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Cervical cancer
Sameer Sawaed
2016
Incidence and mortality
• Worldwide, cervical cancer accounted for an estimated
530,000 new cancer cases and for 275,000 deaths
• In developed countries in 2008, cervical cancer was the
tenth most common type of cancer in women (9.0 per
100,000 women) and ranked below the top ten causes of
cancer mortality (3.2 per 100,000). In contrast, in
developing countries it was the second most common
type of cancer (17.8 per 100,000) and cause of cancer
deaths (9.8 per 100,000) among women
Histopathology:
• Squamous cell carcinoma – 69%
• Adenocarcinoma (including adenosquamous) – 25%
• Other histology (e.g. small cell carcinoma, lymphoma,
sarcoma,…etc.) – 6%
Age distribution
- The lifetime risk of developing cervical cancer for United
States women is 0.76%. The mean age at diagnosis is 48
years
Age (year) Incidence of
cervical cancer
<20 0.1/100,000
20-24 1.5/100,000
30-85 11-15.8/100.000
Pathogenesis
• Human papillomavirus (HPV) is central to the
development of cervical neoplasia and can be detected
in 99.7% of cervical cancers.
• There are four major steps in cervical cancer
development:
1) Oncogenic HPV infection of the metaplastic epithelium
at the cervical transformation zone
2) Persistence of the HPV infection
3) Progression of a clone of epithelial cells from
persistent viral infection to precancer
4) Development of carcinoma and invasion through the
basement membrane
Pathogenesis
• Most HPV infections are transient. When HPV infection
persists, the time from initial infection to development of
high grade cervical intraepithelial neoplasia and, finally,
invasive cancer takes an average of 15 years, although
more rapid courses have been reported
• Among the more than 40 genital mucosal HPV types
identified, approximately 15 are known to be oncogenic.
Subtypes. HPV 16 and 18 are found in over 70 percent of
all cervical cancers.
Risk factors
Most of these factors are associated with an increased risk
of acquiring or having compromised immune response to
infection with human papillomavirus (HPV), the etiologic
agent of most cervical cancers. These include:
• Early onset of sexual activity
• Multiple sexual partners
• A high-risk sexual partner (e.g., a partner with multiple
sexual partners or known human papillomavirus
infection)
• History of sexually transmitted infections (e.g., Chlamydia
trachomatis, genital herpes)
• History of vulvar or vaginal squamous intraepithelial
neoplasia or cancer
Risk factors
• Immunosuppression (e.g. AIDS)
• Low socioeconomic status
• Others:
Non-white women
Early age at first birth (< 20 years old) and increasing
parity (>3 or more)
Smoking (SCC of the cervix only)
Oral contraceptive use
Cervical cancer is less common in sexual partners of
circumcised males
Routes of Spread:
Cervical cancer can spread by:
• Direct extension: may involve uterine corpus, vagina,
parametria, peritoneal cavity, bladder, or rectum.
Ovarian involvement by direct extension of cervical
cancer is rare; (0.5% in SCC and 1.7% of
adenocarcinomas)
• Lymphatic spread
• Hematogenous dissemination: the most common sites
are the lungs, liver, and bone
Clinical manifestation:
• Asymptomatic – abnormal cervical smear
• Vaginal bleeding
• Postcoital bleeding
• Abnormal vaginal discharge
In advanced disease
• Pelvic or lower back pain, which may radiate along the
posterior side of the lower extremities
• Bowel or urinary symptoms, such as pressure-related
complaints, hematuria, hematochezia, or vaginal passage
of urine or stool
FIGO staging of carcinoma of the cervix uteri
Stage 0: preinvasive carcinoma, CIS
Stage I: carcinoma strictly confined to the cervix (extension to the corpus should
be disregarded)
stage Ia - Preclinical carcinoma of the cervix, i.e. those diagnosed only by
microscopy
o Stage Ia1: lesion < 3 mm invasion & < 7 mm in width
o Stage Ia2: lesion 3-5 mm invasion & < 7 mm in width.
Stage Ib - lesion invasion > 5mm & / or diameter > 7 mm
o Stage Ib1: lesion < 4 cm
o Stage Ib2: lesion > 4 cm
Stage II: the carcinoma extend beyond the cervix but has not extend onto the
pelvic wall. The carcinoma involve the vagina, but not the lower one-third
Stage
IIa
- No obvious parametrial involvement (extension to the upper two
third of the vagina)
Stage
IIb
- Obvious parametrial involvement
Stage III: the carcinoma has extended to the pelvic wall. On rectal exam, there is no
cancer-free space between the tumor & the pelvic wall. The tumor involved the
lower third of the vagina. All cases of hydronephrosis or nonfunctioning kidney
Stage
IIIa
- Tumor extend to the lower third of the vagina (no extension to the
pelvic wall)
Stage
IIIb
- Extension onto the pelvic wall &/or hydronephrosis or non-functioning
kidney
Stage IV: the carcinoma has extended beyond the true pelvis or has clinically
involved the mucosa of the bladder or rectum.
Stage
Iva
- Spread to adjacent organs
Stage
IVb
- Spread to distant organs
Diagnosis:
Examination
• Pelvic examination – speculum, bimanual, and
rectovaginal examination for palpation and inspection
of the primary tumor, uterus, vagina, and parametria
• Examination for distant metastases – palpation of groin
and supraclavicular lymph nodes
Cervical biopsy: the diagnosis of cervical cancer is made
based upon histologic evaluation of a cervical biopsy
• Colposcopy with directed cervical biopsy
• Endocervical curettage
• Conization
Diagnosis
• Imaging studies - X rays, CT,MRI, PET…etc
• Lab: CBC,KFT, LFT, UA…etc.
