This document discusses abnormal uterine bleeding (AUB). It defines AUB and normal menstruation. It describes various clinical types of AUB and potential causes. Evaluation involves history, examination, and investigations. Treatment options include medical approaches like hormonal therapies and surgical procedures like endometrial ablation. Dysfunctional uterine bleeding is discussed in depth as the most common cause of AUB.
2. DEFINE
Any deviation in normal frequency, duration or amount of
menstruation in women of reproductive age.
NORMAL MENSES
Frequency: 21-35 d
Duration: 3-7 d
Volume: 30-80 ml
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3. CLINICAL TYPES
Polymenorrhoea: frequent (<21 d) menstruation, at
regular intervals
Menorrhagia: Excessive (>80 ml) & / or prolonged
menstruation, at regular intervals
Metrorrhagia: Excessive (>80 ml) & / or prolonged
menstruation at irregular intervals.
Menometrorrhagia: both.
Intermenstual bleeding: episodes of uterine
bleeding between regular menstruations
Hypomenorrhoea: scanty menstruation.
Oligomenorrhea: infrequent menstruation (>35 d)
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7. Pathology
Endocrine abnormality Endometrium
Anovulatory
90% Insufficient follicles Inadequate proliferative or atrophic
Persistent follicles Proliferative or hyperplastic
Ovulatory
10% Short proliferative phase Normal
Long proliferative phase Normal
Insufficient C. luteum Irregular or deficient secretory
leading to short luteal phase
Persistent C luteum leading to Irregular shedding
long luteal phase
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9. Risk of endometrial cancer
Chronic anovulation has 3 times increased risk
(Coulam,1989).
Chronic proliferation of the endometrium leading to
adenomatous hyperplasia, leading to atypical
adenomatous hyperplasia, leading to endometrial
carcinoma. Transition can take up to 10 yrs or more.
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10. Diagnosis
Aim:
1. Nature & severity of bleeding
2. Exclusion of organic causes
3. Ovulatory or anovulatory
How:
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11. I. History:
1. Personal: age, wishes of the patient
2. Menstrual
3. Obstetric
4. Past
5. Present: amount, duration, color, smell, relation to
sexual intercourse, associated symptoms
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12. II. Examination:
1. General:
pallor, endocrinopathy, coagulopathy, pregnancy
2. Abdominal:
liver, spleen, pelvi abdominal mass
3. Pelvic:
origin of the bleeding, cause
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13. III.Investigations
Systemic:
1. CBC (for all, Grade A)
2. BHCG
3. Prolactin & TSH
4. Prothrombin time, partial thrmoplastin time,
bleeding time, platelets, Von Willebrand factor
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14. Local:
1. Pap smear
2. Endometrial biopsy
3. D & C
4. Hysteroscopy
5. U/S
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16. Assessment of the amount of the bleeding:
50% of excessive menstruation have normal amount of
blood loss by objective methods
1.Subjective methods:
history of passage of clots, flooding, use of large
number of pads, do not reflect the actual blood loss
2.Semiobjective:
i.Iron deficiency anemia
ii.Menstrual calendar
(August,1996)
III. Pictorial blood loss chart
(Higham,1990)
:
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17. Menstrual calender (August,1996)
Saturday 7 14 21 28
Sunday 1 8 15 22 29
Monday 2 9 16 23 30
Tuesday 3 10 17 24 31
Wednesday 4 11 18 25
Thursday 5 12 19 26
Friday 6 13 20 27
. Spotting
- Slight loss
O Moderate loss
Very heavy loss
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18. Pictorial blood loss chart: (Higham,1990)
Days of the bleeding Score
1 2 3 4 5 6 7 8
Towel
1 ponit
5 ponits
10 points
Clots 1p clot 1 point
5p clot 5 points
Flooding 5 points
Score >100 = MenorrrhagiaABOUBAKR ELNASHAR
19. Endometrial biopsy:
Indications:
.Between 20 & 40
.If endometrial thickness on TVS is >12mm, endometrial
sample should be taken to exclude endometrial
hyperplasia (Grade A).
