2 (gastrointestinal GSH-Px) is localized in gastrointestinal
epithelial cells, where it serves to reduce dietary peroxide
levels [100]. GSH-Px-3 (extracellular GSH-Px) is the only
member of the GSH-Px family that resides in the
extracellular compartment and is believed to be one of the
most important extracellular antioxidant enzymes in
mammals [101].
GSTs can inactivate secondary metabolites, such as
unsaturated aldehydes and hydroperoxides. Presently, three
major families of GSTs are recognized—cytosolic GST,
mitochondrial GST [102, 103] and membrane-associated
microsomal GST that plays a role in eicosanoid and GSH
metabolism [104]. During non-stressed conditions, Mu and
Pi classes of cytosolic GSTs can interact with kinases Ask1
and JNK, respectively, resulting in their inhibition [105]. The
dissociation of GSTP1 from JNK in response to oxidative
stress [106] results in the recovery of peroxiredoxin VI (PRX
VI) enzyme activity through glutathionylation of the oxidized
protein [107].
The enzymatic antioxidants also include six different types
of PRXs, each playing a major role in the protection of
alveolar epithelium, PRX VI in particular [108]. PRX V has
been found to function as a peroxynitrite reductase [109];
according to some authors, it may also function as a potential
protective compound in the development of ROS-mediated
lung injury [110].
66
6.2. Nonenzymatic Antioxidants
6.2.1. Vitamin E (α-Tocopherol)
This fat-soluble vitamin is considered a major powerful
membrane-bound antioxidant, employed by the cell [111] as a
protection against lipid peroxidation [112]. During the
antioxidant reaction, α-tocopherol is converted into α-
tocopherol radical by the donation of labile hydrogen to a
lipid or lipid peroxyl radical. Thus, the α-tocopherol radical
can be reduced to the original α-tocopherol form by ascorbic
acid [113].
6.2.2. Vitamin C (Ascorbic Acid)
As it is water-soluble, Vitamin C acts in the aqueous
environments of the body, along with the antioxidant
enzymes. Vitamin C cooperates with Vitamin E to regenerate
α-tocopherol from α-tocopherol radicals in membranes and
lipoproteins [112] (Figure 5). By raising intracellular
glutathione levels, it also plays an important role in protein
thiol group protection against oxidation [114]. Yuanyuan et al.
(2014) [115] reported that vitamin C decreased ROS and
DNA damage of severe CAP PBMC in vitro, and vitamin C
decreased TNF-α and IL-6 in whole blood cells from severe
CAP.
Figure 5. Ascorbic acid – antioxidant and potential prooxidant properties
[92].
6.2.3. Carotenoids (β-Carotene)
These are mainly colored pigments present in plants and
microorganisms. Epidemiological studies have revealed that
a diet rich in carotenoids is correlated with a lower risk of
age-related diseases [116]. Primarily, β-carotene has been
found to react with peroxyl (ROO.) to prevent damage in
lipophilic compartments [117] hydroxyl (.OH), and
superoxide (O2-.) radicals [118]. The antioxidant activity of
carotenoids arises due to their ability to delocalize unpaired
electrons, and thus quench singlet oxygen without
degradation [119]. The efficacy of carotenoids with respect to
physical quenching is related to the number of conjugated
double bonds present in the molecule. Both β-Carotene and
retinoic acid are capable of regulating different transcription
factors [120], β-Carotene inhibits the oxidant-induced NF-κB
activation and interleukin (IL)-6 and tumor necrosis factor-α
production. On the other hand, retinoic acid can affect cell
apoptosis, arrest cell cycle, or both [121, 122].
67 Said M. Al-Dalaen and Aiman I. Al-Qtaitat: Review Article: Oxidative Stress Versus Antioxidants
6.2.4. Thiol Antioxidants
Glutathione (GSH) is the major thiol-disulphide redox
intracellular multifunctional soluble antioxidant of the cell. It
can be found abundant in cytosol, nuclei, and mitochondria
[123]. It can be found in the reduced form, i.e., as GSH, or in
the oxidized form, known as GSSG (glutathione disulphide).
