6 Benefits of Cold Plunge

[1] An Evidence-based approach for choosing post-exercise recovery techniques to reduce markers of muscle damage, soreness, fatigue, and inflammation: a systematic review with meta-analysis

Cold exposure decreases DOMS (massage is most effective)

Cold exposure decreases inflammatory markers (creatine kinase, IL-6, C-reactive protein)

Massage was also effective

[2] Cold Water Immersion (cryotherapy) for preventing and treating muscle soreness after exercise

Cold-water immersion reduces DOMS

Data from 17 trials n=366

Some evidence that cold-water immersion reduces DOMS at 24,48,72,96hrs

[3] Impact of Cold-Water Immersion Compared with Passive Recovery Following a Single Bout of Strenuous Exercise on Athletic Performance in Physically Active Participants: A Systematic Review

Not sure if I agree with the methods they used to perform this meta (pooled counter movement jump and sprints lasting under 10s)

CWI improved:

-recovery of muscular power (but not strength) 24hr after high intensity exercise

-muscular soreness

-reduced circulating Creatine Kinase levels post exercise

-perceived recovery 24 hr after high intensity exercise (but not eccentric, even though perceived DOMS decreased?….)

Dose-response relationship indicating lower-temperature water and shorter duration may be more effective for clearing serum creatine kinase after high-intensity exercise

[4] Effects of Cold Water Immersion on Muscle Oxygenation During Repeated Bouts of Fatiguing Exercise

CWI attenuated a decrease in tissue oxygenation in the 2nd fatiguing bout by 4%

Decrease in perceived muscle soreness 1 day post testing in treatment group

No significant effect on muscle performance

Knee extensions

10 min recovery intervention (CWI or control)

Repeat knee extension

[5] Use of Cold-Water Immersion to Reduce Muscle Damage and Delayed-Onset Muscle Soreness and Preserve Muscle Power in Jiu-Jitsu Athletes

CWI 6℃ for 19 minutes

Significant decrease in Lactate Dehydrogenase in CWI group 24hrs post recovery (might not actually be a good thing though for adaptation)

Decrease perceived muscle soreness

Increased estimated muscle power (they did a weighted chin up – don’t love it) for upper and lower limbs

Higher perceived recovery

[6] The Effect of Different Water Immersion Temperatures on Post-Exercise Parasympathetic Reactivation

Cold Water Immersion improves post-exercise HRV recovery while Hot Water Immersion delays post-exercise HRV recovery 

Cold Water Immersion is an effective recovery modality to re-establish a parasympathetic state – wait how does that work if CWI increases circulating levels of catecholamines which are a sympathetic response?

Cold Water Immersion accelerates post-exercise parasympathetic reactivation (as measured by HRV)

Hot Water Immersion blunts post-exercise parasympathetic reactivation (as measured by HRV)

[7] Stress and Heart Rate Variability: A Meta-analysis and Review of the Literature

Relaxed state = Low heart rate and high Heart Rate Variability (HRV)

Stressed state = Higher heart rate and lower HRV

[8] Effect of cold water immersion on repeat cycling performance and thermoregulation in the heat

CWI might be an effective way to maintain endurance performance if short rest interval (like same day)

Active recovery helped clear blood lactate but decreased performance

CWI did not clear blood lactate and helped maintain endurance performance

n=10 

30 min exercise, 

15 min of one of 4 different cold water immersion therapies, or active recovery, 

Followed by 40 min passive recovery

Repeat 30 min exercise

Active recovery resulted in lower blood lactate concentrations but also 4.1% decrease in performance in second exercise bout

CWI effective in reducing thermal strain and maintaining performance on subsequent exercise bout

[9] The Acute and Longer-Term Effects of Cold Water Immersion in Highly-Trained Volleyball Athletes During an Intense Training Block

CWI did not have any acute effects on performance, trending positive effects over 16 day period

Variables (countermovement jump, squat jump height, medicine ball throw distance)

[11] Post-Exercise cold water immersion attenuates acute anabolic signaling and long-term adaptations in muscle to strength training

CWI may blunt anabolic signals for long term strength and hypertrophy

12 weeks of 2x/week strength training 

Significantly greater increase in isokinetic work, type 2 muscle fiber CSA and number of myonuclei per fiber in active recovery group vs. cold water immersion group

