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    Post TUDCA more than just a liver aid.

    Tauroursodeoxycholic acid*(TUDCA)

    From liver to eyes to insulin sensitivity TUDCA gives you "bang for your buck"

    is an ambiphilic*bile acid. It is the*taurine*conjugate form of*ursodeoxycholic acid*(UDCA). Humans are found to have trace amounts of TUDCA. However,*bears*contain large amounts of TUDCA in their bile; UDCA and conjugates comprise about 47% of the bile in*American black bears*and up to 76% in*Asiatic bears.[1]*TUDCA has been used in ancient Asian*pharmacopoeias*for its supposed beneficial effects. UDCA is produced in several countries for the treatment of*gallstones*and*liver cirrhosis. It is not approved by the*Food and Drug Administration, in the*U.S.*while UDCA is approved in the United States for the treatment of primary*biliary cirrhosis[2][3]Ongoing research is finding TUDCA has diminishing*apoptotic effects, helping with cardiac function,*Huntington's disease,*Parkinson's disease, and stroke.[4]*Recently, TUDCA has been found to have protective effects in the*eye, especially concerning*retinal degenerative disorders.


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    TAUROURSODEOXYCHOLIC ACID

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    SummaryThings to KnowHow to TakeHuman Effect MatrixScientific ResearchCitations

    Tauroursodeoxycholic Acid

    TUDCA is a water soluble bile acid. It shows great potency in treating cholestasis (bile acid backup in the liver) as the water soluble bile acids counteract the toxicity of regular bile acids. Can also protect and rehabilitate the liver, and general protects cells; very promising molecule.

    This page features*73 unique references*to scientific papers.

    History

    Research analysis by*Kamal Patel*and verified by the*Examine.com Research Team. Last updated on*May 10, 2018.

    SUMMARY*

    THINGS TO KNOW*HOW TO TAKE*HUMAN EFFECT MATRIX*SCIENTIFIC RESEARCH*CITATIONS

    Summary of Tauroursodeoxycholic Acid

    Primary Information, Benefits, Effects, and Important Facts

    Tauroursodeoxycholic acid, more commonly referred to as TUDCA, is a bile salt that is found natrually occurring in the body. When regular bile salts reach the intestines, they can be metabolized by bacteria into UDCA and then later bound to a*taurine*molecule to become TUDCA.

    TUDCA is a water-soluble bile salt, which is in contrast to regular bile salts possessing both water soluble and fat soluble ends and conferring a detergent effect. This is good for the bile salt's biological purpose (emulsifying fats in the intestines to help with absorption) but when bile acids back up in the liver, a clinical state called cholestasis which occurs when the liver is unhealthy, these bile salts can be damaging to cells by destroying the membranes and signalling for cell death. TUDCA and other water soluble bile salts like UDCA compete with this toxicity and thus indirectly protect cells from death.

    Additionally, it seems that TUDCA is able to reduce stress to any cell's*Endoplasmic Reticulum; an organelle in cells that serves as a highway from the nucleus out into the cytoplasm, and aids in folding proteins. Through reducing ER stress, TUDCA has been implicated in a wide range of beneficial metabolic effects such as reducing insulin resistance and diabetes, and being a neurological protection agent. However, usages of TUDCA beyond the liver are preliminary whereas usage of TUDCA for helping an already harmed liver is quite reliable as TUDCA is used in clinical settings (hospitals) for treating cholestasis.

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    Things to Know

    Also Known As

    TUDCA

    Do Not Confuse With

    Taurine*(a moiety on the UDCA part)

    Things to Note

    TUDCA is water-soluble

    Caution Notice*

    If using TUDCA for treating an alcohol-abused liver, be aware of the temporal relationship needed. Co-incubation (same time) or rehabilitative (after the matter) usage of TUDCA may be protective of the liver while*pre-loading TUDCA*before drinking*may be harmful*to the liver.

    Examine.com Medical Disclaimer

    How to Take

    Recommended dosage, active amounts, other details

    10-13mg daily has once been shown to improve liver regenesis rates in a clinically ill population, and may be the lowest estimate of an active oral dose. When looking at improving bile salt composition, a dose around 15-20mg/kg bodyweight TUDCA seems best according to one study.

    Benefits have been seen at 1,750mg daily for muscle and liver insulin sensitivity, which is the highest dose used for treatment of fatty liver disease.

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    Human Effect Matrix

    The*Human Effect Matrix*looks at human studies (it excludes animal and*in vitrostudies) to tell you what effects tauroursodeoxycholic acid has on your body, and how strong these effects are.