The antioxidant capacity of thiol compounds is attributed to
the presence of sulfur atom, which can easily accommodate the
loss of a single electron [124]. As oxidized glutathione (GSSG)
is accumulated inside the cells, the GSH/GSSG ratio is a
reliable indicator of oxidative stress of an organism [125]. It
can act as a co-factor for several detoxifying enzymes,
participate in amino acid transport across plasma membrane,
scavenge hydroxyl radical and singlet oxygen directly, and
regenerate Vitamin C and E back to their active forms [123]. In
addition, evidence suggests that GSH protects cells against
apoptosis by interacting with proapoptotic and antiapoptotic
signaling pathways. It also regulates and activates several
transcription factors, such as AP-1, NF-κB, and Sp-1 [123].
Thioredoxin (TRX) is another thiol antioxidant with
oxidoreductase and ubiquitous activity in both mammalian and
prokaryotic cells. In its reduced form, it contains two adjacent
–SH groups that are converted to a disulphide unit in oxidized
TRX when it undergoes redox reactions with multiple proteins.
TRX and GSH may have overlapping as well as
compartmentalized functions in the activation and regulation
of transcription factors [1]. α -Lipoic is another thiol
disulphide derivative of octanoic acid antioxidant. It is both
water- and fat-soluble and is widely distributed in both cellular
membranes and the cytosol of eukaryotic and prokaryotic cells
[126]. Thus, it is readily absorbed from the diet and is
converted rapidly to its reduced form, dihydrolipoic acid,
which is a stronger antioxidant than lipoic acid. Both α-Lipoic
and dihydrolipoic acids are powerful antioxidants. They can
scavenge free radicals, chelate metal ion, act in recycling
antioxidants and repair protein damage due to oxidative stress
either in the cytosol or hydrophobic domains [127].
6.2.5. Melatonin
This is a neurohormone that is derived from tryptophan
mainly in the pineal gland. One of the major functions of
melatonin is scavenging free radicals in oxygen metabolism,
thereby potentially protecting against free radical-induced
damage to DNA, proteins and membranes. Owing to these
properties, it has the potential to play an important role in the
reduction of free radical-mediated diseases [128].
7. Conclusion
Extant research has led to a universal agreement that
oxidative damage to proteins, lipids, and DNA occurs as a
result of ROS overproduction. These are highly reactive due
to the unpaired electrons in their structure that allow them to
react with several biological macromolecules in cell, thus
altering their functions. ROS are produced by cellular
metabolic reactions that use oxygen and shift the balance in
oxidant/antioxidant status in favor of the oxidants. In
addition, a variety of environmental factors, such as air
pollutants or cigarette smoke, can result in the production of
ROS, which can also affect the expression of several genes
by upregulation of redox-sensitive transcription factors and
chromatin remodeling through alteration in histone
acetylation/deacetylation. The human body deals with the
pathological effects of ROS by utilizing the endogenous
antioxidant enzymatic system and by the ingestion of
exogenous antioxidants in the diet. If the oxidative stress
exceeds the protection afforded by antioxidants, the aging
process and some of the diseases associated with it—such as
cardiovascular diseases, neurodegenerative diseases, diabetes
and cancer — can accelerate. Regulation of redox state is
critical for cell viability, activation, and proliferation, as well
as organ function.
References
[1] Valko M, Rhodes CJ, Moncol J, Izakovic M, Mazur M. Free
radicals, metals and antioxidants in oxidative stress-induced
cancer. Chem. Biol. Interact., 2006; 160:1–40.
[2] Marnett LJ. Lipid peroxidation dDNA damage by
malondialdehyde. Mutat. Res., 1999; 424:83–95.
[3] Stadtman ER. Role of oxidant species in aging. Curr. Med.
Chem., 2004; 11:1105–1112
[4] Jenner P. Oxidative stress in Parkinson’s disease. Ann Neurol.,
2003; 53: S26–S36.
[5] Kasparova S, Brezova V, Valko M, Horecky J, Mlynarik V, et
al. Study of the oxidative stress in a rat model of chronic brain
hypoperfusion. Neurochem. Int., 2005; 46:601–611.
[6] Asami S, Manabe H, Miyake J, Tsurudome Y, Hirano T, et al.
Cigarette smoking induces an increase in oxidative DNA
damage, 8-hydroxydeoxyguanosine, in a central site of the
human lung. Carcinogenesis. 1997; 18:1763–1766.
[7] Comhair SA, Ricci KS, Arroliga M, Lara AR, Dweik RA, et al.