Active recovery group saw the following increases

Isokinetic work (19%)

Type 2 fiber CSA (17%)

Number of myonuclei per fiber (26%)

2nd study (also in this paper)

Single bout of exercise on separate days followed by active recovery or cold water immersion

Significantly greater number of satellite cells, and myogenic kinases in active recovery group than CWI group

[12] The Influence of Post-Exercise Cold-Water Immersion on Adaptive Responses to Exercise: A Review of the Literature

Cold Water Immersion may blunt strength and hypertrophy both acutely and chronically

CWI may enhance endurance signaling pathways and genes related to mitochondrial biogenesis but it seems potentially only acutely, not chronically

[13] Adipose-tissue plasticity in health and disease – excellent review on adipose tissue

Chronic cold exposure can increase number of mitochondrial rich, thermogenic beige adipocytes – this process is reversible if cold exposure ceases

“Upon cold exposure, sympathetic neurons release the neurotransmitter norepinephrine, which activates the beta-adrenergic receptor-cAMP-PKA pathway in adipocytes. This signaling cascade induces lipolysis and thermogenesis and stimulates transcription of genes driving the thermogenic program in brown and beige adipocytes. UCP1 function and thus thermogenic respiration is acutely activated by long chain fatty acids (LCFA) and inhibited by purine nucleotides.” from  (Bertholet and Kirichok, 2017; Fedorenko et al., 2012)

[16] Uric acid and glutathione levels during short-term whole body cold exposure

Increased endogenous antioxidants (glutathione) in winter swimmers vs. non-swimmers – may improve immune function

Increased baseline concentration of reduced glutathione in winter swimmers vs. non-winter swimmers 

Significant decrease in uric acid during and following cold exposure, likely because of the increase in ROS which is hypothesized as coming from muscle shivering, or catecholamine oxidation

[17] Improved antioxidative protection in winter swimmers

Higher baseline endogenous antioxidants in winter swimmers than non-swimmers – this is known as “body hardening” – exposing oneself to stressful stimuli (not sure if it’s always  hypothermic conditions or stress in general)

Baseline glutathione was higher and erythrocyte activity of superoxide dismutase (SOD), and Catalase (Cat) were higher at baseline in winter swimmers than non-winter swimmers

[18] Examining the benefits of cold exposure as a therapeutic strategy for obesity and type 2 diabetes

Improvement in glucose utilization is largely due to skeletal muscle thermogenesis, and in part due to Brown Adipose Tissue activation

Dose dependent response to cold exposure and energy expenditure

Major increase in carbohydrate utilization in response to cold exposure, fatty acid utilization and protein metabolism also increase

Cold increases blood pressure and decreases heart rate

[19] Short-term cold acclimation improves insulin sensitivity in patients with type 2 diabetes mellitus

Cold exposure may be an effective therapy for increasing insulin sensitivity in Type 2 diabetics

10 Day Cold air acclimation (14-15℃) increased peripheral insulin sensitivity by 43% in type 2 diabetes

n=8

Increased GLUT4 translocation

[20] The distribution of brown adipose tissue in the human

Brown Fat is located around the kidneys, aorta, neck and the mediastinum (between the lungs?)

–keep the most important parts of the body warm, kidneys, heart, cervical spinal column which is responsible for the contraction of the diaphragm 

Distributed throughout the body when we’re younger

[21] Brown Adipose Tissue: Function and Physiological Significance

Chronic adrenergic stimulation is required to stimulate brown fat

Chronic cold exposure is required to recruit Brown Adipose Tissue (BAT)

Recruited by epinephrine which is released by activation of the sympathetic nervous system

Non-shivering Thermogenesis is due to the activation of BAT

Protein dilution hypothesis – a diet low in protein requires the animal to eat more food in order to meet the metabolic protein requirements which leads to obesity

Obesity causes decreased activation of BAT and UCP1 expression

Leptin activates BAT

Decreased leptin sensitivity with age = decreased BAT activation with age

Decreased activation of BAT during fasting

Polyunsaturated fatty acids result in greater BAT activation (than saturated/monounsaturated FAs)