    GRADELEVEL OF EVIDENCERobust research conducted with repeated double-blind clinical trialsMultiple studies where at least two are double-blind and placebo controlledSingle double-blind study or multiple cohort studiesUncontrolled or observational studies only

    LEVEL OF EVIDENCE

    ?

    OUTCOMEMAGNITUDE OF EFFECT

    ?

    CONSISTENCY OF RESEARCH RESULTS

    ?

    NOTESLiver EnzymesNotableVERY HIGHSee all 5 studies

    The decrease in liver enzymes associated with cholestasis is quite strong, and TUDCA is a reference drug for these effects

    CholestasisNotable-See study

    Is either comparable or exceeds the potency of ursodeoxycholic acid, the reference drug for cholestasis

    Insulin SensitivityNotable-See study

    Notable due to reaching near 30% improvement in obese persons and only being localized to muscle tissue and the liver, but not adipose tissue

    Blood Glucose--See study

    No significant influence on fasting glucose levels

    Fat Mass--See study

    No significant influence on fat mass in obese persons

    Insulin--See study

    No significant influence on fasting insulin levels

    Weight--See study

    No significant influence on weight in obese persons

    HDL-CMinor-See study

    A decrease in HDL-C has been noted to be secondary to treating cholestasis

    Liver Cell ContentMinor-See study

    An increase in hepatocyte regeneration has been noted with TUDCA in persons with liver disease

    Total CholesterolMinor-See study

    A decrease in total cholesterol in serum has been noted secondary to treating cholestasis

    Scientific Research

    Table of Contents:

    1*Sources and Structure1.1*Sources1.2*Structure2*Pharmacology2.1 *Absorption and bioavailability2.2*Distribution3*Interactions with the Endoplasmic Reticulum3.1*ER stress and Ischemia/Reperfusion4*Interactions with the Liver4.1*Cell death and count4.2*Cholestasis4.3*Gallstones5*Interactions with Neurology5.1*Huntington's Disease5.2*Alzheimer's5.3*Stroke6*Interactions with Glucose metabolism6.1*Mechanisms6.2*Interactions with Beta-cells6.3*Interventions7*Interactions with Fat Mass and Obesity7.1*Thyroid and Metabolic Rate7.2*Adipokines7.3*Interventions8*Nutrient-Nutrient Interactions8.1*Alcohol9*Safety and Toxicity9.1*Human Data

    1Sources and Structure

    1.1. Sources

    Tauroursodeoxycholic Acid (Tauro- Urso- Deoxy- Cholic), commonly referred to as TUDCA, is a derivative of a secondary bile salt secreted from the liver. When bile salts created by the liver reach the intestines, they can be converted into UDCA (ursodeoxycholic acid) by intestinal bacteria[1]*and TUDCA is created when a*taurine*molecule is added to the structure.[2]*Both of these related molecules are known as hydrophilic bile acids.[2]

    It is a common constituent of bile acids, and is in high amounts in the bile acids of bears where is has traditionally been extracted.

    1.2. Structure



    2Pharmacology

    2.1. Absorption and bioavailability

    After oral administration, TUDCA appears to be more effective in raising bile concentrations of UDCA (and downstream effects, such as reducing liver enzyme levels) than UDCA itself; this is most likely due to the*taurine*group enhancing bioavailability.[3]*[4]*The process of conjugating UDCA with taurine is a rate-limiting step, and this rate-limit is avoided with supplementation of TUDCA.[5]

    2.2. Distribution

    Orally administered TUDCA, at 750mg daily, was able to significantly change the UDCA content of serum, fecal, and urinary bile measurements after 2 months of supplementation; suggesting systemic distribution.[3]*Only a small amount of UDCA in serum is unconjugated, as most is bound to taurine or glycine; oral administration of 1500mg for 6 months has an unconjugated UDCA contant of 0.6+/-0.3% in serum.[4]

    Orally administered TUDCA is able to reach neuronal tissue in rats.[6]

    3Interactions with the Endoplasmic Reticulum

    The endoplasmic reticulum (ER) is an organelle in cells that extends from the nucleus and forms an interconnected network of pathways in the cell. The ER has a role in folding protein structures, and oxidative stress can cause the ER to misfold or unfold proteins in a response called the 'Unfolding Protein Response' (UPR); which is an adaptive self-protective response in cells, either reversing the stressor or (if it fails to do so) signalling cell death.[7]*TUDCA is seen as an ER stress response attenuator, and is able to block cell death induced by the adaptive UPR and preserve cell function.[2][8][9]

