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The incidence is higher
amongst the white population
of the United States and
lowest in India and Japan.
Persistent stimulation of endometrium with unopposed estrogen is
the single most important factor for the development of
endometrial cancer.
Postmenopausal with a median age of 60
Late menopause—The chance of carcinoma increases, if
menopause fails to occur beyond 52 years.
Common in unmarried
In married – asso with nulliparity
Corpus Cancer Syndrome – obesity, HTN, DM
Obesity  high free oestradiol  which is
due to decreased SHBG
Unopposed oestrogen stimulation (Ovarian
tumours, PCOS)
 Family history or personal history of colon, ovarian or
breast cancer increases the risk of endometrial cancer.
Fibroid is associated in about 30 percent cases.
Endometrial hyperplasia precedes carcinoma in about 25 percent
cases.
Naked eye—The uterus may be smaller, normal or even enlarged.
Two varieties are found:
Localised  on the fundus  sessile/pendulated. Myometrium
involvement is late.
Diffuse  through endometrium then myometrium (commonly) 
reaches the serosal coat.
Adenocarcinoma (endometrioid 80%)
Adenocarcinoma with squamous elements.
 Papillary serous carcinoma (5–10%)
Mucinous adenocarcinoma (5%).
Clear cell adenocarcinoma (5%).
Secretory carcinoma (1%).
Squamous cell carcinoma.
Mixed carcinoma
Direct: It is slow growing, it is confined to the stroma for
a long time but eventually, it spreads in all directions.
Thus, it may infiltrate the myometrium and spread to the
parametrium or into the peritoneal cavity.
Lymphatic: The lymphatic spread is usually late.
Lymphatic spread involves pelvic, paraaortic (through
infundibulopelvic ligament) and rarely inguinal and
femoral (through lymphatics of round ligament) nodes.
Hematogenous: Blood borne spread occurs late. The
common sites of metastases are lungs, liver, bones and
brain.
Usually a nullipara, likely to be postmenopausal.
There may be history of delayed menopause.
She may be obese; likely to have hypertension or diabetes
Postmenopausal bleeding (75%)
which may be slight,
irregular or continuous.
The bleeding at times may be excessive.
In Premenopausal women  irregular & excessive bleeding.
There is watery and offensive discharge due to pyometra.
Pain is common. It may be colicky due to uterine contractions in an
attempt to expel the polypoidal growth.
 Few patients (< 5%) remain asymptomatic.
 Speculum examination reveals the cervix looking healthy and the
blood or purulent offensive discharge escapes out of the external os.
 Bimanual examination reveals—The uterus is either atrophic,
normal or may be enlarged due to spread of the tumor, associated
fibroid or pyometra.
 The uterus is usually mobile unless in late stage, when it becomes
fixed.
 Endometrial biopsy
 Pap Smear  +ve only in 30%  so not a reliable
 Ultrasound and Colour Doppler  ET, Hyperechoic endometrium with
irregular outline. Increased vascularity. Intrauterine fluid.
 Hysteroscopy  direct visualisation of endometrium and targeted
biopsy
 Fractional Curettage  to know the extent of growth.
 CT scan of abdomen and pelvis  Lymph nodes
 MRI  myometrial invasion
 PET differentiate between normal and cancerous tissue.
Endometrial carcinoma
Endometrial carcinoma
Endometrial carcinoma

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Endometrial carcinoma

  • 1.
  • 2.
  • 3. The incidence is higher amongst the white population of the United States and lowest in India and Japan.
  • 4.
  • 5. Persistent stimulation of endometrium with unopposed estrogen is the single most important factor for the development of endometrial cancer.
  • 6. Postmenopausal with a median age of 60
  • 7. Late menopause—The chance of carcinoma increases, if menopause fails to occur beyond 52 years.
  • 8. Common in unmarried In married – asso with nulliparity Corpus Cancer Syndrome – obesity, HTN, DM
  • 9. Obesity  high free oestradiol  which is due to decreased SHBG Unopposed oestrogen stimulation (Ovarian tumours, PCOS)
  • 10.  Family history or personal history of colon, ovarian or breast cancer increases the risk of endometrial cancer.
  • 11. Fibroid is associated in about 30 percent cases. Endometrial hyperplasia precedes carcinoma in about 25 percent cases.
  • 12. Naked eye—The uterus may be smaller, normal or even enlarged. Two varieties are found: Localised  on the fundus  sessile/pendulated. Myometrium involvement is late. Diffuse  through endometrium then myometrium (commonly)  reaches the serosal coat.
  • 13. Adenocarcinoma (endometrioid 80%) Adenocarcinoma with squamous elements.  Papillary serous carcinoma (5–10%) Mucinous adenocarcinoma (5%). Clear cell adenocarcinoma (5%). Secretory carcinoma (1%). Squamous cell carcinoma. Mixed carcinoma
  • 14. Direct: It is slow growing, it is confined to the stroma for a long time but eventually, it spreads in all directions. Thus, it may infiltrate the myometrium and spread to the parametrium or into the peritoneal cavity.
  • 15. Lymphatic: The lymphatic spread is usually late. Lymphatic spread involves pelvic, paraaortic (through infundibulopelvic ligament) and rarely inguinal and femoral (through lymphatics of round ligament) nodes.
  • 16. Hematogenous: Blood borne spread occurs late. The common sites of metastases are lungs, liver, bones and brain.
  • 17.
  • 18. Usually a nullipara, likely to be postmenopausal. There may be history of delayed menopause. She may be obese; likely to have hypertension or diabetes
  • 19. Postmenopausal bleeding (75%) which may be slight, irregular or continuous. The bleeding at times may be excessive.
  • 20. In Premenopausal women  irregular & excessive bleeding. There is watery and offensive discharge due to pyometra. Pain is common. It may be colicky due to uterine contractions in an attempt to expel the polypoidal growth.  Few patients (< 5%) remain asymptomatic.
  • 21.  Speculum examination reveals the cervix looking healthy and the blood or purulent offensive discharge escapes out of the external os.  Bimanual examination reveals—The uterus is either atrophic, normal or may be enlarged due to spread of the tumor, associated fibroid or pyometra.  The uterus is usually mobile unless in late stage, when it becomes fixed.
  • 22.  Endometrial biopsy  Pap Smear  +ve only in 30%  so not a reliable  Ultrasound and Colour Doppler  ET, Hyperechoic endometrium with irregular outline. Increased vascularity. Intrauterine fluid.  Hysteroscopy  direct visualisation of endometrium and targeted biopsy  Fractional Curettage  to know the extent of growth.  CT scan of abdomen and pelvis  Lymph nodes  MRI  myometrial invasion  PET differentiate between normal and cancerous tissue.