Testosterone and Estrogen activate BAT

Serotonin activates BAT

Serotonin helps regulate satiety

Cold exposure results in marked glucose uptake in BAT via sympathetic pathway (especially norepinephrine I believe) and mediated by β-adrenoceptors and cAMP

Fatty Acids are main substrate (fuel) for BAT

BAT utilizes lots of oxygen

BAT secretes Nerve Growth Factor during perinatal stage

VEGF highly expressed in BAT

I don’t understand. Recruiting diets = higher calorie diets where more of the calories come from fat and carbs. It is said that this leads to obesity which decreases activation of BAT, but then it says under “Are diet-adapted animals hyperpyrexic?” that animals adapted to recruiting diets have increased body temps, so wouldn’t that indicate an increase in BAT activation?

Only one study has looked at recruiting diets and BAT in humans, apparently did not show any effect, but author of this review says the norepinephrine stimulus may not have been adequate to activate BAT.

Also if Leptin from White Adipose Tissue activates BAT through receptors in the brain shouldn’t obese people activate BAT more, not less since they have more WAT? Or do they not produce as much Leptin and that’s why they’re obese?

Cold exposure increases precursors of Nitric Oxide

BAT can release Nitric Oxide

BAT generates fatty acids when stimulated by nor-epinephrine

[22] Cold and Exercise: Therapeutic Tools to Activate Brown Adipose Tissue and Combat Obesity

Really good, extremely detailed, review.

Fuels of Brown Adipose Tissue:

Glucose

Fatty Acids

Glutamate (which can directly and indirectly stimulate thermogenesis)

Cold exposure increases mitochondrial content and function in Brown Adipose Tissue

Chronic cold exposure causes “beiging” of White Adipose Tissue (increasing the expression of UCP1, PGC1alpha and other thermogenic proteins)

May cause beiging effect through batokines

[23] Cold Water Swimming – Benefits and Risks: A Narrative Review

Really good recap on benefits of winter swimming, but unclear whether the effects are due to the exercise, the cold, or the combination of the two.

Cold water swimming improves

Insulin sensitivity (seems sex specific – improves for women)

Mood – may be a treatment for Major Depressive Disorder

Potential risks of cold water swimming

Abnormal daily cortisol cycles

May cause arrhythmias that result in cardiac events

May cause pulmonary edemas

[24]. What is the biochemical and physiological rationale for using cold-water immersion in sports recovery? A systematic review

CWI <5 min, lower than 15 Celcius – most common parameters

Evidence that CWI increases

Peripheral catecholamine concentration

Oxidative stress – possibly via shivering, possibly because catecholamines are being oxidized into superoxides 

Potential increase in free-radicals

Magnitude of these responses may decrease with acclimatization 

[25] Altered brown fat thermoregulation and enhanced cold-induced thermogenesis in young, healthy, winter-swimming men

2-3 CWI swims per week (they also did sauna)

Water 1-9℃

Winter simmers exhibited:

Lower core temperature at a “comfortable state” than controls

No BAT glucose uptake at thermal comfort state, (controls did)

Increased cold-induced thermogenesis than controls

Increase in skin temperatures around 4:30-5:30am interestingly enough

They say winter swimming might be a way to combat obesity but wouldn’t decreased BAT glucose uptake at rest indicate a decrease in basal metabolic rate which would have the opposite effect, even though they have an increase in cold-induced thermogenesis than controls?

I believe they did contrast? Since they altered between CWI and sauna? 

Was it actually a swim since it was only 1.4 min in the water? Does exercise play a role?

n=7 for winter swimmers

n=8 for control

Winter swimmers averaged 2-3 swims per week

1.4 minutes in water per immersion

2.6 immersions per swim

Total CWI per week = 11 minutes

They also did sauna an average of ? per week

2 sessions per visit

11.1 minutes per sauna session

Total Sauna per week = 57 minutes

[26] Moving in extreme environments: open water swimming in cold and warm water

Cold water swimming, especially in competition may cause an “autonomic conflict” where the sympathetic nervous system is activated while the parasympathetic is also working, potentially causing arrhythmias

Paper states that anger may be what’s causing this conflict. 