    3.1. ER stress and Ischemia/Reperfusion

    Via reducing the unfolding protein response, TUDCA has been shown to reduce damage to organs from acute oxygen deprivation such as acute kidney trauma,[10]*surgery on the liver,[9][11][12]*and stroke.[13]*It has also been shown to inhibit neovascularization in diabetic rats, which is induced by similar mechanisms above.[14]

    4Interactions with the Liver

    Endoplasmic Reticulum (ER) stress appears to be a significant regulator in liver cells (hepatocytes) of inflammation and injury[12]*and in part insulin signalling.[15]*Tauroursodeoxycholic Acid (TUDCA), as a suppressor of protein unfolding and ER stress, may confer a therapeutic and rehabilitative role.

    4.1. Cell death and count

    TUDCA has been shown to improve liver healing rates in both steatotic and non-steatotic livers via ER stress reduction after ischemia/reperfusion.[9]TUDCA, in this study, resulted in less cell death via alleviating a mechanism known to accelerate cell apoptosis and also suppressed the actions of*IRE-1and*PKR-like ER kinase, two pathways known to induce protein unfolding.[9]*This cell protective effect has also been seen in liver cells undergoing cold storage[16]*as well as the epithelial cells of bile ducts, which are damaged during chronic hepatitis.[17]*These latter benefits are mediated via PKCa and intracellular Ca2+[17]*and may be dependent on basic levels of dietary methionine and*choline.[18]

    After administration in men with chronic liver disease, 10-13mg TUDCA daily for 3 months appears to enhance the rate of hepatocyte proliferation as well.[19]

    Beyond TUDCA's primary treatment purpose (Cholestasis, next section) TUDCA also appears to have beneficial modulation of cells in the liver, promoting regeneration and reducing cell death. May not be relevant in an already health liver (due to high regeneration rates already), but nice for unhealthy livers

    4.2. Cholestasis

    Cholestasis is a condition in which bile flow from the liver is distrupted in some manner. UDCA and TUDCA are currently one of the first lines of treatment for a variety of cholestatic syndromes.[2]

    Accumulation of bile acids in the liver during periods of impeded intestinal secretion (cholestasis) can cause cell death in hepatocytes secondary to the bile acid's detergent-like effects,[20][21][22]*and UDCA/TUDCA confer protective effects in this scenario. The detergent-like effects are related to bile acid's hydrophobicity and lipid solubilizing actions, yet UDCA/TUDCA are highly hydrophilic and unlikely to possess the same toxicity.[23][24]

    The mechanism of protection may be through competitive antagonism of harmful bile salts actions on hepatocytes.[25]*This, in conjunction with TUDCA supplementation increasing the relative amount of hydrophilic bile salts (UDCA, TUDCA) relative to the harmful salts exerts an overall protective effect. The increase in UDCA seen with supplementation is a diminishing response dose-dependent relationship with 500mg, 1000mg, and 1500mg increasing the bile content of TUDCA from 2.9% (in persons with Primary Biliary Cirrhosis) to 34.4+/-4.5%, 32.8+/-2.8%, and 41.6+/-3%, respectively.[4]*The most effective dose for this beneficial partitioning of bile salts, based on plotted curves from serum and bile analysis, may be 15-20mg/kg bodyweight TUDCA.[4]

    For short term treatment of bile acid complications and cholestasis, TUDCA appears to be very potent and reliable. Used in clinical settings for treatment of cholestasis as well.

    4.3. Gallstones

    Gallstones (made of cholesterol) may be treated in a litholytic manner with bile acids,[26]*dissolving them to a size in which they may be passed. The process of dissolving gallstones made of cholesterol is sometimes also referred to as cholelitholytic[27]*(with litholytic being a more general term, and used with more frequency for kidney stones). Cholesterol gallstones are approximately 75% of all hepatic gallstones (at least in Western countries[28][29]) and are thought to be the only formation of gallstone able to be dissolved with bile acids.[30]

    Gallstones may become opaque, which is thought to indicate their inability to dissolve (and thus, a failure of litholysis treatment);[31]*the opacity appears to be related to calcium deposition in the cholesterol gallstone, and appears to make gallstones resistant to bile acid induced cholelitholysis.[32][30]*The opaque gallstones are either black (around 20% in total and consisting of calcium phosphate and/or carbonate with insoluble bilirubin pigment and cholesterol) or brown (around 5% overall containing calcium bilirubinate, calcium palmitate, stearate and cholesterol).[33][30]

