PROGESTIN
A 'progestin' is a synthetic progestogen that has some biological activity similar to progesterone and is most well known for the applications in hormonal contraception, but progestins (and progesterone) also have applications in the treatment of dysmenorrhea, endometriosis, functional uterine bleeding, and amenorrhea. They have also been used to treat habitual miscarriages due to progesterone's role in sustaining pregnancy, but this has not always been successful due to the fact that miscarriage is not always due to hormonal deficiency.
| Contents |
| History |
| Examples |
| Methods of progestin-based contraception |
| Adverse effects |
| See Also |
| References |
History
The recognition of progesterone's ability to suppress ovulation during pregnancy spawned a search for a similar hormone that could bypass the problems associated with administering progesterone (low bioavailability when administered orally and local irritation and pain when continually administered parentally) and, at the same time, serve the purpose of controlling ovulation. The many synthetic hormones that resulted are known as progestins.
The first orally active progestin, norethindrone (norethisterone), was synthesized in 1951 by the Mexican chemist Luis E. Miramontes at Syntex under the supervision of Carl Djerassi and George Rosenkranz, and was used in some of the first oral contraceptives in the early 1960s. Norethynodrel, an isomer of norethindrone, first synthesized in 1952 by Frank Colton at Searle, was the progestin used in Enovid, the first approved oral contraceptive in 1960.
Examples
Some examples of progestins that have been used in hormonal contraceptives are norethynodrel (Enovid), norethindrone (many brand names, most notably Ortho-Novum and Ovcon) norgestimate (Ortho Tricyclen, Ortho-Cyclen), norgestrel, levonorgestrel (Alesse, Trivora-28), medroxyprogesterone (Provera, Depo-Provera) and desogestrel.
Methods of progestin-based contraception
It has been found that the most effective method of contraception was with a combination of estrogen and progestin. This can be done in a monophasic, biphasic, or in a triphasic manner. In the monophasic method, both an estrogen and a progestin are administered for 20 or 21 days and stopped for a 7 or 8 day period that includes the 5 day menstrual period. Sometimes, a 28 day regimen is used that includes 6 or 7 inert tablets. Newer biphasic and triphasic methods are now used to more closely simulate the normal menstrual cycle. Yet another method is to administer a small dose of progestin only (no estrogen) in order to decrease certain risks associated with administering estrogen, but a major side effect is irregular bleeding that is usually observed during the first 18 months of such therapy.
Different progestins have different combinations of androgen (testosterone-like) activity and progesterone activity. If the activity of 1 mg of norethindrone is taken as the baseline, 1 mg of the other progestins have activities as follows:
| Progestin | Progestational activity | Androgen activity |
| norethindrone | 1 | 1 |
| norethindrone acetate | 1.2 | 1.6 |
| desogestrel | 9 | 3.4 |
| drospirenone | 1.5 | 0 |
| ethynodiol diacetate | 1.4 | 0.6 |
| norelgestromin | 1.3 | 1.9 |
| norgestimate | 1.3 | 1.9 |
| levonorgestrel | 5.3 | 8.3 |
| dl-norgestrel | 2.6 | 4.2 |
Adverse effects
If progestins are taken during a pregnancy, there is a risk of progestin-induced virilisation. In this case, the hormone crosses the placenta, and is converted to an androgen (virilizing hormone) by the prenatal XX persons metabolism. Such androgens perform virilizing effects on the unborn child. Healthyplace.com - What is Progestin Induced Virilisation?
See Also
List of steroid abbreviations
References
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