Tretinoin Explained

Watchedfields:changed
Verifiedrevid:470612798
Width:275
Pronounce:See pronunciation note
Tradename:Retin-a, Avita, Renova, others
Drugs.Com:
Topical
Dailymedid:Tretinoin
Pregnancy Au:X
Pregnancy Au Comment:/ (Oral); D (Topical)[1] [2]
Routes Of Administration:Topical, by mouth
Atc Prefix:D10
Atc Suffix:AD01
Atc Supplemental:,
Legal Au:S4
Legal Br:C2
Legal Br Comment:[3]
Legal Uk:POM
Legal Us:Rx-only
Legal Eu:Rx-only
Legal Eu Comment:[4]
Protein Bound:> 95%
Elimination Half-Life:0.5–2 hours
Cas Number:302-79-4
Pubchem:444795
Iuphar Ligand:2644
Drugbank:DB00755
Chemspiderid:392618
Unii:5688UTC01R
Kegg:D00094
Kegg2:C00777
Chebi:15367
Chembl:38
Synonyms:ATRA
Iupac Name:(2E,4E,6E,8E)-3,7-Dimethyl-9-(2,6,6-trimethylcyclohexen-1-yl)nona-2,4,6,8-tetraenoic acid
C:20
H:28
O:2
Smiles:CC1=C(C(CCC1)(C)C)C=CC(=CC=CC(=CC(=O)O)C)C
Stdinchi:1S/C20H28O2/c1-15(8-6-9-16(2)14-19(21)22)11-12-18-17(3)10-7-13-20(18,4)5/h6,8-9,11-12,14H,7,10,13H2,1-5H3,(H,21,22)/b9-6+,12-11+,15-8+,16-14+
Stdinchikey:SHGAZHPCJJPHSC-YCNIQYBTSA-N
Melting Point:180

Tretinoin, also known as all-trans retinoic acid (ATRA), is a medication used for the treatment of acne and acute promyelocytic leukemia.[5] [6] For acne, it is applied to the skin as a cream, gel or ointment. For acute promyelocytic leukemia, it is effective only when the RARA-PML fusion mutation is present[7] and is taken by mouth for up to three months.[8] Topical tretinoin is also the most extensively investigated retinoid therapy for photoaging.[9]

Common side effects when used as a cream are limited to the skin and include skin redness, peeling, and sun sensitivity. When taken by mouth, side effects include hypertriglyceridemia, hypercholesterolemia, shortness of breath, headache, numbness, depression, skin dryness, itchiness, hair loss, vomiting, muscle pains, and vision changes. Other severe side effects include high white blood cell counts and blood clots. Use during pregnancy is contraindicated due to the risk of birth defects. It is in the retinoid family of medications.

Tretinoin was patented in 1957, and approved for medical use in 1962.[10] It is on the World Health Organization's List of Essential Medicines.[11] Tretinoin is available as a generic medication.[12] In 2021, it was the 206th most commonly prescribed medication in the United States, with more than 2million prescriptions.[13] [14]

Medical uses

Skin use

Acne

Tretinoin is most commonly used to treat acne, both inflammatory and noninflammatory. Multiple studies support the efficacy of topical retinoids in the treatment of acne vulgaris.[15] [16] It is sometimes used in conjunction with other topical acne medications to enhance their penetration.[17] In addition to treating active acne, retinoids accelerate the resolution of acne-induced postinflammatory hyperpigmentation.[18] It is also useful as maintenance therapy for people who have responded well to their initial treatment, reducing the prolonged use of antibiotics for acne.[19]

Photoaging

Photoaging is premature skin aging resulting from prolonged and repeated exposure to solar radiation. Features of photoaging include fine and coarse wrinkles, change in skin pigmentation, and loss of elasticity. In human skin, topical retinoids increase collagen production, induce epidermal hyperplasia, and decrease keratinocyte and melanocyte atypia. Topical tretinoin is the most extensively investigated retinoid therapy for photoaging.[20] Topical tretinoin can be used for mild to severe photoaging in people of all skin types. Several weeks or months of use are typically required before improvement is appreciated. Although it has only been studied for a duration of two years, it may be continued indefinitely. A long-term maintenance regimen with a lower concentration or less frequent application may be an alternative to continued use.[21]