    Gallstones can form in the liver from cholesterol, and administration of bile acids is thought to dissolve the gallstones to a level where they may be passed in the urine (not painless, but does not require surgery); this dissolution appears to not influence all gallstones, with gallstones having a calcium content being resistant to bile acids

    Therapy tends to consist of a nightly dose of bile acids (UDCA or TUDCA) paired with a low cholesterol diet to encourage cholesterol efflux.[34][35]*It should be noted that therapy with oral bile acids is not first-line, and that usually a minimal amount of persons with gallstones respond to UDCA or TUDCA (10% or less[36]); standard practise suggests that it be limited to persons unfit for surgery with small (5mm or less diameter) uncalcified and cholesterol rich gallstones.[30]

    In looking at the rate of failure (formation of opacity during treatment of bile acids), there do not appear to be any significant differences between TUDCA, UDCA, or another bile acid known as CDCA.[37]

    Treatment of gallstones with TUDCA is used in clinical settings, but is not the first-line treatment and requires certain conditions to be met (small uncalcified gallstone of mostly cholesterol) to be effective. When comparing TUDCA against other bile acids, there do not appear to be significant differences in efficacy

    5Interactions with Neurology

    5.1. Huntington's Disease

    Oral administration of TUDCA in rats was shown to be protective against a toxin which induces Huntington's Disease,[6][38]*and was later shown in rats to be neuroprotective in a model of Huntington's Disease without said toxin; reducing neuronal death and improving symptoms.[39]

    These protective effects may also extend to dopaminergic neurons and Parkinson's Disease,[40][41]*but no practical oral ingestion studies exist.

    5.2. Alzheimer's

    In vitro*studies suggest that TUDCA incubation alongside beta-amyloid pigment, an insoluble protein involved in the pathology of Alzheimer's, was able to prevent beta-amyloid induced cell death in rat neuronal and astrocyte cells,[42]neuroblastoma cells,[43]*primary corticol neurons,[44]*and PC12 cells.[45]*Mitochondrial permeability associated with beta-amyloid induced toxicity is decreased with TUDCA[42]*and inhibits adverse changes in the mitochondria as a result of beta-amyloid toxicity.[46]

    However, TUDCA has not been implicated in actually reducing beta-amyloid levels. This suggests protective effects on cells independent of beta-amyloid presence.[2]

    5.3. Stroke

    TUDCA has shown neuroprotective actions against stroke and acute neurological injury[47][13]

    In general, TUDCA appears to be quite protective of cells and this applies to the brain as well. Orally ingested TUDCA is able to reach neuronal tissue, but relevance to humans with TUDCA ingestion has not yet been shown

    6Interactions with Glucose metabolism

    6.1. Mechanisms

    TUDCA has been demonstrated to restore glucose homeostasis in a cell culture as well as diabetic mice and increase insulin sensitivity in liver, muscle, and adipose tissue.[8]*ER stress has been linked to both obesity as well as diabetes,[48]possibly through increased ER stress inducing an adaptive unfolded protein response, and inhibiting insulin signalling via activating the JNK pathway via IRE-1.[49][50]*Whether ER stress,*per se, is a causative step in muscle tissue is not known and may be doubtful.[51]

    A study in mice at 0.5mg/kg bodyweight TUDCA suggest that thyroid hormone deiodinase enyzmes, specifically D2, play a role. Supplementation of this dose in rats has been shown to normalize glucose tolerance[8]*but this effect is not seen in mice without the D2 enzyme or mRNA (Dio2−/−*mice).[52]

    6.2. Interactions with Beta-cells

    An*in vitro*study on the interactions of TUDCA and beta-cells found that TUDCA failed to normalize insulin resistance when glucose was incubated with a cell at 6.5mmol/L but restored function at higher levels of glycermia (13 and 22mmol/L) without affecting insulin content of the cells.[53]Hyperglycemia was able to reduce mRNA production of preproinsulin (insulin precursor), and this reduction was prevented with TUDCA.[53]13mmol/L correlates to the cellular concentration of hyperglycemia[54]*and is physiologically relevant. These effects seem to be secondary to reducing ER stress.[53]

    6.3. Interventions

    TUDCA, at 1,750mg daily in obese persons without NAFLD nor type II diabetes over 4 weeks, was able to reduce insulin resistance in skeletal muscle as assessed by increased phosphorylation of Akt and IRS-1 in response to a standardized test meal.[55]No influence on insulin induced JNK activation was seen in myocytes.