Failure to obtain sufficient sample for H/P does not
require further investigation unless the endometrial
thickness is >12 mm (Grade B)
Aim:
diagnosis of the type of the bleeding
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20. Methods:
As an outpatient procedure, without general anesthesia.
1.Pipelle curette
2.Sharman curette, Gravlee jet washer, Isac cell
sampler
3.Accrette
4.vabra aspirator
Advantages:
An adequate & acceptable screening procedure in
females under 40 yrs
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22. D & C:
Indications:
1. Mandatory after 4o yrs
2. Persistent or recurrent bleeding between 20 & 40 yrs
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23. Aim:
1.Diagnosis of organic disease e.g. endometritis, polyp,
carcinoma, TB, fibroid
2.Diagnosis of the type of the endometrium:
hyperplastic, proliferative, secretory, irregular ripening,
shedding, atrophic. This provides a guide to etiology &
treatment
3.Arrest of the bleeding, if the bleeding is severe or
persistent, particularly hyperplastic endometrium.
Curettage is essentially a diagnostic & not a therapeutic
procedure.
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26. Hysteroscopy:
Indications:
Mandatory after 40 yrs
1. Erratic menstrual bleeding
2. Failed medical treatment
3. TVS suggestive of intrauterine pathology e.g. polyp,
fibroid (Grade B)
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27. Aim:
1.Excellent view of the uterine cavity & diagnosis of
polyps, submucous fibroid, hyperplasia.
2.Biopsy of the suspected areas
3.Treatment
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28. Advantages over D &C
1.The whole uterine cavity can be visualized
2.Very small lesions such as polyps can be
identified & biopsed or removed
3.Bleeding from ruptured venules & echymoses can
be readily identified
4.The sensitivity in detecting intrauterine pathology
is 98%
(Loffer,1989)
5.Outpatient procedure
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30. Ultrasonography:
1. TAS:
can exclude pelvic masses, pregnancy complications
2. TVS:
More informative than TAS. Measurement of the
endometrial thickness is not a replacement for
biopsy. All endometrial carcinoma in postmenopausal
with endometrial thickness>4 mm
(Osmers,1990)
3. Saline sonography:
an alternative to office hysteroscopy in selected
cases. It is better tolerated than office hysteroscopy
or HSG
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31. TVS is recommended in:
1. Weight >90 Kg
2. Age > 40 yrs
3. Other risk factors for endometrial hyperplasia or
carcinoma e.g.
infertility,
Nulliparity
family history of colon or endometrial cancer,
exposure to unopposed estrogen (Grade B)
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35. Strategy of treatment
<20 yrs 20-40 yrs > 40 yrs
Medical Always First resort after endometrial biopsy Temporizing & if
surgery is refused or
imminent menopause
Surgical Never Seldom, only if medical treatment fail First resort if bleeding
is recurrent
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36. Medical treatment:
Antifibrinolytics
Mechanism of action:
The endometrium possess an active fibrinolytic
system, & the fibrinolytic activity is higher in
menorrhagia.
Effect:
Greater reduction of menstrual bleeding than other
therapies (PSI, oral luteal phase progestagen &
etamsylate)
(Cochrane library,2002).
Tranexamic acid is effective in treating menorrhagia
associated with IUCD.
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37. Side effects: is dose related.
Nausea , vomiting, diarrhea, dizziness. Rarely:
transient color vision disturbance, intracranial
thrombosis. But, no evidence that tranxemic acid
increases the risk in absence of past or family
history of thrombophilia. This treatment is not
associated with an increase in side effects
compared to placebo or other therapies
(Cochrane library,2002).
Dose:
3-6 gm /d for the first 3 days of the cycle
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38. PSI:
Mechanism;
the endometrium is a rich source of PGE2 & PGF2œ
& its concentrations are greater in menorrhagia. PSI
decreases endometrial PG concentrations.