This may lead to a cardiac event

[29] Cold-water immersion blunts and delays increases in circulating testosterone and cytokines post-resistance exercise

CWI blunted T and cytokine (hypertrophic) response after a bout of resistance exercise

[30] Cold water immersion attenuates anabolic signaling and skeletal muscle fiber hypertrophy, but not strength gain, following whole-body resistance training 

CWI blunted muscle hypertrophy but not 1RM

[31] Post exercise cooling impairs muscle protein synthesis rates in recreational athletes

Post exercise cooling decreased uptake of amino acids 

Post exercise cooling lowered the rate of myofibrillar protein synthesis

n=12

[33] The Effect of Cold Exposure on Cognitive Performance in Healthy Adults: A Systematic Review

Processing speed and executive function were most negatively affected by cold exposure

Memory and attention showed conflicting results

Acute Cold Exposure showed impaired cognitive performance in 15/18 studies…

18 studies included

May be a difference between males and females

May be a difference in single vs. multiple (chronic) exposures

[34] Swimming Induced Pulmonary Edema

Cold water increases pulmonary blood flow, exercise increases cardiac output, this combination can sometimes cause excess pressure on the capillaries in the lungs causing them to leak fluid into the alveoli

Recovery was spontaneous and quick with no recurrence of symptoms (although pulmonary edema can be fatal in other circumstances)

[35] Immune changes in humans during cold exposure: effects of prior heating and exercise

Cold air exposure increased white blood cell counts increased in all protocols

Significantly more leukocytes were in circulation 1 hour into cold exposure in the pre-exercise  in water treatment

Natural Killer cell activity increased significantly in response to exercise in water pretreatment

Passive heating in water + 2 hours of cold exposure also increased NK cell activity

Cold exposure significantly increased stress hormones (Epinephrine, Nor-epinephrine, and cortisol) within 60 min of passive heating or control water immersion pre-treatment, within 120 min of exercise pre-treatment 

Increases in circulating norepinephrine may be the cause of the rise in immune response in comparison to the other treatment protocols

[36] Improved mood following a single immersion in cold water

Improvement in vigor and esteem related effects – this was the ocean

Decrease in negative emotion subset (including depression by 2.1 points in CWI)

n=64 (42 CWI, 22 control) about 18 min at (56 ℉ = 13.6℃)

Other studies, uncited in this article:

[37] Contrast water immersion hastens plasma lactate decrease after intense anaerobic exercise

Contrast bath (36℃ and 12℃) resulted in faster clearing of lactate after intense anaerobic exercise (I don’t believe this is a good thing because it blunts the training stimulus – think about BFR)

4 wingate tests separated by 30s rest…ouch – n=11 randomized trial

Other research papers used to gather information but not specifically cited in the article above.

Scientific Evidence-Based Effects of Hydrotherapy on Various Systems of the Body

Discusses both cold water and hot water immersion and a number of different styles of immersions 

Lot of great citations in Musculoskeletal section, and the endocrine section for cold water immersion and contrasting

Leg Immersion in warm water, stretch-shortening exercise, and exercise-induced muscle damage

Leg immersion in warm water decreased markers of exercise induced muscle damage, including creating kinase activity in the blood, muscle soreness.

Effects of cold-water immersion and contrast-water therapy after training in young soccer players

Cold Water Immersion reduces perceived fatigue after training sessions

Cold water immersion did not change inflammatory or hematological markers

Alternating hot and cold water immersion for athlete recovery: a review – 2004 review

Not a ton of conclusive evidence

Water Immersion Recovery for Athletes: Effect on Exercise Performance and Practical Recommendations – good review

Contrast bathing using consists of:

Alternating 3-7 times between hot water (bath not shower seems more beneficial) and cold water 

1-2 in both cold and hot water

Mixed results but the above protocol seems to yield significant results, especially when accumulated fatigue and muscle damage over the course of 2+ days are considered

Take home: it’s likely helpful for recovery – but again, do you want to blunt the stimulus?

