Endometrial Cancer

British Gynaecological Cancer Society (BGCS) uterine cancer guidelines: Recommendations for practice. Published: Mar 2022.

NICE guideline [NG12] Suspected cancer: recognition and referral. 1.5 Gynaecological cancers. Last updated: Apr 2026.

BMS guideline Management of unscheduled bleeding on hormone replacement therapy (HRT). Published: Apr 2024.

Article Last Updated:20/04/2026

Endometrial Cancer

Endometrial cancer arises from the endometrium, the lining of the uterus, and is the most common type of uterine cancer. It most often presents with post-menopausal bleeding.

Updated UKMLA guide to endometrial cancer based on the BGCS guideline: risk factors, symptoms, diagnosis, referral, and management.

Definition

Endometrial cancer is a specific type and the most common form of uterine cancer.

Endometrial cancer arises from the endometrium, the lining of the uterus (womb).

Histology

Most common histological type: adenocarcinoma

To be precise, the most common type is endometrioid carcinoma, which is a type of adenocarcinoma

Other less common types include:

Serous carcinoma
Clear cell carcinoma

Epidemiology

Uterine cancer is the 4th most common cancer in females in the UK

Peak incidence: 75-79 y/o

Causes and Risk Factors

Type	Description	Risk factors
Type I (~80%) ^[Ref]	Strongly linked to oestrogen excess (oestrogen stimulates growth of endometrium without being opposed by progesterone) Better prognosis: lower-grade and slower-growing	Obesity – primary driver of the rising incidence of endometrial cancer BMI ≥40 is considered a major risk factor Metabolic conditions (diabetes, hyperlipidaemia, hypertension) PCOS Reproductive history that increases lifetime oestrogen exposure Early menarche Late menopause Nulliparity Long-term use of tamoxifen History of atypical endometrial hyperplasia
Type II	Unrelated to oestrogen exposure Worse prognosis: higher-grade and aggressive	Advanced age p53 tumour suppressor gene loss-of-function mutation BRCA1/2 mutations

Type

Description

Risk factors

Type I (~80%) ^[Ref]

Strongly linked to oestrogen excess (oestrogen stimulates growth of endometrium without being opposed by progesterone)

Better prognosis: lower-grade and slower-growing

Obesity – primary driver of the rising incidence of endometrial cancer
- BMI ≥40 is considered a major risk factor
Metabolic conditions (diabetes, hyperlipidaemia, hypertension)
PCOS
Reproductive history that increases lifetime oestrogen exposure
- Early menarche
- Late menopause
- Nulliparity
Long-term use of tamoxifen
History of atypical endometrial hyperplasia

Type II

Unrelated to oestrogen exposure

Worse prognosis: higher-grade and aggressive

Advanced age
p53 tumour suppressor gene loss-of-function mutation
BRCA1/2 mutations

Lynch syndrome (HNPCC) is a major inherited genetic cause of endometrial cancer

Lynch syndrome is considered a major risk factor for endometrial cancer (both type I and II)
- 40-60% lifetime risk of developing endometrial cancer
- ~3% of all endometrial cancers are directly caused by Lynch syndrome
Autosomal dominant mutation in DNA mismatch repair genes (e.g. MLH1, MSH2)
Other manifestations
- Early-onset colorectal cancer (see the Colorectal Cancer article for more information)
- Gastric cancer
- Ovarian cancer

Note that the following are protective factors against developing endometrial cancer

COCP (the progesterone counters oestrogen exposure)
LNG-IUS (the progesterone counters oestrogen exposure)
Smoking
- Note that the BGCS guideline did NOT comment on smoking as a protective factor
- However, traditional teaching considers smoking as a protective factor, supported by the general medical literature ^[Ref]

Clinical Features

Post-menopausal women (more common):

Post-menopausal bleeding – most common symptom
- Defined as vaginal bleeding that occurs at least 1 year after the last menstrual period in those who are NOT taking HRT
- ~50% probability of endometrial cancer in >70 y/o women presenting with post-menopausal bleeding (overall probability is 50-10%)
Unscheduled bleeding (unexpected / persistent bleeding) on HRT
Abnormal vaginal discharge
Haematuria

Pre-menopausal women:

Persistent intermenstrual bleeding
Heavy menstrual bleeding

Features of advanced disease:

Abdominal pain, distension, bloating
Changes in bowel or bladder habits
New cough (suggest lung metastasis)

Frequent sites for spread and metastasis:

Adjacent pelvic structures (e.g. vagina, ovaries, fallopian tubes, parametrium, bladder, rectum)
Pelvic and para-aortic lymph nodes
Lungs – primary site for distant spread
Other: liver, bones, peritoneum and abdominal cavity

Red Flags and When to Refer

Since clinical features alone do not distinguish endometrial hyperplasia from endometrial cancer, the same red flags and referral indications apply for both endometrial hyperplasia and cancer.