Leukemia

Tretinoin is used to induce remission in people with acute promyelocytic leukemia (APL) who have a mutation (the t(15;17) translocation that gives rise to the PML::RARα fusion gene). It is not used for maintenance therapy.[22] [23] [24]

Tretinoin is not effective for the treatment of non-APL forms of Acute Myeloid Leukemia[25] or other forms of leukemia. Preclinical studies and clinical data analysis suggests that retinoic acid promotes the growth of T cell acute lymphoblastic leukemia.[26]

Side effects

Dermatology

Topical tretinoin is for use only on the skin and should not be applied to eyes or mucosal tissues. Common side effects include skin irritation, redness, swelling, and blistering.[27] If irritation is a problem, a decrease in the frequency of application to every other or every third night can be considered, and the frequency of application can be increased as tolerance improves. The fine skin flaking that is often seen can be gently exfoliated with a washcloth. A non-comedogenic facial moisturizer can also be applied if needed. Delaying application of the retinoid for at least 20 minutes after washing and drying the face may also be helpful. Topical retinoids are not true photosensitizing drugs, but people using topical retinoids have described symptoms of increased sun sensitivity. This is thought to be due to thinning of the stratum corneum leading to a decreased barrier against ultraviolet light exposure, as well as an enhanced sensitivity due to the presence of cutaneous irritation.[28]

Acute Promyelocytic Leukemia

The oral form of the drug has boxed warnings concerning the risks of retinoic acid syndrome and leukocytosis. Other significant side effects include a risk of thrombosis, benign intracranial hypertension in children, high lipids (hypercholesterolemia and/or hypertriglyceridemia), and liver damage.

There are many significant side effects from this drug that include malaise (66%), shivering (63%), hemorrhage (60%), infections (58%), peripheral edema (52%), pain (37%), chest discomfort (32%), edema (29%), disseminated intravascular coagulation (26%), weight increase (23%), injection site reactions (17%), anorexia (17%), weight decrease (17%), and myalgia (14%).

Respiratory side effects usually signify retinoic acid syndrome, and include upper respiratory tract disorders (63%), dyspnea (60%), respiratory insufficiency (26%), pleural effusion (20%), pneumonia (14%), rales (14%), and expiratory wheezing (14%), and many others at less than 10%. Around 23% of people taking the drug have reported earache or a feeling of fullness in their ears. Gastrointestinal disorders include bleeding (34%), abdominal pain (31%), diarrhea (23%), constipation (17%), dyspepsia (14%), and swollen belly (11%) and many others at less than 10%.

Cardiovascular side effects include arrhythmias (23%), flushing (23%), hypotension (14%), hypertension (11%), phlebitis (11%), and cardiac failure (6%) and for 3% of patients: cardiac arrest, myocardial infarction, enlarged heart, heart murmur, ischemia, stroke, myocarditis, pericarditis, pulmonary hypertension, secondary cardiomyopathy.

In the nervous system, side effects include dizziness (20%), paresthesias (17%), anxiety (17%), insomnia (14%), depression (14%), confusion (11%), and many others at less than 10% frequency.

In the urinary system, side effects include chronic kidney disease (11%) and several others at less than 10% frequency.

Mechanism of action

For its use in Acute Promyelocytic Leukemia, tretinoin causes the RARA:PML fusion oncogene to degrade, resulting in the loss of the key driver oncogene.[29] This degradation allows the blasts to mature and results in dramatic responses. This response is typically short-lived as Cyp26 genes are rapidly upregulated to degrade tretinoin. The RARA:PML oncogene is not present in other cancer types, thus explaining why tretinoin and other retinoids have not been effective across hundreds of different trials.[30]

For its use in acne, tretinoin (along with other retinoids) are vitamin A derivatives that act by binding to two nuclear receptor families within keratinocytes: the retinoic acid receptors (RAR) and the retinoid X receptors (RXR). These events contribute to the normalization of follicular keratinization and decreased cohesiveness of keratinocytes, resulting in reduced follicular occlusion and microcomedone formation.[31] The retinoid-receptor complex competes for coactivator proteins of AP-1, a key transcription factor involved in inflammation. Retinoids also down-regulate expression of toll-like receptor (TLR)-2, which has been implicated in the inflammatory response in acne.[32] Moreover, tretinoin and retinoids may enhance the penetration of other topical acne medications.