Effect:
PSI decreased menstrual blood by 24% &
norethisterone by 20%.
The beneficial effect of mefenamic acid on
MBL & other symptoms e.g. dysmenorrhea, headache,
nausea, diarrhea & depression persists for several
months.
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39. Dose:
Mefenamic acid 500 mg tds during menses.
Side effects:
nausea, vomiting, gastric discomfort, diarrhea,
dizziness. Rarely: haemolytic anemia,
thrombocytopenia. The degree of reduction of MBL
is not as great as it is with tranxamic acid but PSI
have a lower side effect profile.
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40. Etamsylate:
Mechanism of action:
maintain capillary integrity, anti-hyalurunidase activity
& inhibitory effect on PG
Dose:
500 mg qid, starting 5 days before anticipated onset
of the cycle & continued for 10 days
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41. Effect:
20% reduction in MBL.
There is no conclusive evidence of the effectivness of
etamsylate in reducing menorrhgea (Grade A)
Side effects:
headache, rash, nausea
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42. Systemic progestagens:
Norethisterone & medroxyprogesterone acetate
Effect:
Ovulatory DUB:
not effective if given at low dose for short duration
(5-10 days) in the luteal phase. Effective if NEA is
given at higher dose for 3 w out of 4 w (5 mg tds
from D5 to 26)
Anovulatory DUB:
useful
Side effects:
weight gain, nausea, bloating, edema, headache,
acne, depression, exacerbation of epilepsy &
migraine, loss of libido
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43. Intrauterine progestagens
Levonorgestrel intrauterine system
levonova,Mirena:
Delivers 20ug LNG /d. for 5 yr
Metraplant:
T shaped IUCD & levonorgestrel on the
shoulder & stem
Azzam IUCD:
Cu T & levonorgestrel on the stem
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44. Effect;
1.Comparable to endometrial resection for
management of DUB.
2.Superior to PSI & antifibrinolytics
3.May be an alternative to hysterectomy in some
patients
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46. Side effects;
1.BTB in the first cycles
2.20% develop amenorrhea within 1 yr
3.Functional ovarian cysts
Special indications:
1. Intractable bleeding associated with chronic illness
2. Ovulatory heavy bleeding
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47. The combined contraceptive pill:
Effect:
Reduce MBL by 50%
Mechanism of action:
endometrial suppression
Side effects;
headache, migraine, weight gain,
breast tenderness, nausea, cholestatic jaundice,
hypertension, thrombotic episodes,
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48. Danazol:
synthetic androgen with antioestrogenic &
antiprogestagenic activity
Mechanism;
inhibits the release of pituitary Gnt & has direct
suppressive effect on the endometrium
Effect:
reduction in MBL (more effective than PSI) &
amenorhea at doses >400 mg/d
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49. Side effects:
headache, weight gain, acne, rashes, hirsuitism,
mood & voice changes, flushes, muscle spasm,
reduced HDL, diminished breast size.
Rarely: cholestatic jaundice.
It is effective in reducing blood loss but side effects
limit it to a second choice therapy or short term use
only (Grade A)
Dose:
200 mg/d
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50. GnRH analog
Side effects;
hot flushes, sweats, headache, irritability,
loss of libido, vaginal dryness,
lethargy, reduced bone density.
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55. Indications:
1. Failure of medical treatment
2. Family is completed
3. Uterine cavity <10 cm
4. Submucos fibroid <5 cm
5. Endometrium is normal or low risk hyperplasia.
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56. Complications of hysteroscopic methods
1. Uterine perforation
2. Bleeding
3. Infection.
4. Fluid overload
5. Gas embolism
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58. Advantages:
1. Complete cure
2. Avoidance of long term medical treatment
3. Removal of any missed pathology
Disadvantages:
1.Major operation
2.Hospital admission
3.Mortality & morbidity
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