Different testosterone routes and dosages can achieve widely varying circulating testosterone levels.[2] For purposes of comparison with normal physiological circumstances, circulating levels of total testosterone in men range from about 250 to 1,100 ng/dL (mean 630 ng/dL) and in women range from about 2 to 50 ng/dL (mean 32 ng/dL).[4][5][6][7] Testosterone levels decline with age in men.[8] In women with polycystic ovary syndrome (PCOS), a condition of androgen excess, testosterone levels are typically around 50 to 80 ng/dL, with a range of about 30 to 140 ng/dL.[9][10][7] Total testosterone levels are about 20-fold and free testosterone levels about 40-fold higher in men than in women on average.[11] Similarly, testosterone production is approximately 30 times higher in men than in women.[12]
^This table does not include combination products with other medications/hormones. The availability of specific products may vary by country - see Testosterone (medication) § Availability.
^These dosages may be given at varying frequencies - dosages listed are "each" (ex: per tablet, per spray, etc) and not indicative of total daily dose or equivalent.
^Other brand names may be currently or historically marketed.
Notes: Men produce about 3 to 11 mg of testosterone per day (mean 7 mg/day in young men). Footnotes:a = Never marketed. b = No longer used and/or no longer marketed. Sources: See template.
Notes:Premenopausal women produce about 230 ± 70 μg testosterone per day (6.4 ± 2.0 mg testosterone per 4 weeks), with a range of 130 to 330 μg per day (3.6–9.2 mg per 4 weeks). Footnotes:a = Mostly discontinued or unavailable. b = Over-the-counter. Sources: See template.
Testosterone is well-absorbed but extensively metabolized with oral administration due to the first pass through the intestines and liver.[2][27][28][3] It is rapidly and completely inactivated in men at doses of less than 200 mg.[2][27] In large doses, such as 200 mg however, significant increases in circulating testosterone levels become apparent.[2][27] In addition, while a 60 mg dose has no effect on testosterone levels in men, this dose does measurably increase testosterone levels in prepubertal boys and women.[27] The oral bioavailability of testosterone in young women after a single 25 mg dose was found to be 3.6 ± 2.5%.[29] High levels of testosterone are also achieved with a 60 mg dose of oral testosterone in men with liver cirrhosis.[2] These findings are attributed to induction of liverenzymes by testosterone and consequent activation of its own metabolism.[2][27] Substitution dosages of oral testosterone in men are in the range of 400 to 800 mg/day.[27][28] Such doses exceed the amount of testosterone produced by the body, which is approximately 7 mg/day, by approximately 100-fold.[2][27][28] The elimination half-life of oral testosterone is rapid at about 5 to 7 hours.[28][30] As a result, it requires administration several times per day in divided doses.[28] Due to its limitations, such as the high doses required and necessity of multiple daily doses, oral testosterone is not used clinically in its unmodified form.[28][3]
Instead of in its free unesterified form, testosterone is used by oral administration in the form of testosterone undecanoate.[2] Due to the unique chemical properties afforded by its long fatty acid ester chain, this testosterone ester is partially absorbed from the gastrointestinal tract into the lymphatic system, thereby bypassing a portion of first-pass metabolism in the liver and producing measurable increases in testosterone levels at much lower doses than free testosterone.[2][3] Of oral testosterone undecanoate that reaches circulation, 90 to 100% is transported lymphatically.[32] However, its duration remains short, with an elimination half-life of 1.6 hours and a mean residence time of 3.7 hours.[33][34][35] Oral testosterone undecanoate is provided as 40 mg oil-filled capsules and requires administration 2 to 4 times per day (i.e., 80 to 160 mg/day) for substitution in men.[2][33][3] It must be taken with food containing at least a moderate or "normal" amount of fat in order to achieve adequate absorption.[2][36][37][38] In addition, there is very high interindividual variability in levels of testosterone with oral testosterone undecanoate.[39] The bioavailability of oral testosterone undecanoate taken with food is 3 to 7%.[32][40] Inappropriately high levels of testosterone have been observed with 10 to 40 mg/day oral testosterone undecanoate in women.[41][42] The oral bioavailability of testosterone undecanoate in young women after a single 40 mg dose was found to be 6.8 ± 3.3%.[29]
A novel self-emulsifying formulation of oral testosterone undecanoate in 300-mg capsules for use once per day is under development.[39]
Testosterone can be used by sublingual administration.[2][44][45] A 10 mg sublingual tablet with the brand name Testoral was previously marketed for use one to four times per day in men.[46]