Correlation of systemic superoxide dismutase deficiency to
airflow obstruction in asthma. Am. J. Respir. Crit. Care Med.,
2005; 172:306–313.
[8] Dut R, Dizdar EA, Birben E, Sackesen C, Soyer OU, Besler T,
Kalayci O. Oxidative stress and its determinants in the
airways of children with asthma. Allergy. 2008; 63:1605–1609.
[9] Ercan H, Birben E, Dizdar EA, Keskin O, Karaaslan C, et al.
Oxidative stress and genetic and epidemiologic determinants
of oxidant injury in childhood asthma. J. Allergy Clin.
Immunol., 2006; 118:1097–1104.
[10] Fitzpatrick AM, Teague WG, Holguin F, Yeh M, Brown LA.
Severe Asthma Research Program. Airway glutathione
homeostasis is altered in children with severe asthma:
evidence for oxidant stress. J Allergy Clin Immunol. 2009;
123:146–152.
[11] Esra B, Umit S, Cansin S, Serpil E and Omer K. Oxidative
Stress and Antioxidant Defense. WAO Journal 2012; 5:9–19
[12] Fatmah AM, Siti BB, Zariyantey AH, Nasar A and Jamaludin
M. The Role of Oxidative Stress and Antioxidants in Diabetic
Complications. SQU Med J, 2012; 12: 5-18.
 American Journal of Bioscience and Bioengineering 2014; 2(5): 60-71
[13] Han D, Williams E, Cadenas E. "Mitochondrial respiratory
chain-dependent generation of superoxide anion and its
release into the intermembrane space". Biochem., J. 2001; 353
(Pt 2): 411–6.
[14] Li X, Fang P, Mai J, "et al. "Targeting mitochondrial reactive
oxygen species as novel therapy for inflammatory diseases
and cancers". J. Hematol. Oncol., 2013; 6 (19).
[15] Van Raamsdonk JM, Hekimi S. "Deletion of the mitochondrial
superoxide dismutase sod-2 extends lifespan in
Caenorhabditis elegans". PLoS Genet., 2009; 5 (2): e1000361.
[16] Liochev SI, Fridovich I. The Haber–Weiss cycled70 years
later: an alternative view. Redox Rep., 2002; 7:55–57.
[17] Granger DN. Role of xanthine oxidase and granulocytes in
ischemia reperfusion injury. Am. J. Physiol., 1988;
255:H1269–H1275.
[18] Fenton HJH. Oxidation of tartaric acid in the presence of iron.
J. Chem. Soc., 1984; 65:899–910.
[19] Klebanoff SJ. Myeloperoxidase: friend and foe. J. Leukoc.
Biol., 2005; 77:598–625.
[20] Kulcharyk PA, Heinecke JW. Hypochlorous acid produced by
the myeloperoxidase system of human phagocytes induces
covalent cross-links between DNA and protein. Biochemistry
2001; 40:3648–3656.
[21] Brennan ML, Wu W, Fu X, Shen Z, Song W, et al. A tale of
two controversies: defining both the role of peroxidases in
nitrotyrosine formation in vivo using eosinophil peroxidase
and myeloperoxidase deficient mice, and the nature of
peroxidase-generated reactive nitrogen species. J. Biol. Chem.,
2002; 277:17415–17427.
[22] Wood LG, Fitzgerald DA, Gibson PG, Cooper DM, Garg ML.
Lipid peroxidation as determined by plasma isoprostanes is
related to disease severity in mild asthma. Lipids 2000;
35:967–974.
[23] Cho AK, Sioutas C, Miguel AH, Kumagai Y, Schmitz DA, et
al. Redox activity of airborne particulate matter at different
sites in the Los Angeles Basin. Environ. Res., 2005 ; 99:40–47.
[24] Church DF, Pryor WA. Free-radical chemistry of cigarette
smoke and its toxicological implications. Environ Health
Perspect., 1985’ 64:111–126.
[25] Comhair SA, Thomassen MJ, Erzurum SC. Differential
induction of extracellular glutathione peroxidase and nitric
oxide synthase 2 in airways of healthy individuals exposed to
100% O2 or cigarette smoke. Am J Respir Cell Mol Biol.
2000; 23:350–354.
[26] Stohs SJ, Bagchi D. Oxidative mechanisms in the toxicity of
metal ions. Free Radic. Biol. Med., 1995; 18:321–336.