The effectiveness of hydrotherapy in the management of fibromyalgia syndrome: A systematic review

Mostly water at or around 37℃ 

Also includes exercise and balneotherapy (bathing in thermal mineral water)

Hydrotherapy was associated with positive health outcomes for pain, health status, and tender point count

Sex-related responses of beta-endorphin, ACTH, GH and PRL to cold exposure in humans

Don’t love this study, small sample size, also unless the subjects have similar lean muscle mass and BMIs subjects with less muscle / less mass in general would likely get colder overall (aka women might see a greater decrease in core temperature and as a result increase in hormone release but men may not because of difference in core temperature change)

8 men, 8 women 30 min in 25℃ room, then 30 min in 4℃ room

Significant increase in beta-endorphin, ACTH, cortisol and GH levels observed in women

Non-significant increased of same hormones observed in men

Significant increase in blood pressure for men and decrease in HR for men, but not in women

Skin temp significantly lower in women but not men

Are beta-endorphins and thermoregulation during cold-water immersion related?

Beta-endorphins were significantly lower in the high fat group vs. the low fat group

Beta-endorphins did not increase in proportion ot level of heat loss (no dose-dependent relationship between heat loss and beta-endorphin release

Perfect study to discuss what I mentioned above

No significant relationship between beta-endorphins, tissues insulation, and core temperature

No significant relationship between changes in thermoregulatory variables and High fat vs. Low fat groups

Effect of Cold Stimulation on Cardiac-Vagal Activation in Healthy Participants a Randomized Controlled Trial

This runs counter intuitive to the idea that CWI causes a stress response via the sympathetic nervous system

Heart rate variability is the fluctuation of the length of heartbeat intervals

Diving reflex effects respiratory, cardiac, and vascular responses – occurs when water contacts the face

Cold stimulation to the neck and cheek increases HRV

The importance of norepinephrine in depression – finish reading

Decreased levels of Norepinephrine, serotonin, and dopamine are associated with depression

Hormone response of normal and intermittent cold-preadapted humans to continuous cold

Cold increases epinephrine release in both acclimatized and non-acclimatized groups

Exposure to cold in Non acclimatized group resulted in increased urine volume, norepinephrine (+48%), epinephrine (+84%), and hydroxycorticosteroids

Prior cold exposure resulted in no elevation in metabolism (it may have already adapted to be higher metabolism and additional cold exposure did not further increase Basal metabolic rate) and decrease in body temp in response to cold exposure

Prior cold exposure still resulted in an increase in epinephrine (+65%)

Human physiological responses to immersion into water of different temperatures

CWI 14℃ resulted increased dopamine, noradrenaline, and metabolic rate

Metabolic rate increased by 350%

Noradrenaline increased by 530%

Dopamine increased by 250%

Cortisol levels tended to decrease (not sure if they were significant – also the opposite of the other studies I’ve read)

Plasma adrenaline levels remained unchanged

Thermoneutral water resulted in “strengthened” parasympathetic tone (decreased HR blood pressure, and cortisol by 34%) (aka had a relaxing effect) – not sure this is convincing enough that I would site it, but still cool

20℃ water decreased HR, BP (not sure if cortisol decreased significantly)

Change in sympathetic activity, cardiovascular functions and plasma hormone concentrations due to immersion in men

Increase in noradrenaline

No significant increase in adrenaline or dopamine

n=10

14℃

Effects of Temperature and Water Immersion on Plasma Catecholamines and Circulation

CWI at 6℃ caused increase in Norepinephrine (don’t believe it specifically talked about cortisol)

Acute and chronic effects of winter swimming on LH, FSH, prolactin, growth hormones, TSH, cortisol, serum glucose and insulin

Once weekly winter swimming for 2-10 minutes at 2-6℃)

Acute effects

Increase in TSH and cortisol

Mild decrease in prolactin

No change in FSH, LH, growth hormone

Chronic effects

Increase of basal prolactin levels

Decrease in insulin serum levels

The Effect of Cold Exposure on Cognitive Performance in Healthy Adults: A Systematic Review

Processing speed and executive function were most negatively affected by cold exposure

Memory and attention showed conflicting results

Acute Cold Exposure showed impaired cognitive performance in 15/18 studies…

18 studies included

May be a difference between males and females

May be a difference in single vs. multiple (chronic) exposures

Cold Water Swimming Beneficially Modulates Insulin in Middle Aged Individuals

Increased insulin sensitivity mid way through Cold Water swim season – only in women (where were the leaner individuals in this study) and lean individuals