Transdermal testosterone gel has a bioavailability of about 8 to 14% when administered to recommended skin sites including the abdomen, arms, shoulders, and thighs.[48][49]Scrotal skin is the thinnest skin of the body[50] and has enhanced absorption characteristics relative to other skin areas.[51][52][53][54] Application of testosterone gels and creams to the scrotum has been studied and achieves much higher levels of testosterone than conventional skin sites.[55][56][57][58] Scrotal application of testosterone requires approximately 5-fold lower doses relative to non-scrotal application.[59][50]
The development of transdermal preparations of testosterone (and of progesterone)[60] has been more difficult than the case of estradiol.[50] This is because testosterone levels in men are about 100 to 1,000 times higher than estradiol levels in women (300 to 1,000 ng/dL vs. 50 to 150 pg/mL, respectively).[50] Non-scrotal testosterone patches were assessed and were found to be ineffective in raising testosterone levels in men.[50] As a result, scrotal testosterone patches were initially marketed.[50] Subsequently, however, non-scrotal testosterone patches with special permeation enhancers that could successfully increase testosterone levels were developed and marketed.[50] However, non-scrotal testosterone patches nonetheless require a large skin area for application (up to 60 cm2) and must be replaced daily.[50]
Supraphysiological levels of dihydrotestosterone (DHT) occur with scrotal application of testosterone, whereas this does not occur with non-scrotal transdermal application.[50] This is due to the high expression of 5α-reductase in scrotal skin.[50] Estradiol levels are similar with scrotal versus non-scrotal application of transdermal testosterone.[50]
Low-dose transdermal testosterone patches in women have been found to result in testosterone levels of 64 ng/dL with 150 μg/day and 102 ng/dL with 300 μg/day.[41] When testosterone is used transdermally in women or trans men, hair growth at the application sites can happen.[61]
Testosterone was marketed as a suppository for rectal administration by Ferring Pharmaceuticals from the early 1960s under brand names such as Rektandron and Testosteron.[43][25][26] Rectal administration of testosterone avoids the first-pass effect with oral administration similarly to other non-oral routes.[2] A single 40 mg dose of rectal testosterone has been found to result in maximal testosterone levels of almost 1,200 ng/dL within 30 minutes.[27] Subsequently, testosterone levels steadily decline, reaching levels of about 700 ng/dL after 4 hours and levels of about 400 ng/dL after 8 hours.[27] Other studies have also assessed the use of rectal testosterone, with similar findings.[2][68][69][70][71][72] Rectal use of testosterone requires administration two or three times per day to maintain adequate testosterone levels.[27][2] The route is poorly accepted, owing to its inconvenience.[2] Rectal testosterone has been used in transmasculine hormone therapy.[69]
The bioavailability of drugs that are administered intramuscularly is generally almost 95%.[73]
As oil solutions by intramuscular injection, the elimination half-lives of testosterone esters are 0.8 days for testosterone propionate, 4.5 days for testosterone enanthate, 20.9 days (in tea seed oil) and 33.9 days (in caster oil) for testosterone undecanoate, and 29.5 days for testosterone buciclate.[8][33] The pharmacokinetics of testosterone cypionate are said to be the same as those of testosterone enanthate, with "extremely comparable" patterns of testosterone release.[35][33] Due to their varying and different elimination half-lives, the different intramuscular testosterone esters are administered with differing frequencies.[74] Testosterone propionate is injected two to three times per week, testosterone enanthate and testosterone cypionate are injected once every two to four weeks, and testosterone undecanoate and testosterone buciclate are injected once every 10 to 14 weeks.[74] Due to its relatively short duration, testosterone propionate is now relatively little used and testosterone undecanoate is the preferred testosterone ester for intramuscular use.[8][33] Testosterone undecanoate and testosterone buciclate can be injected intramuscularly as infrequently as four times per year.[8][33]
High doses of testosterone esters by intramuscular injection have been studied in healthy young men.[75] Levels of testosterone with intramuscular injections of testosterone cypionate were about 700 ng/dL for 100 mg/week, 1100 ng/dL for 250 mg/week, and 2000 ng/dL for 500 mg/week.[75][76] In another study, testosterone levels with 600 mg/week testosterone enanthate by intramuscular injection were 2,800–3,200 ng/dL.[75][77]
Intramuscular injection of testosterone propionate as an oil solution, aqueous suspension, and emulsion has been compared.[78]
Note: All are via i.m. injection. Footnotes:a = TP, TV, and TUe. b = TP and TKL. c = TP, TPP, TiCa, and TD. d = Studied but never marketed. e = Developmental code names. Sources: See template.
