Progestins and antiprogestins

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Progestins and antiprogestins

HDF3 Repro/Neuro

HDF3 Repro/Neuro

Anatomy of the pelvic girdle
Anatomy of the pelvic cavity
Anatomy of the breast
Arteries and veins of the pelvis
Nerves and lymphatics of the pelvis
Anatomy of the female urogenital triangle
Anatomy of the perineum
Anatomy of the female reproductive organs of the pelvis
Anatomy clinical correlates: Breast
Anatomy clinical correlates: Female pelvis and perineum
Development of the reproductive system
Mammary gland histology
Ovary histology
Fallopian tube and uterus histology
Cervix and vagina histology
Anatomy and physiology of the male reproductive system
Puberty and Tanner staging
Testosterone
Anatomy and physiology of the female reproductive system
Estrogen and progesterone
Menstrual cycle
Menopause
Pregnancy
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Stages of labor
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Precocious puberty
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Klinefelter syndrome
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Krukenberg tumor
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Female sexual interest and arousal disorder
Orgasmic dysfunction
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Intraductal papilloma
Phyllodes tumor
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Hyperemesis gravidarum
Gestational hypertension
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Gestational diabetes
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Placenta previa
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Oligohydramnios
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Potter sequence
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Chorioamnionitis
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Congenital rubella syndrome
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Miscarriage
Gestational trophoblastic disease
Ectopic pregnancy
Fetal hydantoin syndrome
Fetal alcohol syndrome
Disorders of sex chromosomes: Pathology review
Prostate disorders and cancer: Pathology review
Testicular tumors: Pathology review
Uterine disorders: Pathology review
Ovarian cysts and tumors: Pathology review
Cervical cancer: Pathology review
Vaginal and vulvar disorders: Pathology review
Benign breast conditions: Pathology review
Breast cancer: Pathology review
Complications during pregnancy: Pathology review
Congenital TORCH infections: Pathology review
Disorders of sexual development and sex hormones: Pathology review
Amenorrhea: Pathology review
Testicular and scrotal conditions: Pathology review
Sexually transmitted infections: Warts and ulcers: Pathology review
Sexually transmitted infections: Vaginitis and cervicitis: Pathology review
HIV and AIDS: Pathology review
Androgens and antiandrogens
PDE5 inhibitors
Adrenergic antagonists: Alpha blockers
Estrogens and antiestrogens
Progestins and antiprogestins
Aromatase inhibitors
Uterine stimulants and relaxants
Anatomy clinical correlates: Male pelvis and perineum
Bones of the cranium
Anatomy of the cranial base
Anatomy of the cerebral cortex
Anatomy of the cerebellum
Anatomy of the cranial meninges and dural venous sinuses
Anatomy of the brainstem
Anatomy of the basal ganglia
Anatomy of the white matter tracts
Anatomy of the limbic system
Anatomy of the blood supply to the brain
Anatomy of the diencephalon
Anatomy of the ventricular system
Anatomy clinical correlates: Cerebral hemispheres
Anatomy of the vertebral canal
Anatomy of the descending spinal cord pathways
Anatomy of the ascending spinal cord pathways
Anatomy clinical correlates: Vertebral canal
Anatomy clinical correlates: Spinal cord pathways
Memory
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Congenital neurological disorders: Pathology review
Traumatic brain injury: Pathology review
Dementia: Pathology review
Movement disorders: Pathology review
Demyelinating disorders: Pathology review
Pediatric brain tumors: Pathology review
Adult brain tumors: Pathology review
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Anti-parkinson medications
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Questions

USMLE® Step 2 style questions USMLE

0 of 6 complete

A 30-year-old woman comes to the office after a positive home pregnancy test, which she took after missing her period. The patient has not had any recent vaginal bleeding or abdominal cramping. Menarche was at age 12 years, and she reports having a regular 28-day menstrual cycle. Past medical history is unremarkable, and the patient does not take any medications. Family history is noncontributory. Vitals are within normal limits. Physical examination shows a small, mobile, nontender uterus. A transvaginal ultrasound confirms a 7-week fetus. The patient describes her wish to terminate the pregnancy and opts for medical abortion. Which of the following is the most appropriate abortive agent for this patient?  

Transcript

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Progestins are a group of synthetic progestogens that have similar effects to those of natural progesterone.

They can be divided into two categories: the progesterone derivatives and the testosterone derivatives.

They are mainly used as contraceptives, in hormone replacement therapy, or HRT, and in the treatment of various gynecologic conditions.

Now, antiprogestins act as progesterone antagonists and include mifepristone and ulipristal.

Mifepristone is used for medical abortion while ulipristal is used as an emergency contraceptive.

The hypothalamus secretes gonadotropin-releasing hormone, or GnRH, which travels to the nearby pituitary gland and stimulates it to secrete two hormones, follicle stimulating hormone, or FSH, and luteinizing hormone, or LH.

During the two weeks following ovulation, which is referred to as the ovarian luteal phase, the remnant of the ovarian follicle becomes the corpus luteum, which is made up of luteinized theca and granulosa cells, meaning that these cells have been exposed to the high luteinizing hormone levels that occur just before ovulation.