N = 30

Health Effects of Voluntary Exposure to Cold Water – a Continuing Subject of Debate

BAT is used to produce heat to warm the body

BAT can generate heat by “the action of free fatty acids in uncoupling mitochondrial electron transport” – aka BAT burns triglycerides to generate heat

And by “Noradrenaline-induced membrane depolarisation and sodium pumping”

BAT energy consumption is less than 20 calories per day – the equivalence of running for 2 min at a moderate pace

Adiponectin is a hormone produced by adipocytes 

Adiponectin 

Reduces inflammation 

Reduces atherogenesis (buildup of fatty acid plaques in the arteries) 

Improves insulin sensitivity

Effect of Regular Winter Swimming on the Activity of the Sympathoadrenal System Before and After a Single Cold Water Immersion

Regular Winter Swimming attenuates catecholamine response to cold water

Cold Water Immersion Directly and Mediated by Alleviated Pain to Promote Quality of Life in Indonesian with Gout Arthritis: A community-based Randomized Controlled Trial

I’m not familiar with generalized estimating equations and am thus tentative to cite these findings

Cold water immersion

Decreased pain

Decreased depression

Improved Joint mobility

Improved Quality of life

The Effect of Cold Showering on Health and Work: A Randomized Controlled Trial

Finishing a warm shower with 90 seconds of cold water decreased number of self reported sickness days by 29% (but not a reduction in illness days – so I believe they only called in sick when they were actually sick)

Health Effects of Voluntary Exposure to Cold Water – a Continuing Subject of Debate

UCP1: the only protein able to mediate adaptive non-shivering thermogenesis and metabolic inefficiency

Brown Adipose Tissue at the Intersection of Sleep and Temperature Regulation

This is a hypothesis, not an experiment. Impaired brown fat activation may play a role in poor sleep and/or metabolic function

Endocrine Effects of Repeated Hot Thermal Stress and Cold Water Immersion in Young Adult Men

Contrast bath caused significant decrease in cortisol concentrations especially for young men with higher baseline cortisol concentrations

No change in Testosterone, DHEA-S or prolactin

4 x 12 min sauna at 90℃, 6 min CWI at 10℃

Analgesic and anti-inflammatory drugs in sports: Implications for exercise performance and training adaptations 

NSAIDs likely impair muscle hypertrophy by inhibiting cyclooxygenase (COX) activity

Role of macrophages during skeletal muscle generation and hypertrophy – implications for immunomodulatory strategies

Effects of immersion in water containing high concentrations of CO2 (CO2-water) at thermoneutral on thermoregulation and heart rate variability in humans

CO2 enriched water 

increased cutaneous blood flow (peripheral vasodilation)

Decreased body temp

Increased HRV

Compared to freshwater

Adapted cold shower as a potential treatment for depression

Referenced a lot but not actually a research study….it’s just a hypothesis….

The Science & Use of Cold Exposure for Health & Performance – Huberman lab

Role of Norepinephrine in the Pathophysiology and Treatment of Mood Disorders – great review

Norepinephrine is important for attention and learning – especially for novel stimuli

NE is also important for consolidating memories & creating stronger associations in the limbic system 

(I believe whether these associations are positive or negative depends on our perception of ability to handle the challenge in front of us – example: the rapid heart rate from NE when you get nervous before a speech and cause you to stumble over your words or deliver it flawlessly depending on your perception of the situation, your ability to handle it, and what that sensation (rapid heart rate) means.

Norepinephrine (NE) cells primarily located in the Locus Coeruleus (LC) of the brain stem – projections from the LC innervate cortical and subcortical as well as the spinal cord.

Synaptic control of LC firing is in part determined by glutamate and GABA

Norepinephrine potentiates the firing of Dopamine cells in the ventral tegmental area that project to the limbic forebrain

Firing of the LC is correlated with behaviorally orienting responses.