    Preliminary, but TUDCA appears to be able to protect cells from dysfunction associated with hyperglycemia and may reduce the effects of insulin resistance before they happen (beta-cells) and even therapeutically with the potency of some diabetic pharmaceuticals (in regards to the liver and skeletal muscle)

    7Interactions with Fat Mass and Obesity

    7.1. Thyroid and Metabolic Rate

    Circulating Bile Acids (those not found in the liver, but the blood) have been found to be correlated with energy expenditure in humans. With correlation coefficients of 0.648 in healthy persons and 0.833 in those with cirrhosis,[56]*although other smaller studies (n=24) find no such correlations.[57]

    TUDCA has been shown*in vitro*to increase protein content and mRNA levels for the deiodinase enzyme D2 in cells expressing this protein normally; this protein converts relatively low-activity thyroid hormone T4 to T3, and incubation with TUDCA was able to double protein content of the enzyme and increase T3 levels at concentrations between 100-800uM, reaching three-fold increases at the highest level.[52]Although the delayed response to max potency and prior evidence that deiodinases are regulated post-transcriptionally,[58]*the authors noted that the increase in deiodinase mRNA (Dio2) makes it unlikely that the effects seen are secondary to protein stabilization.[52]

    When fed to mice at 0.5mg/kg bodyweight, TUDAC was unable to induce fat loss over 7 days but induced a change in respiratory quotient by 5% towards using fatty acids as substrate.[52]*Serum levels of T3 and T4 were unchanged in these animals, suggesting localized usage of T3 or a mechanism independent of thyroid hormones.[52]Another report noted small but statistically significant decreases in body weight in mice over 15-30 days, but did not specify dose of TUDCA used.[8]*It is possible that these effects are through increasing activity of the D2 receptor, which has been demonstrated in animals with 0.5% cholic acid in the diet that induced similar effects such as an increase in metabolic rate alongside a decrease in respiratory quotient (indicative of a greater % of energy from fatty acids).[59]

    These mechanisms may be relevant to humans due to muscle cells expressing the same D2 receptor, and at least cholic acid has been found to increase human myocyte mRNA of this receptor (TGR5) and similar trends were found with all tested bile acids.[59]

    7.2. Adipokines

    It has been noted that the obesity-related suppression of adiponectin content may be related to ER stress, and one rat study has shown TUDCA in diet-induced obesity was able to increase circulating adiponectin levels via the protein DsbA-L.[60]

    7.3. Interventions

    After ingestion of 1,750mg TUDCA for 4 weeks in obese but otherwise healthy persons, no significant effects were observed on body fat or weight.[55]*Insulin sensitivity was improved in skeletal muscle and the liver, but not in the adipose (body fat) tissue of these persons.[55]*This differs from previous rat studies[8]*and may be due to the dose in the rat studies being higher.

    Appears to have mechanisms to augment Thryoid Hormone actions and induce fat loss, but the dose may be too high to be practically relevant

    8Nutrient-Nutrient Interactions

    8.1. Alcohol

    Alcohol, or drinking ethanol, can be as fun as it is damaging to the liver.

    TUDCA, and its taurine-free conjugate UDCA, have been shown to attenuate the reduction of bioenergetics in a liver cell after incubation with acetaldehyde (metabolite of alcohol that does the damage) as well as significantly reduce cell death induced by ethanol when TUDCA is at 0.1mM concentration and UDCA at 0.01mM.[61]Concentrations of 0.5mM of both have shown similar mechanistic protection but slightly weaker,[62]*but dose-response is not present as higher concentrations (>0.1mM) were reported to induce cell death.[61]*TUDCA appeared to be geared towards preserving membrane function while UDCA was more potent at preserving mitochondrial function.[61]

    Most critically, these benefits were seen with co-incubation or adminstration of them both at the same time.[62][61]*When pre-loaded before ethanolic insult, they have been shown to exacerbate damage to liver cells.[61]*These effects may be secondary to alterations in the lipid membrane of cells with TUDCA/UDCA exposure.[63]

    Might alleviate alcohol's adverse effects on the liver, but appears to be needed to be taken after drinking and may be damaging if taken before

    9Safety and Toxicity

    9.1. Human Data

    Usage of 500mg TUDCA daily for one year (in persons after liver transplants) was not assocaited with any adverse effects[64]*and in otherwise healthy obese persons doses of 1,750mg have been well tolerated for up to 4 weeks.[55]

    In persons with primary biliary cirrhosis, 750mg daily for 2 months was not associated with any adverse effects[3]*and a similar population was able to tolerate 1,500mg daily for 6 months with no adverse effects.[4]

    Although TUDCA/UDCA have shown beneficial effects in a number of different experimental and clinical models as noted thus far, a randomized controlled trial evaluating the efficacy of UDCA treatment in patients with primary sclerosing cholangitis (PSC) suggest that high doses for long periods of time may be toxic.[65]

    PSC is a rare, chronic liver disease characterized by inflammatory fibrosis of the bile ducts and is typically associated with biliary cirrhosis and portal hypertension, which eventually profress to liver failure.[66]*In some cases cholangiocarcinoma, (bile duct cancer) can also develop.