The combination of the 10% benzoyl peroxide and light results in more than 50% degradation of tretinoin in about 2 hours and 95% in 24 hours.[33] This lack of stability in the presence of light and oxidizing agents has led to the development of novel formulations of the drug. When microencapsulated tretinoin is exposed to benzoyl peroxide and light only 1% degradation takes place in about 4 hours and only 13% after 24 hours.[34]

The biological mechanism behind triglyceride and cholesterol elevations remains under investigation.

Synthesis

All-trans retinoic acid is produced by the body from dietary factors including retinol, retinyl esters or beta-carotene. The beta-carotene is first cleaved by beta-carotene 15-15'-monooxygenase to retinol which is subsequently oxidized by RDH and ALDH enzymes to produce all-trans retinoic acid (see retinoic acid). Tretinoin is produced synthetically using standard industrial practices.[35]

History

Tretinoin was co-developed for its use in acne by James Fulton and Albert Kligman when they were at University of Pennsylvania in the 1960s.[36] [37] Phase I trials, the first conducted on human subjects, were performed on inmates at Holmesburg Prison during a long-running regime of non-therapeutic and unethical testing on prison inmates at Holmesburg.[38] [39] The University of Pennsylvania held the patent for Retin-A, which it licensed to pharmaceutical companies.

Treatment of acute promyelocytic leukemia was first introduced at Ruijin Hospital in Shanghai by Wang Zhenyi in a 1988 clinical trial.[40]

Etymology

The origin of the name tretinoin is uncertain, although several sources agree (one with probability,< one with asserted certainty) that it probably comes from trans- + retinoic [acid] + -in, which is plausible given that tretinoin is the all-trans isomer of retinoic acid. The name isotretinoin is the same root tretinoin plus the prefix iso-. Regarding pronunciation, the following variants apply equally to both tretinoin and isotretinoin. Given that retinoic is pronounced, it is natural that is a commonly heard pronunciation. Dictionary transcriptions also include and .

Hair loss

Tretinoin has been explored as a treatment for hair loss, potentially as a way to increase the ability of minoxidil (by acting as an enzyme and accelerating the production of minoxidil sulfate) to penetrate the scalp, but the evidence is weak and contradictory.[41] [42]