Highest spike occurs when an automatic behavior is interrupted (think if you’re driving and a car cuts you off)

New stimuli – especially new faces and other meaningful stimuli elicit a strong, phasic firing from LC

Repeated exposure to new stimuli rapidly desensitizes firing of the LC

Low firing rates and release of NE = behavioral sedation

Optimal firing rates = focused attention

Extremely high firing rates = hyperarousal and distractibility

Changes in neurotrophin levels may lead to target and NE neuron degeneration or axonal pruning

Beneficial and Detrimental Effects of Reactive Oxygen Species on Lifespan: A Comprehensive Review of Comparative and Experimental Studies

Free Radical Theory of Aging (FRTA) – increases in Reactive Oxygen Species (ROS)s and oxidative damage are correlated with aging.

There are studies however that show the opposite, and common sense, exercise, sauna, ice baths, all increase ROS (but also likely increase endogenous antioxidants)

ROS that are free radicals – have an unpaired electron in their shell and are therefore highly reactive
Superoxide (O–2), 

Hydroxyl (HO), 

Peroxyl (RO–2), 

Hydroperoxyl (HO2), 

Alkoxyl radicals (RO)

ROS that are not free radicals – more stable, able to pass through membranes but can still be reduced (and thus cause damage I believe)

Peroxide (H2O2)

Hydroxide Ion (OH–)

Organic Peroxides (ROOH)

Reactive Nitrogen Species (RNS) – can cause cellular damage, but also have functional roles in cellular signaling and pathogen defense. We don’t know how they impact longevity.

Nitric Oxide (NO) is produced from L-arginine by the enzyme nitric oxide synthase

Nitric oxide can then react with superoxide to produce peroxynitrite (ONOO–)

Peroxynitrite (ONOO–) can damage cells or form other types of RNSs

Free Radical RNSs

Nitric Dioxide (NO2)

Nitrate Radical (NO3)

Non Free Radical RNSs:

Peroxynitrite

Nitrous Acid (HNO2)

Nitrite (NO–2)

Nitrosyl cation (NO+)

Nitroxyl Anion (NO-)

Peroxynitrous Acid (ONOOH)

Dinitrogen Trioxide (N2O3)

ROS can damage:
1.) DNA – cause mutations in both nuclear and mitochondrial DNA

2.) Proteins – can cause protein carbonylation. Especially thiol-containing cysteine and methionine residues

3.) Lipids – can cause lipid peroxidation which can cause reactive by products

All of these are correlated with advanced aging

Mitochondrial respiration is a major source of ROS within the cell.

Electrons may leak out while being transported between the complexes, binding with oxygen and creating superoxide

Immune system uses ROS to attack pathogens in the body

Membrane Phagocyte NADPH oxidase and myeloperoxidase (MPO) help to attack pathogens ROS also play a role in signaling for growth, survival, and apoptosis

ROS-generating enzymes that play a role in cell signaling

Cytochrome P450 (CYP) – produce ROS in detoxification and excretion of xenobiotics

Xanthine oxidoreductase (XOR) – produces superoxide anions to break down purines to uric acid

Superoxide Dismutase (SOD) – converts dopamine after signaling occurs and produces hydrogen peroxide in neurons in the process

ROS  are also produced during Beta Oxidation of Fatty Acids in the peroxisome – producing hydrogen peroxide

Peroxisome-generated ROS are thought to contribute to the regulation of NF-kB and MTORC1

(NADPH Oxidase generated ROS are also thought to contribute) 

Doesn’t seem to distinguish between endogenous and exogenous antioxidants which is surprising given what I’ve heard / read about anti-inflammatory substances blunting the hypertrophy response)

Enzymatic Antioxidants

1. Superoxide Dismutase (SOD) – converts highly reactive superoxide anion to a less reactive hydrogen peroxide

3 types of SOD

1. SOD1 – located in the cytosol – active site is Cu/Zn
2. SOD2 – located in the mitochondria – active site is Mn
3. SOD3 – located extracellularly – active site is Cu/Zn

2.) Catalase (CAT) – converts hydrogen peroxide to water and oxygen (aka downstream of SOD)

Primarily located in peroxisomes where hydrogen peroxide can be high due to Beta oxidation of lipids

3.) Glutathione Peroxidase (GPx) – works with CAT to reduce hydrogen peroxide to water and oxygen

GPx is located in the mitochondria and the cytoplasm (as opposed to the peroxisomes like CAT)