[27] Chiu SM, Xue LY, Friedman LR, Oleinick NL. Copper ion-
mediated sensitization of nuclear matrix attachment sites to
ionizing radiation. Biochemistry. 1993; 32:6214–6219
[28] Hiltermann JT, Lapperre TS, van Bree L, Steerenberg PA,
Brahim JJ, et al. Ozone-induced inflammation assessed in
sputum and bronchial lavage fluid from asthmatics: a new
noninvasive tool in epidemiologic studies on air pollution and
asthma. Free Radic. Biol. Med., 1999; 27:1448–1454.
[29] Matthay MA, Geiser T, Matalon S, Ischiropoulos H. Oxidant-
mediated lung injury in the acute respiratory distress
68
syndrome. Crit Care Med. 1999; 27:2028–2030.
[30] Reid TM, Feig DI, Loeb LA. Mutagenesis by metal-induced
oxygen radicals. Environ. Health Perspect., 1994; 102 (suppl
3):57–61.
[31] Biaglow JE, Mitchell JB, Held K. The importance of peroxide
and superoxide in the X-ray response. Int. J. Radiat. Oncol.
Biol. Phys., 1992; 22:665–669.
[32] Guo G, Yan-Sanders Y, Lyn-Cook BD, Wang T, Tamae D, et al.
Manganese superoxide dismutase-mediated gene expression in
radiation induced adaptive responses. Mol. Cell Biol., 2003;
23:2362–2378.
[33] Azzam EI, de Toledo SM, Spitz DR, Little JB. Oxidative
metabolism modulates signal transduction and micronucleus
formation in bystander cells from a-particle irradiated normal
human fibroblasts. Cancer Res., 2002; 62:5436–5442.
[34] Dent P, Yacoub A, Fisher PB, Hagan MP, Grant S. MAPK
pathways in radiation responses. Oncogene. 2003; 22:5885–
5896
[35] Butterfield DA, Howard B, Subramaniam R, Hall N, Hensley
K, Yatin S, et al. Structural and functional changes in proteins
induced by free radicalmediated oxidative stress and
protective action of the antioxidants N-tert-butyl-alpha-
phenylnitrone and vitamin E. Ann. N. Y. Acad. Sci., 1998;
854:448–62.
[36] Oxidative stress. From: http://www.plantstress.com/ Articles.
1996; Accessed
[37] Dean RT, Roberts CR, Jessup W. Fragmentation of
extracellular and intracellular polypeptides by free radicals.
Prog. Clin. Biol. Res., 1985; 180:341–350
[38] Keck RG. The use of t-butyl hydroperoxide as a probe for
methionine oxidation in proteins. Anal. Biochem., 1996;
236:56–62.
[39] Lyras L, Cairns NJ, Jenner A, Jenner P, Halliwell B. An
assessment of oxidative damage to proteins, lipids, and DNA
in brain from patients with Alzheimer’s disease. J.
Neurochem., 1997; 68:2061–2069.
[40] Stadtman ER. Metal ion-catalyzed oxidation of proteins:
biochemical mechanism and biological consequences. Free
Radic. Biol. Med., 1990; 9:315–325.
[41] Giugliano D, Ceriollo A, Paolisso G. Oxidative stress and
diabetic vascular complications. Diabetes Care 1996; 19:257-
67.
[42] Esterbauer H, Koller E, Slee RG, Koster JF. Possible
involvement of the lipid-peroxidation product 4-
hydroxynonenal in the formation of fluorescent chromolipids.
Biochem. J. 1984; 239:405–409
[43] Uchida K, Shiraishi M, Naito Y, Torii Y, Nakamura Y, Osawa
T. Activation of stress signaling pathways by the end product
of lipid peroxidation. 4-hydroxy-2-nonenal is a potential
inducer of intracellular peroxide production. J. Biol. Chem.,
1999; 274:2234–2242
[44] Suc I, Meilhac O, Lajoie-Mazenc I, Vandaele J, Jurgens G,
Salvayre R, Negre-Salvayre A. Activation of EGF receptor by
oxidized LDL. FASEB J. 1998; 12:665–671.