External links

Notes and References

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  2. Web site: Tretinoin topical Use During Pregnancy . Drugs.com . 1 July 2019 . 16 January 2020.
  3. Web site: Anvisa . Brazilian Health Regulatory Agency . 31 March 2023 . RDC Nº 784 - Listas de Substâncias Entorpecentes, Psicotrópicas, Precursoras e Outras sob Controle Especial . Collegiate Board Resolution No. 784 - Lists of Narcotic, Psychotropic, Precursor, and Other Substances under Special Control. live . https://web.archive.org/web/20230803143925/https://www.in.gov.br/en/web/dou/-/resolucao-rdc-n-784-de-31-de-marco-de-2023-474904992 . 3 August 2023 . 15 August 2023 . . pt-BR . 4 April 2023.
  4. Web site: List of nationally authorised medicinal products:Active substance(s): tretinoin (oral formulations) . ema.europa.eu . European Medicines Agency . https://web.archive.org/web/20230130131600/https://www.ema.europa.eu/en/documents/psusa/tretinoin-oral-formulations-list-nationally-authorised-medicinal-products-psusa/00003015/202203_en.pdf . 30 January 2023 . 1 December 2022 . live.
  5. Book: Tivnan A . Resistance to Targeted Therapies Against Adult Brain Cancers . 2016 . Springer . 978-3-319-46505-0 . 123 . live . https://web.archive.org/web/20171105200032/https://books.google.ca/books?id=XaCYDQAAQBAJ&pg=PA123 . 5 November 2017.
  6. Book: British national formulary : BNF 69 . 2015 . British Medical Association . 978-0-85711-156-2 . 627, 821–822 . 69.
  7. Yoshida H, Kitamura K, Tanaka K, Omura S, Miyazaki T, Hachiya T, Ohno R, Naoe T . Accelerated degradation of PML-retinoic acid receptor alpha (PML-RARA) oncoprotein by all-trans-retinoic acid in acute promyelocytic leukemia: possible role of the proteasome pathway . Cancer Research . 56 . 13 . 2945–2948 . July 1996 . 8674046 .
  8. Web site: Tretinoin . The American Society of Health-System Pharmacists . 8 December 2016 . live . https://web.archive.org/web/20161130124932/https://www.drugs.com/monograph/tretinoin.html . 30 November 2016.
  9. Web site: Retinoids, topical. American Osteopathic College of Dermatology.
  10. Book: Fischer J, Ganellin CR . Analogue-based Drug Discovery . 2006 . John Wiley & Sons . 978-3-527-60749-5 . 476 . live . https://web.archive.org/web/20171105200032/https://books.google.ca/books?id=FjKfqkaKkAAC&pg=PA476 . 5 November 2017.
  11. Book: ((World Health Organization)) . World Health Organization model list of essential medicines: 21st list 2019 . 2019 . 10665/325771 . World Health Organization . World Health Organization . Geneva . WHO/MVP/EMP/IAU/2019.06. License: CC BY-NC-SA 3.0 IGO . free.
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  13. Web site: The Top 300 of 2021 . ClinCalc . 14 January 2024 . 15 January 2024 . https://web.archive.org/web/20240115223848/https://clincalc.com/DrugStats/Top300Drugs.aspx . live .
  14. Web site: Tretinoin - Drug Usage Statistics . ClinCalc . 14 January 2024.
  15. Leyden JJ, Shalita A, Thiboutot D, Washenik K, Webster G . Topical retinoids in inflammatory acne: a retrospective, investigator-blinded, vehicle-controlled, photographic assessment . Clinical Therapeutics . 27 . 2 . 216–24 . February 2005 . 15811485 . 10.1016/j.clinthera.2005.02.009.
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  17. Gollnick H, Cunliffe W, Berson D, Dreno B, Finlay A, Leyden JJ, Shalita AR, Thiboutot D . Management of acne: a report from a Global Alliance to Improve Outcomes in Acne . Journal of the American Academy of Dermatology . 49 . 1 Suppl . S1-37 . July 2003 . 12833004 . 10.1067/mjd.2003.618 . Global Alliance to Improve Outcomes in Acne.
  18. Book: Kang S, Voorhees JJ . Topical retinoids. . Fitzpatrick's Dermatology in General Medicine . 7th . Wolff K, Goldsmith LA, Katz SI, etal . McGraw Hill . New York . 2008 . 2106 .
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  20. Han A, Chien AL, Kang S . Photoaging . Dermatologic Clinics . 32 . 3 . 291–9, vii . July 2014 . 24891052 . 10.1016/j.det.2014.03.015.
  21. Kang S, Bergfeld W, Gottlieb AB, Hickman J, Humeniuk J, Kempers S, Lebwohl M, Lowe N, McMichael A, Milbauer J, Phillips T, Powers J, Rodriguez D, Savin R, Shavin J, Sherer D, Silvis N, Weinstein R, Weiss J, Hammerberg C, Fisher GJ, Nighland M, Grossman R, Nyirady J . Long-term efficacy and safety of tretinoin emollient cream 0.05% in the treatment of photodamaged facial skin: a two-year, randomized, placebo-controlled trial . American Journal of Clinical Dermatology . 6 . 4 . 245–53 . 2005 . 16060712 . 10.2165/00128071-200506040-00005 . 40127961.