Active site is Selenocysteine (an amino acid that has Selenium I believe)

GPx requires 2 Glutathione (GSH) molecules to return it to its functional state which is catalyzed by Glutathione Reductase (GR) and uses electrons donated by NADPH 

4 subcellular compartments

1. GPx1 – cytosol – hydrogen peroxide and organic peroxides
2. GPx2 – cytosol – hydrogen peroxide and organic peroxides
3. GPx3 – extracellular – antioxidants
4. GPx4 – cell membranes and mitochondria – can metabolize phospholipid hydroperoxides

4.) Glutaredoxin (Grx) and thioredoxin (Trx)

Protect thiol-containing proteins by repairing damage caused by exposure to oxidants

Active sites consist of cysteine residues

Requires 2 Glutathione molecules to be reduced back

Both require electrons from NADPH

Play important roles in redox signaling pathways

Located in:

1. Trx1 & Grx1 – nucleus and cytosol – can be secreted
2. Trx2 & Grx2 – mitochondria
3. Grx3 – nucleus and cytosol
4. Grx5 – mitochondria

1. Peroxiredoxin (Prx)

Cysteine containing enzymes that reduce peroxides including organic peroxides

Returned to their active state by either being reduced by Trx or Glutathione

Locations:

1. Prx1 – nucleus and cytosol
2. Prx2 – nucleus and cytosol
3. Prx3 – mitochondria
4. Prx4 – endoplasmic reticulum
5. Prx5 – peroxisomes
6. Prx6 – cytosol

6.) Glutathione S-transferase (GST)s

Linked to various stress responses.

Thought to help GPx in attenuating lipid peroxidation by reducing fatty acid hydroperoxides

Binds GSH 

Active site is serine residue

GSTs may also help detoxify the end products of lipid peroxidation (which can be harmful to the cell)

Located in the cytosol, microsomes, and plasma membrane

Non-enzymatic Antioxidants

1. Glutathione

Essential for the activity of GPx and Grx since it helps convert each enzyme back to its active state

GSH can act as an antioxidant by donating the electrons on the sulfhydryl group to reduce ROS

GSH levels are restored to its reduced state by GR and NADPH or dietary supplementation

1. N-acetyl cysteine (NAC)

Precursor to Glutathione. 

Also has its own thiol group, which allows it to reduce ROS and protect sulfhydryl-containing protein groups from oxidative damage

NAC levels are maintained by consuming high protein foods with cysteine

1. Vitamin C

Water soluble antioxidant

Present intracellularly and extracellularly

Helps prevent oxidation of cholesterols (that’s interesting…)

1. Vitamin E

Lipid soluble 

Present in cell membranes and lipoproteins

Helps to mitigate lipid peroxidation from oxidative stress

Vitamin C can help convert Vitamin E back to its reduced form 

Antioxidants can also repair oxidative damage  

-glutaredoxins and thioredoxins reduce thiol-containing proteins

14kDa reduces cysteine residues

Methionine sulfide reductase reduces methionine residues

Cysteine and Methionine are amino acids most susceptible to oxidation by ROS

DNA repair mechanism can be triggered by redox sensors which signal to enzymes responsible for:

Base excision repair (BER)

Nucleotide excision repair (NER)

Mismatch repair

Irreversibly damaged molecules/organelles are metabolized by proteasomes (in the cytosol) or proteases (in the mitochondria)

Oxidative stress can cause autophagy of:

1.  Peroxisomes (pexophagy)
2. Mitochondria (mitophagy)

Which removes the dysfunctional ROS generating organelles and synthesizes new ones

ROS can oxidize cysteine residues within proteins which can change that protein’s function

Those cysteine residues can be reduced to thioredoxin or glutaredoxin to restore their original function or be further oxidized (presumably to be metabolized?)

ROS can activate protein kinase signaling pathways by inactivating phosphatases or

ROS can inactivate protein kinase signaling pathways (not entirely sure how)

Protein kinases – transfer a phosphate group (usually from ATP) to a target cell to:

1. Activate
2. Deactivate
3. Signal to other cells to interact with that cell

Phosphatases – remove the phosphate group from a molecule

Oxidation

Is

Loss (electrons)

Reduction

Is

Gain (electrons)