[45] Tsukagoshi H, Kawata T, Shimizu Y, Ishizuka T, Dobashi K,
Mori M. 4-Hydroxy-2-nonenal enhances fibronectin
69 Said M. Al-Dalaen and Aiman I. Al-Qtaitat: Review Article: Oxidative Stress Versus Antioxidants
production by IMR-90 human lung fibroblasts partly via
activation of epidermal growth factor receptor-linked
extracellular signal-regulated kinase p44/42 pathway.
Toxicol .Appl. Pharmacol., 2002; 184:127–135.
[46] Sies, H. "Oxidative stress: introductory remarks". In H. Sies,
(Ed.). Oxidative Stress. London: Academic Press. 1985; pp. 1–
7.
[47] Ghosh R, Mitchell DL. Effect of oxidative DNA damage in
promoter elements on transcription factor binding. Nucleic
Acids Res., 1999; 27:3213–3218.
[48] Docampo, R. "Antioxidant mechanisms". In J. Marr and M.
Müller, (Eds.). Biochemistry and Molecular Biology of
Parasites. London: Academic Press. 1995; pp. 147–160.
[49] Cooke MS, Evans MD, Dizdaroglu M, Lunec J. 2003.
Oxidative DNA damage: mechanisms, mutation, and disease.
FASEB J. 17:1195–1214.
[50] Seaver LC, Imlay JA. "Are respiratory enzymes the primary
sources of intracellular hydrogen peroxide?". J. Biol. Chem.,
2004; 279 (47): 48742–50.
[51] Sun T, Oberley LW. Redox regulation of transcriptional
activators. Free Radic. Biol. Med., 1996; 21:335–348.
[52] Perkins ND. Integrating cell-signalling pathways with NF-
kappaB and IKK function. Nat. Rev. Mol. Cell Biol., 2007;
8:49–62.
[53] Gilmore TD. Introduction to NF-kappaB: players, pathways,
perspectives. Oncogene. 2006; 25:6680–6684.
[54] Akira S, Kishimoto A. NF-IL6 and NF-kB in cytokine gene
regulation. Adv. Immunol., 1997; 65:1–46.
[55] Balaban RS, Nemoto S, Finkel T. Mitochondria, Oxidants, and
Aging. Cell Vol, 2005; 120:483–95.
[56] Sohal RS, Mockett RJ, Orr WC. Mechanisms of Aging: An
appraisal of the oxidative stress hypothesis. Free Rad. Biol.
Med., 2002; 33:575–86
[57] Harman D. Ageing: a theory based on free radical and
radiation chemistry. J. Gerontol., 1956; 2:298–300.
[58] Sohal RS, Weindruch R. Oxidative stress, caloric restriction,
and ageing. Science, 1996; 273:59–63.
[59] Ku HH, Brunk UT, Sohal RS. Relationship between
mitochondrial superoxide and hydrogen peroxide production
and longevity of mammalian species. Free Rad. Biol. Med.,
1993; 15:621–7.
[60] Kowald A, Kirkwood TB. Accumulation of defective
mitochondria through delayed degradation of damaged
organelles and its possible role in ageing of post-mitotic and
dividing cells. J. Theor. Biol., 2000; 202:145–60.
[61] Ames BN, Shigenaga MK, Hagen TM. Oxidants, antioxidants
and degenerative diseases of aging. Proc. Natl. Acad. Sci.,
1993; 90:7915–22.
[62] Dzau VJ, Braun-Dullaeus RC, Sedding DG. Vascular
proliferation and atherosclerosis: new perspectives and
therapeutic strategies. Nat. Ned., 2002; 8:1249–56.
[63] Schachinger V, Zeiher AM. Atherogenesis-recent insights into
basic mechanisms and their clinical impact. Nephrol. Dial.
Transplant., 2002; 17:2055–64
[64] Galle J, Hansen-Hagge T, Wanner C, Seibold S. Impact of
oxidized low density lipoprotein on vascular cells.
Atherosclerosis, 2006; 185:219–26.
[65] Elahi MM, Matata BM. Free radicals in blood: Evolving
concepts in the mechanism of ischemic heart disease. Arch.
Biochem. Biophys., 2006; 450:78–88.
[66] Wright Ejr, Scism-Bacon JL, Glass LC. Oxidative stress in
type 2 diabetes: the role of fasting and postprandial glycemia.
Int. J. Clin. Prac., 206; 60:308–14.
