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1. By Dr. Sahar Al-Suwailem
Consultant OB-Gyn, KFMC – WSH
Gyn-Lapascopy
3. Abnormal Uterine Bleeding Heavy regular menstrual bleeding (Menorrhagia)
Irregular menstrual bleeding
Irregular bleeding
Inter menstrual bleeding
Post coital bleeding
Oligomenorrhoea and Amenorrhoea
DUB – heavy prolonged flow with or without breakthrough bleeding it may occur with or without ovulation
4. Despite improved education and the media, most women don’t know how much they should lose, and 1 in 3 think they are heavier than normal
30ml (6 teaspoons) - (range 20-60ml)
Last 5 days (range 3-8 days)
90% of bleeding in first 3 days What is normal ?
5. Greater than 80mls
Teens and perimenopause
Commonest in 40–44 years olds (20%)
Any bleeding which affects the physical, psychological or social welfare of the patient What is a Heavy Period?
6. Abnormal Uterine Bleeding - WHY? Exact pathophysiology still not known
Basis of excessive bleeding?
Endocrine abnormality: estrogen - progesterone imbalance (usually estrogen dominance)
Deficiency in clotting mechanism
Altered prostaglandin synthesis in favor of E2 than F2?.
8. Cycle
Regular vs. irregular
i.e. ovulatory vs. anovulatory
Heaviness
Flooding
Pain
Timing and severity
PMT “suggestive of ovulatory cycle” History tells all – back to basics
9. These symptoms may indicate different pathologies and management pathways:
Intermenstrual bleeding
Post coital bleeding
Pelvic pain
Pressure symptoms
Offensive discharge
Dyspareunia
E.g. polyps or submucous fibroids are present in 25 to 50% of women with irregular bleeding Why consider HMB separately from IMB or PCB?
10. Differential Diagnosis of Noncyclic Uterine Bleeding Anovulation
Uterine leiomyoma
Endometrial polyp
Endometrail hyperplasia or carcinoma
Cervical or vaginal neoplasia
Endometritis
Adenomyosis
Bleeding associated with pregnancy
Bleeding associated with pueperium
Coagulopathies (von Willebrand’s disease, platelet abnomalities thromboytopenic purpura)
Iatorgenic causes and medications
Systemic diseases (Thyroid, Hyperprolactinemia)
11. Abdominal and pelvic examination with visualization of the cervix, a smear or swabs if appropriate and a bimanual assessment
BMI
Sign of excess androgen
CBS ± ferritin ± coagulation if appropriate
TV ultrasound
Endometrial thickness
Enlarged uterus ? cause Diagnosis
12. Endometrial sampling
All women over 40 years of age
Women with high risk of endometrial cancer: nulliparity with history of infertility, obesity = 90 kg, PCO, family history of endometrial and colonic cancer, and on tamoxifen therapy
Women who has no improvement in her bleeding pattern following a course of therapy of three months Diagnosis – cont.
13. Saline sonohysterography
R/o intrauterine masses during TVS
Curettage
10 to 25% D&C alone does not uncover endometrial pathology
Risk of anesthesia
Risk of perforation
Hysteroscopy directed biopsy
Endometrial culture Diagnosis – cont.
14. Your history and examination will reveal 3 categories of patients
For patients with normal bleeding who are happy you can reassure, or address their other concerns
If you suspect a problem refer to AUB clinics
If straightforward HMB discuss the options The Discussion
15. A U B - Management Options
16. Medical Treatment for AUB Hormonal
Es+Pr (COCP)
Progestogens
Norethisterone?