    UDCA has been tested as a possible treatment for primary sclerosing cholangitis (PSC), a rare liver disease.

    Given the poor prognosis of PSC, there have been a number of trials testing the efficacy of UDCA for treating this disease. A few pilot trials testing UDCA in a dose range of 10-15 mg/kg bodyweight/day did show improvements in liver enzymes (an indicator of liver stress), and in certain cases liver histology (i.e. the appearance of liver biopsy sections under a microscope), although patient symptoms were not improved.[67][68][69]

    Given the promising improvements of clinical markers but lack of effect on symptoms in these pilot studies, researchers reasoned that the dose and/or duration of UDCA treatment was insufficient to alleviate symptoms. This was addressed in the Lindor trial, where patients with PSC were administered 28-30 mg/kg bodyweight/day UDCA or a placebo.[65]Treatments were assigned in a randomized, double-blinded fashion and liver biopsies were taken before the trial and after 5 years. The investigators were specifically examining the ability of UDCA to reduce or delay the following primary outcomes: development of cirrhosis, bile duct cancer, liver transplantation, or death. Ultimately the study was terminated after 6 years, because patients receiving the UDCA treatment were substantially worse-off than those who took the placebo. Although liver enzyme levels decreased more in the UDCA group, 39% of these patients reached one of the primary outcomes by the end of the study. In contrast, only 19% of patients that received the placebo reached a primary endpoint. Overall, patients receiving UDCA were 2.3x more likely to reach a primary endpoint and 2.1x more likely to die or require liver transplantation.[65]

    Patients in the Lindor trial were 2.3x more likely to reach an adverse primary endpoint and 2.1x more likely to die or require a liver transplant after several years of high-dose UDCA treatment.

    Why was high-dose UDCA so toxic in PSC patients?

    Although unexpected, the authors of the Lindor study speculated that high-dose UDCA may cause hepatocyte necrosis caused in part by the increased amount of bile duct obstruction associated with advanced PSC. Alternatively, high levels of UDCA in the right colon could lead to increased levels of toxic bile acids.[70]