[67] Jay D, Hitomi H, Griendling KK. Oxidative stress and
diabetic cardiovascular complications. Free Rad. Biol. Med.,
2006; 40:183–92.
[68] Wautier JL, Schmidt AM. Protein glycation. Circulation Res,
2004; 95:233–8.
[69] Izzotti A, Bagnis A, Saccà SC. The role of oxidative stress in
glaucoma. Mutation Res., 2006; 612:105–14.
[70] Klaunig JE, Kamendulis LM. The role of oxidative stress in
carcinogenesis. Ann. Rev. Pharmacol. Toxicol., 2004; 44:239–
67.
[71] Dizdaroglu M, Jaruga P, Birincioglu M, et al. Free-radical-
induced damage to DNA: mechanisms and measurement. Free
Rad. Bio. Med., 202; 32:1102–15.
[72] Loft S, Poulsen HE. Cancer risk and oxidative DNA damage
in man. J. Mol. Med., 1996; 74:297–312.
[73] Dreher D, Junod AF. Role of oxygen free radicals in cancer
development. Eur. J. Cancer, 1996; 32A:30–8.
[74] Emerit J, Edeas M, Bricaire F. Neurodegenerative diseases
and oxidative stress. Biomed. Pharmacother., 2004; 58:39–46.
[75] Moore DJ, West AB, Dawson VL, et al. Molecular pathology
of Parkinson’s disease. Annu. Rev. Neurosci., 2005; 28:57–87.
[76] Hald A, Lotharius J. Oxidative stress and inflammation in
Parkinson’s disease: is there a causal link? Exp. Neurol., 2005;
193:279–90.
[77] Migliore L, Petrozzi L, Lucetti C, et al. Oxidative damage and
cytogenetic analysis in leukocytes of Parkinson’s disease
patients. Neurology, 2002; 58:1809–15.
[78] Choi J, Sullards MC, Olzmann JA, et al. Oxidative damage of
DJ-1 is linked to sporadic Parkinson and Alzheimer diseases. J.
Biol. Chem., 2006; 281:10816–24.
[79] Agil A, Durản R, Barrero F, et al. Plasma lipid peroxidation in
sporadic Parkinson’s: Role of the L-dopa. J. Neuro. Scien.,
2006; 240:31–6.
[80] Margolis RL, Ross CA. Diagnosis of Huntington’s disease.
Clin. Chem., 2003 ; 49:1726–32.
[81] Montine TJ, Beal MF, Robertson D, et al. Cerebrospinal fluid
F2-isoprostanes are elevated in Huntington’s disease.
Neurology, 1999; 52:1104–5.
[82] Selkoe DJ. Alzheimer disease: mechanistic understanding
predicts novel therapies. Ann. Intern. Med., 2004; 140:627–38.
[83] Troncoso JC, Costello A, Watson AL et al. In vitro
polymerization of oxidized tau into filaments. Brain Res.,
1993; 613:313–6.
 American Journal of Bioscience and Bioengineering 2014; 2(5): 60-71
[84] Völkel W, Sicilia T, Pähler A, et al. Increased brain levels of
4-hydroxy-2-nonenal glutathione conjugates in severe
Alzheimer’s disease. Neurochem. Intern., 2006; 48:679–686.
[85] Korolainen MA, Goldsteins G, Tuula A, et al. Oxidative
modification of proteins in the frontal cortex of Alzheimer’s
disease brain. Neuro. Biol. Aging, 2006; 27:42–53.
[86] Alexandrova M, Bochev P, Markova V, et al. Dynamics of free
radical processes in acute ischemic stroke: influence on
neurological status and outcome. J. Clin. Neurosci., 2004;
11:501–6.
[87] Simms NR, Anderson MF. Mitochondrial contributions to
tissue damage in stroke. Neurochem. Int., 2002; 40:511–26.
[88] Mariani E, Polidori MC, Cherubini A, et al. Oxidative stress in
brain aging, neurodegenerative and vascular diseases: An
overview. J. Chromat. B, 2005; 827:65–75
[89] Cherubini A, Ruggiero C, Cristina M, et al. Potential markers
of oxidative stress in stroke. Free Rad. Biol. Med., 2005;
39:841–52.