The bioavailability of testosterone when administered as a subcutaneous pellet implant is virtually 100%.[86] Levels of testosterone vary considerably between individuals, but are fairly constant within individuals.[41] The absorption half-life of subdermal testosterone implants is 2.5 months.[8] The replacement interval is once every four to six months.[41][87] A single 50 mg testosterone pellet implanted every 4 to 6 months has been found to result in testosterone levels of 70 to 90 ng/dL in women.[41]
Intravenous injection
Testosterone esters like testosterone enanthate are hydrolyzed into testosterone so rapidly in the blood that testosterone and testosterone enanthate have nearly identical pharmacokinetics when administered via intravenous injection.[2]
General
Absorption
The oral bioavailability of testosterone is very low.[8][88] The bioavailability of oral testosterone undecanoate is 3 to 7%.[32][40] Topical testosterone gels have a bioavailability of about 8 to 14% when administered to recommended skin sites including the abdomen, arms, shoulders, and thighs.[48][49] The bioavailability of testosterone by subcutaneous implant is virtually 100%.[86] The bioavailability of drugs that are administered intramuscularly is generally almost 95%.[73]
Distribution
In the circulation, 97.0 to 99.5% of testosterone is bound to plasma proteins, with 0.5 to 3.0% unbound.[1] It is tightly bound to SHBG and weakly to albumin.[1] Of circulating testosterone, 30 to 44% is bound to SHBG while 54 to 68% is bound to albumin.[1] Testosterone that is unbound is referred to as free testosterone and testosterone that is bound to albumin is referred to as bioavailable testosterone.[1] Unlike testosterone that is bound to SHBG, bioavailable testosterone is bound to plasma proteins weakly enough such that, similarly to free testosterone, it may be biologically active, at least to a certain extent.[1] When referenced collectively (i.e., free, bioavailable, and SHBG-bound), circulating testosterone is referred to as total testosterone.[1]
^ abSteinberger E, Ayala C, Hsi B, Smith KD, Rodriguez-Rigau LJ, Weidman ER, Reimondo GG (1998). "Utilization of commercial laboratory results in management of hyperandrogenism in women". Endocrine Practice. 4 (1): 1–10. doi:10.4158/EP.4.1.1. PMID15251757.
^Balen AH, Conway GS, Kaltsas G, Techatrasak K, Manning PJ, West C, Jacobs HS (August 1995). "Polycystic ovary syndrome: the spectrum of the disorder in 1741 patients". Human Reproduction. 10 (8): 2107–2111. doi:10.1093/oxfordjournals.humrep.a136243. PMID8567849.
^Styne DM (6 December 2019). "Physiology and Disorders of Puberty". In Melmed S, Koenig RJ, Rosen CJ, Auchus R, Goldfine AB, Williams RH (eds.). Williams Textbook of Endocrinology (14 ed.). Philadelphia, PA: Elsevier. pp. 1023–1164. ISBN9780323555968.
^Nieschlag E (September 2006). "Testosterone treatment comes of age: new options for hypogonadal men". Clin. Endocrinol. (Oxf). 65 (3): 275–81. doi:10.1111/j.1365-2265.2006.02618.x. PMID16918944.
^Nieschlag E (January 2015). "Current topics in testosterone replacement of hypogonadal men". Best Pract. Res. Clin. Endocrinol. Metab. 29 (1): 77–90. doi:10.1016/j.beem.2014.09.008. PMID25617174.
^Byrne M, Nieschlag E (May 2003). "Testosterone replacement therapy in male hypogonadism". J. Endocrinol. Invest. 26 (5): 481–9. doi:10.1007/bf03345206. PMID12906378.
^ abLauritzen C (1988). "Natürliche und Synthetische Sexualhormone – Biologische Grundlagen und Behandlungsprinzipien" [Natural and Synthetic Sexual Hormones – Biological Basis and Medical Treatment Principles]. In Schneider HP, Lauritzen C, Nieschlag E (eds.). Grundlagen und Klinik der Menschlichen Fortpflanzung [Foundations and Clinic of Human Reproduction] (in German). Walter de Gruyter. pp. 229–306. ISBN978-3110109689. OCLC35483492.
^ abTäuber U, Schröder K, Düsterberg B, Matthes H (1986). "Absolute bioavailability of testosterone after oral administration of testosterone-undecanoate and testosterone". European Journal of Drug Metabolism and Pharmacokinetics. 11 (2): 145–149. doi:10.1007/BF03189840. PMID3770015. S2CID32305408.