MPA
LNG IUS
Danazol
GnRHa
Estrogen
Androgens + Estrogen Non-Hormonal
ANTIFIBRINOLYTICS
TRANEXAMIC ACID (TA)
NSAIDs
Mefenamic acid (MA)
Naproxen,Ibuprofen, Aspirin
17. Antifibrinolytics
Tranexamic acid
Anti-prostaglandins – NSAID
Mefenamic acid
Ibuprofen Medical treatments: Non Hormonal
18. When period are regular / ovulatory
When women trying to conceive
When women request medication that is non-hormonal
When awaiting investigation or other definitive treatment When to use non-hormonal medication
19. Antifibrinolytics
Competitive inhibitor of plasminogen activator
Reduce MBL 34-59% (based an 10 randomized placebo-controlled trails)
Low risk of side-effects - gastrointestinal
No effects of coagulation within healthy vessels
Non Hormonal
Short half life - take regularly
1 gm every 6 hours Tranexamic acid (cyclokapron)
20. Is not contraceptive
Does not reduce dysemenorrhoea
Does not regulate the cycle
Only recommended for 4 days Tranexamic acid – “drawbacks”
21. PG synthesis inhibitors
(via inhibition of cyclo-oxygenase)
Reduce MBL 16-49%
Reduce dysmenorrhoea (70%)
Few side-effects ? Asthma
Can be used with other medications
Mefenamic acid, Ibuprofen (NSAID)
22. Need to be told to take them regularly
Many think they are painkillers
Side-effects
Asthmatics
Not contraceptive
Do not regulate the cycle
No evidence regarding effectiveness in the presence of fibroids NSAIDs - “drawbacks”
23. HMB may present in absence of organic pathology
Disruption of the hypothalamo–pituitary–ovarian endometrial axis leads to failure of ovulation and progesterone induced secretory change
Bleeding results from endometrial instability and is less defined, heavier and often less regular than that to progesterone withdrawal
Pattern seen particularly at menarche and perimenopause Medical treatment – Hormonal
24. Mode of action:
High local progestogen concentration
Induces endometrial atrophy
Low systemic absorption with small effect on ovulation
Licensed use: 5 years
High Contraceptive efficacy Levonogestrel IUS
25. RCTs: MBL reduction 71-96%
Benefit may take 6/12
Low incidence of side effects
Majority satisfied (OR 0.61) and will continue (OR 0.73) Levonogestrel IUS – cont.
26. Synthetic oestrogen and progestogen combinations
Act on HPO axis to suppress ovulation but balanced effect on endometrium – bleed on withdrawal
One RCT (n=45) using 30 mcgEE showed MBL reduction of 43%
Non-contraceptive benefits e.g.
Good cycle control
Reduction in breast pain, dysmenorrhoea Combined Oral Contraceptives (COC)
27. The likely mechanism of action is that is induces endometrial atrophy
Luteal phase norethisterone (day 19-26) does not affect MBL
RCT of 15mg NET from day 5-26 shows:
MBL reduction 83% (LNG IUS=94%)
Satisfaction 22% (LNG IUS=66%)
RCT shows cyclic progestins to be ineffective in controlling regular heavy bleeding compared to NSAID and tranexamic acid (IA) Oral Progestogens
28. Neither product is licensed for HMB Injected /depot progestogens
29. Mimics action of natural GnRH but with much longer half-life
Initial stimulation then block FSH &LH production
Profound hypogonadism results
Used clinically for
Perimenopusal women
Oestrogen dependent lesions (e.g. fibroids)
Data drawn from fibroid studies Gonadotrphin Releasing Hormone analogue (GnRH–a)
30. Reduction in MBL with 89% amenorrhoea
Use alone is associated with significant side effects due to hormone deficiency
Add-back therapy reduces adverse effects and benefit is not lost Gonadotrphin Releasing Hormone analogue (GnRH–a)
31. Danazol Danazol inhibits secretion of pituitary gonadotrophins and also has androgenic, anti-oestrogenic, and anti-progestogenic activity
It reduces excessive menstrual bleeding by up to 80% [NZ, 1998; RCOG, 1999]
It is poorly tolerated, due to androgenic side effects of weight gain, hirsutism, acne, mood changes, and occasionally deepening of the voice, which may be irreversible
It should generally only be used selectively, following specialist advice [NZ, 1998; RCOG, 1998]
32. Investigate to exclude pathology
Hormonal manipulation essential to regulate the cycle
Luteal phase progestogen may be useful (5 mg bd from day 19-26 )
Otherwise COC or Mirena
Compliance limited by side effects and back of efficacy in regard to decrease in MBL Irregular Bleeding
33. Review in 3 months
? Continue treatment
? Change treatment / add second therapy
? Refer The review
34. Treatment for Menorrhagia (AUB) Current Recommendation
35. Treatment for Menorrhagia (AUB) Current Recommendation – cont.