  22. Web site: Tretinoin capsule . DailyMed . 12 December 2018 . 16 January 2020.
  23. Huang ME, Ye YC, Chen SR, Chai JR, Lu JX, Zhoa L, Gu LJ, Wang ZY . Use of all-trans retinoic acid in the treatment of acute promyelocytic leukemia . Blood . 72 . 2 . 567–72 . August 1988 . 3165295 . 10.1182/blood.V72.2.567.567 . free .
  24. Castaigne S, Chomienne C, Daniel MT, Ballerini P, Berger R, Fenaux P, Degos L . All-trans retinoic acid as a differentiation therapy for acute promyelocytic leukemia. I. Clinical results . Blood . 76 . 9 . 1704–9 . November 1990 . 2224119 . 10.1182/blood.V76.9.1704.1704 . free .
  25. Küley-Bagheri Y, Kreuzer KA, Monsef I, Lübbert M, Skoetz N . Effects of all-trans retinoic acid (ATRA) in addition to chemotherapy for adults with acute myeloid leukaemia (AML) (non-acute promyelocytic leukaemia (non-APL)) . The Cochrane Database of Systematic Reviews . 2018 . CD011960 . August 2018 . 8 . 30080246 . 6513628 . 10.1002/14651858.CD011960.pub2 . Cochrane Haematological Malignancies Group.
  26. Ono Y, Fukuhara N, Yoshie O . TAL1 and LIM-only proteins synergistically induce retinaldehyde dehydrogenase 2 expression in T-cell acute lymphoblastic leukemia by acting as cofactors for GATA3 . Molecular and Cellular Biology . 18 . 12 . 6939–6950 . December 1998 . 9819382 . 109277 . 10.1128/MCB.18.12.6939 .
  27. Web site: Tretinoin Cream- tretinoin cream . DailyMed . 1 December 2018 . 16 January 2020.
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  29. Yoshida H, Kitamura K, Tanaka K, Omura S, Miyazaki T, Hachiya T, Ohno R, Naoe T . Accelerated degradation of PML-retinoic acid receptor alpha (PML-RARA) oncoprotein by all-trans-retinoic acid in acute promyelocytic leukemia: possible role of the proteasome pathway . Cancer Research . 56 . 13 . 2945–2948 . July 1996 . 8674046 .
  30. Esposito M, Amory JK, Kang Y . The pathogenic role of retinoid nuclear receptor signaling in cancer and metabolic syndromes . The Journal of Experimental Medicine . 221 . 9 . September 2024 . 39133222 . 10.1084/jem.20240519 . free .
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  32. Liu PT, Krutzik SR, Kim J, Modlin RL . Cutting edge: all-trans retinoic acid down-regulates TLR2 expression and function . Journal of Immunology . 174 . 5 . 2467–70 . March 2005 . 15728448 . 10.4049/jimmunol.174.5.2467 . 20740543 . free.
  33. Martin B, Meunier C, Montels D, Watts O . Chemical stability of adapalene and tretinoin when combined with benzoyl peroxide in presence and in absence of visible light and ultraviolet radiation . The British Journal of Dermatology . 139 . Suppl 52 . 8–11 . October 1998 . 9990414 . 10.1046/j.1365-2133.1998.1390s2008.x . Wiley . 43287596 .
  34. Web site: The Stability of Tretinoin in Tretinoin Gel Microsphere 0.1%. 14 May 2021. www.mdedge.com. en.
  35. Web site: WIPO - Search International and National Patent Collections . 2024-08-15 . patentscope.wipo.int.
  36. Web site: Vivant Pharmaceuticals, LLC Press Release . 10 July 2013 . Vivant Skin Care Co-founder James E. Fulton, MD, Loses Colon Cancer Battle . https://web.archive.org/web/20160418081737/http://vivantskin.blogspot.com/2013/07/vivant-skin-care-co-founder-james-e.html . 18 April 2016 .
  37. Web site: Gellene D . The New York Times . 22 February 2010 . Dr. Albert M. Kligman, Dermatologist, Dies at 93.
  38. Book: Washington HA . Medical apartheid : the dark history of medical experimentation on Black Americans from colonial times to the present . 2006 . Doubleday . 0-385-50993-6 . New York . 61131882.
  39. Book: Hornblum AM . Acres of skin : human experiments at Holmesburg Prison : a story of abuse and exploitation in the name of medical science . 1998 . Routledge . 0-415-91990-8 . New York . 37884781.
  40. Huang ME, Ye YC, Chen SR, Chai JR, Lu JX, Zhoa L, Gu LJ, Wang ZY . Use of all-trans retinoic acid in the treatment of acute promyelocytic leukemia . Blood . 72 . 2 . 567–72 . August 1988 . 3165295 . 10.1182/blood.V72.2.567.567 . free.
  41. Book: Trüeb RM . Diagnosis and Treatment . The Difficult Hair Loss Patient: Guide to Successful Management of Alopecia and Related Conditions. . 2015 . Springer . Cham . 978-3-319-19701-2 . https://books.google.com/books?id=0ue5BAAAQBAJ&pg=PA95 . https://web.archive.org/web/20171105200032/https://books.google.com/books?id=0ue5BAAAQBAJ&pg=PA95 . 5 November 2017.
  42. Rogers NE, Avram MR . Medical treatments for male and female pattern hair loss . Journal of the American Academy of Dermatology . 59 . 4 . 547–66; quiz 567–8 . October 2008 . 18793935 . 10.1016/j.jaad.2008.07.001.