The luteinized cells secrete more progesterone than estrogen and progesterone becomes the dominant hormone.

Under the influence of progesterone, the uterus enters into the secretory phase of the endometrial cycle.

During this time, spiral arteries continue to grow, and the endometrial glands continue to produce more secretions that make the endometrium more receptive to the implantation of a fertilized gamete.

After day 15 of the cycle, the optimal window for fertilization begins to close and the corpus luteum gradually degenerates into the nonfunctional corpus albicans.

The corpus albicans doesn’t make hormones, so estrogen and progesterone levels slowly decrease.

When progesterone reaches its lowest level, the spiral arteries collapse and the functional layer of the endometrium prepares to shed during menstruation.

This shedding marks the beginning of a new menstrual cycle and another opportunity for fertilization.

Alright, apart from the female sex organs, progesterone also plays a role in bone strength, as well as keeping the skin elastic.

Also, during pregnancy, the placenta takes over progesterone secretion, which is required to maintain the pregnancy and also helps prepare the breasts for lactation after delivery.

But after menopause, the ovaries run out of functional ovarian follicles. So there’s no theca or granulosa cells to produce any more hormones, which accounts for many of the symptoms preceding menopause, like hot flashes, night sweats, vaginal atrophy, and osteoporosis.

Okay, now progestogens in general are a class of steroid hormones that bind to and activate the progesterone receptor.

Once they’re inside the cells, they bind to progesterone receptors found in the cytoplasm, and together they form a complex that can travel into the nucleus and bind to progesterone-related genes, modifying the gene expression.

Synthetic progestogens, which are also called progestins are divided into two groups: the progesterone derivatives and the testosterone derivatives.

The progesterone derivatives include medroxyprogesterone, hydroxyprogesterone, and megestrol acetate.

Now, the testosterone derivatives are basically derivatives of 19-nortestosterone and differ primarily in the degree of androgenic effects.

The older testosterone derivatives like danazol norgestrel, levonorgestrel, and ethynodiol are more androgenic than the newer testosterone derivatives such as desogestrel, norgestimate, and etonogestrel.

Progestins in general decrease growth and increase vascularization of the endometrium, and also thickens the cervical mucus.

While they are able to stabilize the endometrium, they can’t support pregnancy effectively like endogenous progesterone does.

Okay, let’s move on to indications that are common for all progestins.

They can be used as contraceptives, or birth control, either alone or in combination with an estrogen.

They can be administered orally, intramuscularly, through an intrauterine device, or a transdermal implant.

They can also be used in combination with estrogen in hormone replacement therapy after menopause, in women with an intact uterus to prevent endometrial hyperplasia or endometrial cancer.

Even though transitioning into menopause is a natural step in the aging of the female reproductive system, the postmenopausal symptoms may have a negative impact on overall well-being. So in some cases, hormone replacement therapy with estrogens are used to relieve symptoms.

But all women with an intact uterus need progesterone in addition to estrogen in order to counteract the proliferative effects of estrogen to the endometrium, and prevent endometrial hyperplasia and endometrial cancer.

However, women who have undergone hysterectomy should not receive a progestin, because its key benefit is prevention of endometrial hyperplasia and carcinoma, and that’s no longer relevant.

Progestins can also be used in the diagnosis and treatment of various gynecological conditions such as: secondary amenorrhea, which is when a female who previously had menstrual periods suddenly stopped having them for at least 3 months; dysfunctional or abnormal uterine bleeding, which is when vaginal bleeding occurs outside of the regular menstrual cycle; and endometriosis, which is when cells of the endometrium grow outside the uterus.

In amenorrhea for example, individuals might have intrauterine adhesions, or Asherman syndrome.

This is when there is scar tissue inside the uterine cavity, typically in a female who has undergone uterine instrumentation in the past, like dilation and curettage.

Key Takeaways

Progestins are synthetic that mimic the effects of progesterone, a hormone that plays a role in the menstrual cycle and pregnancy. Common uses of progestins include hormonal contraception (either alone or with estrogen), and prevention of endometrial hyperplasia from unopposed estrogen in hormone replacement therapy. Progestins are also used to treat secondary amenorrhea, dysfunctional uterine bleeding, endometriosis, and breast cancer. On the other hand, antiprogestins are drugs that block the effects of progesterone. Antiprogestins are used in pregnancy termination and emergency contraception.

Sources

  1. "Katzung & Trevor's Pharmacology Examination and Board Review,12th Edition" McGraw-Hill Education / Medical (2018)
  2. "Rang and Dale's Pharmacology" Elsevier (2019)
  3. "Goodman and Gilman's The Pharmacological Basis of Therapeutics, 13th Edition" McGraw-Hill Education / Medical (2017)
  4. "Mechanism of Telapristone Acetate (CDB4124) on Progesterone Receptor Action in Breast Cancer Cells" Endocrinology (2018)
  5. "Antiprogestins in gynecological diseases" REPRODUCTION (2015)
  6. "An efficient model of human endometriosis by induced unopposed estrogenicity in baboons" Oncotarget (2016)