^Corona G, Rastrelli G, Vignozzi L, Maggi M (June 2012). "Emerging medication for the treatment of male hypogonadism". Expert Opinion on Emerging Drugs. 17 (2): 239–259. doi:10.1517/14728214.2012.683411. PMID22612692. S2CID22068249.
^Behre HM, Abshagen K, Oettel M, Hübler D, Nieschlag E (May 1999). "Intramuscular injection of testosterone undecanoate for the treatment of male hypogonadism: phase I studies". European Journal of Endocrinology. 140 (5): 414–419. CiteSeerX10.1.1.503.1752. doi:10.1530/eje.0.1400414. PMID10229906. S2CID22597244.
^Kühnert B, Byrne M, Simoni M, Köpcke W, Gerss J, Lemmnitz G, Nieschlag E (August 2005). "Testosterone substitution with a new transdermal, hydroalcoholic gel applied to scrotal or non-scrotal skin: a multicentre trial". European Journal of Endocrinology. 153 (2): 317–326. doi:10.1530/eje.1.01964. PMID16061839.
^Amano T, Iwamoto T, Sato Y, Imao T, Earle C (September 2018). "The efficacy and safety of short-acting testosterone ointment (Glowmin) for late-onset hypogonadism in accordance with testosterone circadian rhythm". The Aging Male. 21 (3): 170–175. doi:10.1080/13685538.2018.1471129. PMID29734846. S2CID13701612.
^Needham S, Needham S (2018). "Case Study: Absorption of Testosterone Cream via Scrotal Delivery". International Journal of Pharmaceutical Compounding. 22 (6): 466–468. PMID30384346.
^Nieschlag E (January 2015). "Current topics in testosterone replacement of hypogonadal men". Best Practice & Research. Clinical Endocrinology & Metabolism. 29 (1): 77–90. doi:10.1016/j.beem.2014.09.008. PMID25617174.
^Davis SR, Nieschlag E, Behre HM, Nieschlag S (26 July 2012). "Testosterone use in women". In Nieschlag E, Behre HM, Nieschlag S (eds.). Testosterone: Action, Deficiency, Substitution. Cambridge University Press. pp. 494–516. doi:10.1017/CBO9781139003353.024. ISBN978-1-107-01290-5.
^Culligan PJ, Goldberg RP (6 March 2007). Urogynecology in Primary Care. Springer Science & Business Media. pp. 116–. ISBN978-1-84628-167-9. Topical vaginal testosterone is often used in premenopausal women as a first step in the treatment of sexual dysfunction and vaginal lichen planus. Topical testosteorne preparations can be compounded in 1% to 2% formulations and should be applied up to 3 times per week.
^Papadakis MA, McPhee SJ, Rabow MW (11 September 2017). Current Medical Diagnosis and Treatment 2018, 57th Edition. McGraw-Hill Education. pp. 1217–1218. ISBN978-1-259-86149-9. Testosterone can also be compounded as a cream containing 1 mg/mL, with 1 mL applied to the abdomen daily. Vaginal testosterone is an option for postmenopausal women who cannot use systemic or vaginal estrogen due to breast cancer. Testosterone 150–300 mcg/day vaginally appears to reduce vaginal dryness and dyspareunia without increasing systemic estrogen levels.
^Pizzorno JE (2013). Textbook of Natural Medicine. Elsevier Health Sciences. pp. 1602–. ISBN978-1-4377-2333-5. At present, bioidentical testosterone can be obtained only from a compounding pharmacy, where 4 to 6 mg of bioidentical testosterone is generally formulated alone or together with the biestrogen or triestrogen formulation. Testosterone cream applied to the genital region can be used as an alternative delivery method. Common prescriptions are anywhere from 1 to 10 mg/g of cream.
^Hamburger C (August 1958). "Testosterone treatment and 17-ketosteroid excretion. V. Administration of testosterone per rectum". Acta Endocrinologica. 28 (4): 529–536. doi:10.1530/acta.0.0280529. PMID13570882.
^ abAakvaag A, Vogt JH (March 1969). "Plasma testosterone values in different forms of testosterone treatment". Acta Endocrinologica. 60 (3): 537–542. doi:10.1530/acta.0.0600537. PMID5395873.
^Nieschlag E, Cüppers HJ, Wiegelmann W, Wickings EJ (1976). "Bioavailability and LH-suppressing effect of different testosterone preparations in normal and hypogonadal men". Hormone Research. 7 (3): 138–145. doi:10.1159/000178721. PMID1002121.