The only way to definitively distinguish between endometrial hyperplasia and cancer is via biopsy and histological examination.

For ≥55 y/o individuals with female reproductive organs (including women, trans-men and non-binary people):

Action	Indications
Suspected cancer pathway referral (to receive a diagnosis or exclusion of cancer within 28 days)	>55 y/o with unexplained post-menopausal bleeding that cannot be attributed to HRT*
Consider an urgent (within 2 weeks) TVUS	Unexplained vaginal discharge PLUS any of the following 1st presentation of vaginal discharge Thrombocytosis Haematuria
Visible haematuria PLUS any of the following Low haemoglobin levels Thrombocytosis Hyperglycaemia

Action

Indications

Suspected cancer pathway referral (to receive a diagnosis or exclusion of cancer within 28 days)

>55 y/o with unexplained post-menopausal bleeding that cannot be attributed to HRT*

Consider an urgent (within 2 weeks) TVUS

Unexplained vaginal discharge PLUS any of the following

1st presentation of vaginal discharge
Thrombocytosis
Haematuria

Visible haematuria PLUS any of the following

Low haemoglobin levels
Thrombocytosis
Hyperglycaemia

*if <55 y/o with unexplained post-menopausal bleeding → consider a suspected cancer pathway referral

Red flags and referral for women who are taking HRT:

Bleeding >3-6 months after starting HRT (the 6-month cut-off applies to those without risk factors for endometrial cancer)
Bleeding >3 months after changing HRT regimen

See the Hormone Replacement Therapy (HRT) article for details on the management of unscheduled bleeding on HRT.

Investigation and Diagnosis

Pre-Diagnosis Investigations

1st line: TVUS

Purpose: measure the double-layer endometrial thickness
An endometrial thickness of ≥4 mm requires further investigation
- The 4mm cut-off is specifically for post-menopausal women who are NOT on HRT
- Any abnormal bleeding in tamoxifen users should prompt urgent investigation, as ultrasound is unreliable in these patients

While TVUS is a useful imaging tool, its primary role is to measure the thickness and structure of the endometrial lining to determine if further testing is needed. It is useful in ruling out disease; if the endometrial thickness is below the cut-off, the probability of cancer is reduced to <1%

TVUS alone cannot reliably distinguish between endometrial hyperplasia and endometrial cancer. Histological examination (biopsy) is the only reliable way.

Further investigation (definitive): outpatient endometrial biopsy (e.g. Pipelle biopsy)

If the patient has persistent / recurrent bleeding despite a -ve biopsy → hysteroscopy for direct visualisation

Tumour marker CA125 is NOT recommended for routine testing.

CA125 may be raised non-specifically in the presence of bulky metastatic disease. Its main clinical role is in the diagnostic work-up of ovarian cancer.

Post-Diagnosis Work-Up

Purpose	Investigations
Staging	Chest X-ray / CT chest – ALL patients to check for lung metastasis MRI pelvis to assess for local invasion CT TAP – for high-grade / high-risk cancers
Lynch syndrome screening	Immunohistochemistry testing for mismatch repair deficiency – ALL patients
Lymph node assessment	Sentinel lymph node biopsy

Management

Clinical category	Corresponding FIGO stage	Management principles
Locally early	I (confined to the uterus)	Total hysterectomy with bilateral salpingo-oophorectomy A minimally invasive (laparoscopic or robotic) approach is recommended
Locally overt	II (invaded the cervical stroma, but not beyond the uterus)	Total hysterectomy with bilateral salpingo-oophorectomy Either minimally invasive or open surgery is appropriate (depending on the patient’s frailty, size of uterus, extent of tumour)
Locally advanced	III (spread to serosa, adnexae, vagina, parametrium, or pelvic/para-aortic lymph nodes) / IVA (invasion to bladder or bowel mucosa)	2 approaches: Primary debulking surgery to remove all visible tumour (if complete macroscopic resection is feasible), or Neoadjuvant approach (if complete resection is unlikely): neoadjuvant chemotherapy followed by interval debulking surgery
Metastatic	IVB (distant metastasis e.g. to the lungs, liver, bones, inguinal lymph nodes)	Systemic therapy Standard 1st line: doublet chemotherapy (carboplatin and paclitaxel) Hormonal therapy (progestins) can be used for low-grade hormone-receptor +ve disease

Fertility sparing management:

Eligibility: ONLY stage 1 AI endometrial cancer (no myometrial invasion) or atypical endometrial hyperplasia
Treatment options:
- Mainstay: primary hormonal therapy for 6-12 months (oral progestins or LNG-IUS)
- Alternative: combination of progestins with GnRH or metformin
- A hysteroscopic resection to remove visible tumour bulk prior to starting progestin therapy may be considered