[90] Yanli L., Richard W. B., Matthew R. B., Furong D., Lili T. and
Lina M. Positive Relationship between Total Antioxidant
Status and Chemokines Observed in Adults. Oxidative
Medicine and Cellular Longevity Article ID 693680, 2014; 6
pages
[91] Sies H, Stahl W, Sevanian A. Nutritional, dietary and post-
prandial oxidative stress. J. Nutr., 2005; 135:969–72.
[92] Ďuračková Z. Some current insights into oxidative Stress
(Review). Physiol. Res., 2010 ; 59: 459-469
[93] Halliwell, B.; Gutteridge, J.M.C. Free Radicals in Biology and
Medicine; 2007; Clarendon Press: Oxford, UK.
[94] Landis GN, Tower J. Superoxide dismutase evolution and life
span regulation. Mech. Ageing Dev., 2005; 126:365–79.
[95] Kinnula VL. Production and degradation of oxygen
metabolites during inflammatory states in the human lung.
Curr. Drug Targets Inflamm. Allergy. 2005; 4:465–470
[96] Zelko IN, Mariani TJ, Folz RJ. Superoxide dismutase
multigene family: a comparison of the CuZn-SOD (SOD1),
Mn-SOD (SOD2), and EC-SOD (SOD3) gene structures,
evolution, and expression. Free Radic. Biol. Med., 2002;
33:337–349.
[97] Mates JM, Perez-Gomez C and De Castro IN. Antioxidant
enzymes and human diseases. Clin. Biochem., 999 ; 132:595–
603.
[98] Kirkman HN, Rolfo M, Ferraris AM, Gaetani GF.
Mechanisms of protection of catalase by NADPH. Kinetics
and stoichiometry. J. Biol. Chem., 1999; 274:13908–13914
[99] Arthur JR. The glutathione peroxidases. Cell Mol Life Sci.
2000; 57:1825–1835
[100] Chu FF, Doroshow JH, Esworthy RS. Expression,
characterization, and tissue distribution of a new cellular
selenium-dependent glutathione peroxidase, GSHPx-GI. J.
Biol. Chem., 1993; 268:2571–2576
[101] Comhair SA, Bhathena PR, Farver C, Thunnissen FB,
Erzurum SC. Extracellular glutathione peroxidase induction
in asthmatic lungs: evidence for redox regulation of
expression in human airway epithelial cells. FASEB J. 2001;
70
15:70–78
[102] Ladner JE, Parsons JF, Rife CL, Gilliland GL, Armstrong RN.
Parallel evolutionary pathways for glutathione transferases:
structure and mechanism of the mitochondrial class kappa
enzyme rGSTK1-1. Biochemistry. 2004; 43:52–61
[103] Robinson A, Huttley GA, Booth HS, Board PG. Modelling and
bioinformatics studies of the human kappa class glutathione
transferase predict a novel third transferase family with
homology to prokaryotic 2-hydroxychromene-2-carboxylate
isomerases. Biochem. J. 2004; 379:541–552
[104] Jakobsson P-J,Morgenstern R, Mancini J, Ford-Hutchinson A,
Persson B. Common structural features of MAPEGda
widespread superfamily of membrane associated proteins with
highly divergent functions in eicosanoid and glutathione
metabolism. Protein Sci., 1999; 8:689–692
[105] Dorion S, Lambert H, Landry J. Activation of the p38
signaling pathway by heat shock involves the dissociation of
glutathione S-transferase Mu from Ask1. J. Biol. Chem., 2002;
277:30792–30797
[106] Adler V, Yin Z, Fuchs SY, Benezra M, Rosario L, et al.
Regulation of JNK signaling by GSTp. EMBO J. 1999;
18:1321–1334
[107] Manevich Y, Feinstein SI, Fisher AB. Activation of the
antioxidant enzyme 1-CYS peroxiredoxin requires
glutathionylation mediated by heterodimerization with pGST.
Proc. Natl. Acad. Sci. U S A. 2004; 101:3780–3785.
[108] Kinnula VL, Lehtonen S, Kaarteenaho-Wiik R, Lakari E,
Pääkkö P, et al. Cell specific expression of peroxiredoxins in
human lung and pulmonary sarcoidosis. Thorax. 2002;
57:157–164
[109] Dubuisson M, Vander Stricht D, Clippe A, Etienne F, Nauser T,
et al. Human peroxiredoxin 5 is a peroxynitrite reductase.