    Scientific Support & Reference Citations

    References

    Lepercq P, et al.*Increasing ursodeoxycholic acid in the enterohepatic circulation of pigs through the administration of living bacteria.*Br J Nutr. (2005)Amaral JD, et al.*Bile acids: regulation of apoptosis by ursodeoxycholic acid.*J Lipid Res. (2009)Invernizzi P, et al.*Differences in the metabolism and disposition of ursodeoxycholic acid and of its taurine-conjugated species in patients with primary biliary cirrhosis.*Hepatology. (1999)Setchell KD, et al.*Metabolism of orally administered tauroursodeoxycholic acid in patients with primary biliary cirrhosis.*Gut. (1996)Zouboulis-Vafiadis I, Dumont M, Erlinger S.*Conjugation is rate limiting in hepatic transport of ursodeoxycholate in the rat.*Am J Physiol. (1982)Keene CD, et al.*A bile acid protects against motor and cognitive deficits and reduces striatal degeneration in the 3-nitropropionic acid model of Huntington's disease.*Exp Neurol. (2001)Bernales S, Papa FR, Walter P.*Intracellular signaling by the unfolded protein response.*Annu Rev Cell Dev Biol. (2006)Ozcan U, et al.*Chemical chaperones reduce ER stress and restore glucose homeostasis in a mouse model of type 2 diabetes.*Science. (2006)Ben Mosbah I, et al.*Endoplasmic reticulum stress inhibition protects steatotic and non-steatotic livers in partial hepatectomy under ischemia-reperfusion.*Cell Death Dis. (2010)Gao X, et al.*The nephroprotective effect of tauroursodeoxycholic Acid on ischaemia/reperfusion-induced acute kidney injury by inhibiting endoplasmic reticulum stress.Basic Clin Pharmacol Toxicol. (2012)Hertl M, et al.*In vivo protection of the pig liver against ischemia/reperfusion injury by tauroursodeoxycholate.Langenbecks Arch Surg. (1999)Anderson CD, et al.*Endoplasmic reticulum stress is a mediator of posttransplant injury in severely steatotic liver allografts.Liver Transpl. (2011)Rodrigues CM, et al.*Neuroprotection by a bile acid in an acute stroke model in the rat.*J Cereb Blood Flow Metab. (2002)Amin A, et al.*Chronic inhibition of endoplasmic reticulum stress and inflammation prevents ischaemia-induced vascular pathology in type II diabetic mice.*J Pathol. (2012)Achard CS, Laybutt DR.*Lipid-induced endoplasmic reticulum stress in liver cells results in two distinct outcomes: adaptation with enhanced insulin signaling or insulin resistance.Endocrinology. (2012)Falasca L, et al.*Protective role of tauroursodeoxycholate during harvesting and cold storage of human liver: a pilot study in transplant recipients.*Transplantation. (2001)Marzioni M, et al.*Ca2+-dependent cytoprotective effects of ursodeoxycholic and tauroursodeoxycholic acid on the biliary epithelium in a rat model of cholestasis and loss of bile ducts.Am J Pathol. 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(1997)Therapy of gallstone disease: What it was, what it is, what it will be.Lanzini A, Northfield TC.*Pharmacological treatment of gallstones. Practical guidelines.*Drugs. (1994)Portincasa P, et al.*Medicinal treatments of cholesterol gallstones: old, current and new perspectives.*Curr Med Chem. (2009)Diseases of the Liver and Biliary System, Eleventh Edition.Lanzini A, Facchinetti D, Northfield TC.*Maintenance of hepatic bile acid secretion rate during overnight fasting by bedtime bile acid administration.*Gastroenterology. (1988)Kupfer RM, Maudgal DP, Northfield TC.*Gallstone dissolution rate during chenic acid therapy. Effect of bedtime administration plus low cholesterol diet.*Dig Dis Sci. (1982)Paumgartner G, Pauletzki J, Sackmann M.*Ursodeoxycholic acid treatment of cholesterol gallstone disease.*Scand J Gastroenterol Suppl. (1994)Bazzoli F, et al.*Acquired gallstone opacification during cholelitholytic treatment with chenodeoxyholic, ursodeoxycholic, and tauroursodeoxycholic acids.*Am J Gastroenterol. (1995)Rodrigues CM, et al.*Tauroursodeoxycholic acid partially prevents apoptosis induced by 3-nitropropionic acid: evidence for a mitochondrial pathway independent of the permeability transition.*J Neurochem. (2000)Keene CD, et al.*Tauroursodeoxycholic acid, a bile acid, is neuroprotective in a transgenic animal model of Huntington's disease.*Proc Natl Acad Sci U S A. (2002)Ved R, et al.*Similar patterns of mitochondrial vulnerability and rescue induced by genetic modification of alpha-synuclein, parkin, and DJ-1 in Caenorhabditis elegans.*J Biol Chem. (2005)Duan WM, et al.*Tauroursodeoxycholic acid improves the survival and function of nigral transplants in a rat model of Parkinson's disease.*Cell Transplant. (2002)Rodrigues CM, et al.*Bilirubin and amyloid-beta peptide induce cytochrome c release through mitochondrial membrane permeabilization.*Mol Med. (2000)Ramalho RM, et al.*Tauroursodeoxycholic acid modulates p53-mediated apoptosis in Alzheimer's disease mutant neuroblastoma cells.*J Neurochem. (2006)Ramalho RM, et al.*Apoptosis in transgenic mice expressing the P301L mutated form of human tau.*Mol Med. (2008)Ramalho RM, et al.*Inhibition of the E2F-1/p53/Bax pathway by tauroursodeoxycholic acid in amyloid beta-peptide-induced apoptosis of PC12 cells.