^Lentini S, Fortunio G (1952). "[Absorption and action of testosterone administered rectally]" [Absorption and action of testosterone administered rectally]. Clinica Nuova; Rassegna del Progresso Medico Internazionale (in Italian). 14 (1–2): 5–16. PMID14945075.
^Hamburger C (February 1974). "[Letter: Testosterone suppositories DAK]" [Letter: Testosterone suppositories DAK]. Ugeskrift for Laeger (in Danish). 136 (6): 307–308. PMID4820554.
^ abcMorgentaler A, Traish AM (February 2009). "Shifting the paradigm of testosterone and prostate cancer: the saturation model and the limits of androgen-dependent growth". European Urology. 55 (2): 310–320. doi:10.1016/j.eururo.2008.09.024. PMID18838208.
^Cooper CS, Perry PJ, Sparks AE, MacIndoe JH, Yates WR, Williams RD (February 1998). "Effect of exogenous testosterone on prostate volume, serum and semen prostate specific antigen levels in healthy young men". The Journal of Urology. 159 (2): 441–443. doi:10.1016/s0022-5347(01)63944-2. PMID9649259.
^Hamburger C (1952). "17-Ketosteroid Excretion and Modes of Administering Testosterone Preparations". Ciba Foundation Symposium - Steroid Hormone Administration (Book II of Colloquia on Endocrinology, Vol. 3). Novartis Foundation Symposia. John Wiley & Sons. pp. 304–322. doi:10.1002/9780470715154.ch7. ISBN9780470715154. ISSN1935-4657.
^Olson J, Schrager SM, Clark LF, Dunlap SL, Belzer M (September 2014). "Subcutaneous Testosterone: An Effective Delivery Mechanism for Masculinizing Young Transgender Men". LGBT Health. 1 (3): 165–167. doi:10.1089/lgbt.2014.0018. PMID26789709.
^Wilson DM, Kiang TK, Ensom MH (March 2018). "Pharmacokinetics, safety, and patient acceptability of subcutaneous versus intramuscular testosterone injection for gender-affirming therapy: A pilot study". American Journal of Health-System Pharmacy. 75 (6): 351–358. doi:10.2146/ajhp170160. PMID29367424. S2CID3886536.
Behre HM, Nieschlag E, Nieschlag E, Behre HM, Nieschlag S (26 July 2012). "Testosterone preparations for clinical use in males". In Nieschlag E, Behre HM, Nieschlag S (eds.). Testosterone: Action, Deficiency, Substitution. Cambridge University Press. pp. 309–335. doi:10.1017/CBO9781139003353.016. ISBN978-1-107-01290-5.
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Yaeko Nogami Yaeko Nogami (野上 弥生子?, Nogami Yaeko; Usuki, 6 maggio 1885 – 30 marzo 1985) è stata una scrittrice giapponese. Indice 1 Biografia 2 Opere (parziale) 3 Adattamenti cinematografici 4 Premi e riconoscimenti 4.1 Vincitrice 5 Note 6 Bibliografia 7 Altri progetti 8 Collegamenti esterni Biografia Figlia maggiore di Masa e Kakusaburo, proprietari di un famoso negozio di sakè, è nata Yae Kotegawa il 6 maggio 1885 a Usuki, prefettura di Ōita[1]. Ha compiuto gli studi...
Lihat Bahasa Bugis di: ISO • Ethnologue • Wikipedia bahasa Inggris Bahasa Bugis Basa Ugi ᨅᨔ ᨕᨘᨁᨗ بهاس بوڬيس Dituturkan diIndonesiaWilayahSulawesi SelatanEtnisBugisPenutur4 juta (termasuk 500.000 penutur B2) (2015 UNSD) Rumpun bahasaAustronesia Melayu-PolinesiaSulawesi SelatanBugisBahasa Bugis Sistem penulisanLontara, Alfabet Latin dan Jawi-SerangKode bahasaISO 639-2bugISO 639-3bugGlottologbugi1244[1]IETFbug Status pemertahana...
American TV series or program Real Chance of LoveCreated byCris AbregoMark CroninStarringKamal GivensAhmad GivensOpening themeDoes She Love Me?ComposerThe StallionairesCountry of originUnited StatesNo. of seasons2No. of episodes26ProductionExecutive producersCris AbregoMark CroninBen SamekRunning time45–48 minutesProduction company51 Minds EntertainmentOriginal releaseNetworkVH1ReleaseOctober 20, 2008 (2008-10-20) –October 26, 2009 (2009-10-26) Real Chance of Love is an Am...