FEBS Lett. 2004; 571:161–165
[110] Holmgren A. Antioxidant functions of thioredoxin and
glutaredoxin systems. Antioxid. Redox Signal. 2000; 2:811–
820
[111] Hensley K, Benakass EJ, Bolli R, et al. New perspectives on
vitamin E: γ-tocopherol and carboxyethylhydroxychroman
metabolites in biology and medicine. Free Rad. Biol. Med.,
2004; 36:1–15.
[112] Pryor WA. Vitamin E and heart disease: basic science to
clinical intervention trials. Free Rad. Biol. Med., 2000;
28:141–64.
[113] Kojo S. Vitamin C: basic metabolism and its function as an
index of oxidative stress. Curr. Med. Chem., 2004; 11:1041–
64.
[114] Naziroglu M, Butterworth P. Protective effects of moderate
exercise with dietary vitamin C and E on blood antioxidative
defense mechanism in rats with streptozotocin-induced
diabetes. Can. J. Appl. Physiol., 2005; 30:172–85.
[115] Yuanyuan C., Guangyan L., Jiao Y., Yuanyuan W., Xiaoqiong
Y., Xiaoyun W., Guoping L., Zhiguang L. and Nanshan Z.
Vitamin C Mitigates Oxidative Stress and Tumor Necrosis
Factor-Alpha in Severe Community-Acquired Pneumonia and
LPS-Induced Macrophages. Mediators of Inflammation
Article ID 426740, 2014; 11 pages.
71 Said M. Al-Dalaen and Aiman I. Al-Qtaitat: Review Article: Oxidative Stress Versus Antioxidants
[116] Khalid R. Studies on free radicals, antioxidants, and co-factors
(Review). Clinical Interventions in Aging. 2007; 2(2):219–236
[117] Stahl W, Sies H. Antioxidant activity of carotenoids. Mol.
Aspect Med., 2003; 24:345–51.
[118] El-Agamey A, Lowe GM, McGarvey DJ, Mortensen A,
Phillip DM, Truscott TG. Carotenoid radical chemistry and
antioxidant/pro-oxidant properties. Arch. Biochem. Biophys.,
2004; 430:37–48.
[119] Mortensen A, Skibsted LH, Truscott TG. 2001. The interaction
of dietary carotenoids with radical species. Arch. Biochem.
Biophs., 2001; 385:13–19.
[120] Niles RM. Signaling pathways in retinoid chemoprevention
and treatment of cancer. Mutat. Res., 2004; 555:81–96.
[121] Donato LJ, Noy N. Suppression of mammary carcinoma
growth by retinoic acid: proapoptotic genes are targets for
retinoic acid receptor and cellular retinoic acid-binding protein
II signaling. Cancer Res., 2000; 65:8193–8199.
[122] Niizuma H, Nakamura Y, Ozaki T, Nakanishi H, Ohira M, et
al. Bcl-2 is a key regulator for the retinoic acid-induced
apoptotic cell death in neuroblastoma. Oncogene. 2006;
25:5046–5055.
View publication stats
[123] Masella R, Di Benedetto R, Vari R, et al. Novel mechanisms
of natural antioxidant compounds in biological systems:
involvement of glutathione and glutathione-related enzymes. J.
Nutr. Biochem., 2005; 16:577–86.
[124] Karoui H, Hogg N, Frejaville C, et al. Characterization of
sulfur-centered radical intermediates formed during the
oxidation of thiols and sulfite by peroxynitrite. ESR-spin
trapping and oxygen uptake studies. J. Biol. Chem., 1996;
271:6000–9
[125] Dröge W. 2002. Aging-related changes in the thiol/disulfide
redox state: implications for the use of thiol antioxidants.
Exper. Geront., 2002 ; 37:1333–45.
[126] Smith AR, Shenvi SV, Widlansky M, et al. Lipoic acid as a
potential therapy for chronic diseases associated with
oxidative stress. Curr. Med. Chem., 2004; 11:1135–46.
[127] Navari-Izzo F, Quartacci MF, Sgherri C. Lipoic acid: a unique
antioxidant in the detoxification of activated oxygen species.
Plant Physiol. Biochem., 2002; 40:463–70.
[128] Rahimi R, Nikfar S, Larijani B, et al. A review on the role of
antioxidants in the management of diabetes and its
complications. Biomed. Pharmacothe., 2005; 59:365–73.