*J Neurochem. (2004)Rodrigues CM, et al.*Amyloid beta-peptide disrupts mitochondrial membrane lipid and protein structure: protective role of tauroursodeoxycholate.*Biochem Biophys Res Commun. (2001)Rodrigues CM, et al.*Tauroursodeoxycholic acid reduces apoptosis and protects against neurological injury after acute hemorrhagic stroke in rats.*Proc Natl Acad Sci U S A. (2003)Ozcan U, et al.*Endoplasmic reticulum stress links obesity, insulin action, and type 2 diabetes.*Science. (2004)Hirosumi J, et al.*A central role for JNK in obesity and insulin resistance.*Nature. (2002)Urano F, et al.*Coupling of stress in the ER to activation of JNK protein kinases by transmembrane protein kinase IRE1.*Science. (2000)Rieusset J, et al.*Reduction of endoplasmic reticulum stress using chemical chaperones or Grp78 overexpression does not protect muscle cells from palmitate-induced insulin resistance.Biochem Biophys Res Commun. (2012)da-Silva WS, et al.*The chemical chaperones tauroursodeoxycholic and 4-phenylbutyric acid accelerate thyroid hormone activation and energy expenditure.*FEBS Lett. (2011)Tang C, et al.*Glucose-induced beta cell dysfunction in vivo in rats: link between oxidative stress and endoplasmic reticulum stress.*Diabetologia. (2012)Boden G, et al.*Effects of prolonged glucose infusion on insulin secretion, clearance, and action in normal subjects.*Am J Physiol. (1996)Kars M, et al.*Tauroursodeoxycholic Acid may improve liver and muscle but not adipose tissue insulin sensitivity in obese men and women.*Diabetes. (2010)Ockenga J, et al.*Plasma bile acids are associated with energy expenditure and thyroid function in humans.*J Clin Endocrinol Metab. (2012)Brufau G, et al.*Plasma bile acids are not associated with energy metabolism in humans.*Nutr Metab (Lond). (2010)Sagar GD, et al.*Ubiquitination-induced conformational change within the deiodinase dimer is a switch regulating enzyme activity.*Mol Cell Biol. (2007)Watanabe M, et al.*Bile acids induce energy expenditure by promoting intracellular thyroid hormone activation.*Nature. (2006)Zhou L, et al.*DsbA-L alleviates endoplasmic reticulum stress-induced adiponectin downregulation.*Diabetes. (2010)Henzel K, et al.*Toxicity of ethanol and acetaldehyde in hepatocytes treated with ursodeoxycholic or tauroursodeoxycholic acid.*Biochim Biophys Acta. (2004)Neuman MG, et al.*Effect of tauroursodeoxycholic and ursodeoxycholic acid on ethanol-induced cell injuries in the human Hep G2 cell line.*Gastroenterology. (1995)Leuschner U, et al.*TUDCA and UDCA are incorporated into hepatocyte membranes: different sites, but similar effects.*Ital J Gastroenterol. (1995)Angelico M, et al.*One-year pilot study on tauroursodeoxycholic acid as an adjuvant treatment after liver transplantation.*Ital J Gastroenterol Hepatol. (1999)Lindor KD, et al.*High-dose ursodeoxycholic acid for the treatment of primary sclerosing cholangitis.*Hepatology. (2009)Maggs JR, Chapman RW.*An update on primary sclerosing cholangitis.*Curr Opin Gastroenterol. (2008)O'Brien CB, et al.*Ursodeoxycholic acid for the treatment of primary sclerosing cholangitis: a 30-month pilot study.Hepatology. (1991)Beuers U, et al.*Ursodeoxycholic acid for treatment of primary sclerosing cholangitis: a placebo-controlled trial.*Hepatology. (1992)Stiehl A, et al.*Effect of ursodeoxycholic acid on liver and bile duct disease in primary sclerosing cholangitis. A 3-year pilot study with a placebo-controlled study period.*J Hepatol. (1994)Chapman RW.*High-dose ursodeoxycholic acid in the treatment of primary sclerosing cholangitis: throwing the urso out with the bathwater?.*Hepatology. (2009)

    Via HEM and FAQ:

    Crosignani A, et al.*Tauroursodeoxycholic acid for the treatment of HCV-related chronic hepatitis: a multicenter placebo-controlled study.*Hepatogastroenterology. (1998)Larghi A, et al.*Ursodeoxycholic and tauro-ursodeoxycholic acids for the treatment of primary biliary cirrhosis: a pilot crossover study.*Aliment Pharmacol Ther. (1997)Crosignani A, et al.*Tauroursodeoxycholic acid for treatment of primary biliary cirrhosis. A dose-response study.*Dig Dis Sci. (1996)

    (Common misspellings for Tauroursodeoxycholic Acid include TURD, TURDA, TUCDA)


    This guide sums up over 5000 human studies into a monster 1500+ page reference that clearly tells you what works (and what doesn't)*
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    SORRY MAN, THE SUPPLEMENT FORUM WAS MODERATED THIS WHOLE TIME, I HAD NO IDEA
    TUDCA more than just a liver aid.

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    Well worth the money!
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    Its ok just lost on why it didnt post at the time lmao thanks for fixing
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    I love TUDCA, seems its starting to become pretty popular Allmax just put one out, so did SNS, everyones rolling out TUDCA supps right now
     

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