Treatment
Surgical Management of Early Invasive Cancer of the
Cervix
Stage Comment Rx
Stage
Ia1
< 3 mm invasion
No lymph vascular
space invasion
Conization (or)
Simple hysterectomy
(abdominal or vaginal)
Stage
Ia1
< 3 mm invasion
With lymph vascular
space invasion
Trachelectomy + pelvic LNDs
(or)
Simple hysterectomy or
modified radical hysterectomy
+ pelvic LNDs
Treatment
Stage
Ia2
>3-5 mm invasion &
<7 mm in diameter
Radical trachelectomy + pelvic
LNDs
(or)
Modified radical hysterectomy
+ pelvic LNDs
Stage
Ib1
Lesion <2 cm Modified radical hysterectomy
with pelvic lymphadenectomy
Stage
Ib1
Lesion > 2 cm Radical hysterectomy with
pelvic lymphadenectomy
Complicationof radical hysterectomy:
Acute / subacute Complications
• Ureterovaginal / vesicovaginal fistula (2-3%)
• Pulmonary embolus (1-2%)
• Blood loss
• Febrile morbidity (25-50%): atelectasis, pelvic cellulitis,
urinary tract infection, wound infection, pelvic abscess,
and phlebitis
• Postoperative bladder dysfunction
• Lymphocyst formation
Chronic Complications
• Bladder hypotonic
• Ureteral strictures
• Compromised sexual activity, decreased lubrication, &
shortened vagina
Treatment
For more advanced disease (> stage 1B1): Chemoradiation
Compared with surgery, chemoradiation resulted in:
• Higher incidence of sexual dysfunction
• Higher incidence of bowel dysfunction
• A higher incidence of urinary incontinence
• Ovarian failure — women treated with surgery may be at
risk for premature ovarian failure possibly due to
impairment of ovarian perfusion. Pelvic RT (with or
without concomitant chemotherapy) uniformly results in
ovarian failure due to the doses required for curative
intent therapy.
Comparison of surgery versus radiations for stage Ib / IIa
cancer of the cervix
Surgery Radiation
Serious
complicat
ions
- Urologic fistula 3% - Intestinal & urologic
fistula & stricture in
1.4-5.3%
Vagina - Initially shortened, but
may lengthen with
regular intercourse
- Fibrosis & possible
stenosis particularly in
postmenopausal
women
Ovaries - may be conserved - Destroyed
Chronic
effects
- Bladder atony in 3% - Radiation fibrosis of
bladder & bowel in 6-
8%
Anatomic
structure
Simple
hysterectomy
Modified radical Radical
Uterus Removed Removed Removed
Ovaries Optional removal Optional removal Optional removal
Cervix Removed Removed Removed
Vaginal margin None 1-2 cm margin > 2-3 cm margin
Ureters Not mobilized Dissected through
broad ligament
Dissected through
broad ligament
Cardinal
ligaments
Divided at uterine
border
Divided where
ureter transit the
broad ligament
Divided at pelvic
sidewall
Uterosacral
ligaments
Divided at cervical
border
Partially resected Divided near sacral
origin
Bladder Mobilized to base of
cervix
Mobilized to upper
vagina
Mobilized to
middle vagina
Rectum Not mobilized Mobilized below
cervix
Mobilized below
middle vagina
Treatment
• Women who are not surgical candidates due to
poor functional status – chemoradiation
• Women who wish to preserve fertility – For
women of reproductive age who wish to
preserve their fertility and have a lesion size ≤2
cm and no lymph node metastases
Trachelectomy +/- PLNs may be offered
Prognosis
The major prognostic factors affecting survival among
women with cervical cancer are stage, nodal status, tumor
volume, depth of cervical stromal invasion, and
lymphovascular space invasion (LVSI).
Disease stage is the most important prognostic factor
Stage 5-years Survival rate
Ia 95%
Ib 80%
II 64%
III 38%
IV 14%
Recurrent Disease
• Following treatment of early stage cervical cancer, distant
metastases or multiple recurrence sites develop in 15 to
61 percent of cases, usually within the first two years of
completing treatment.
• Recurrent cervical cancer presents as disease isolated to
the pelvis (locoregional recurrence) or with disease
involving other organs or outside the pelvis
• Treatment depends on the mode of primary therapy &
the site of the recurrence, e.g.:
Patient who have initial treatment by surgery should be
considered for radiotherapy
Patient who had radiotherapy should be considered for
surgery provided the recurrence is central & there is no
evidence of distal recurrence
Screening and Prevention
• Cervical smear: the rate of cervical cancer has declined
significantly in settings in which cervical cancer screening
is employed
• HPV vaccine

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cervical cancer

  • 2. Incidence and mortality • Worldwide, cervical cancer accounted for an estimated 530,000 new cancer cases and for 275,000 deaths • In developed countries in 2008, cervical cancer was the tenth most common type of cancer in women (9.0 per 100,000 women) and ranked below the top ten causes of cancer mortality (3.2 per 100,000). In contrast, in developing countries it was the second most common type of cancer (17.8 per 100,000) and cause of cancer deaths (9.8 per 100,000) among women
  • 3. Histopathology: • Squamous cell carcinoma – 69% • Adenocarcinoma (including adenosquamous) – 25% • Other histology (e.g. small cell carcinoma, lymphoma, sarcoma,…etc.) – 6%
  • 4. Age distribution - The lifetime risk of developing cervical cancer for United States women is 0.76%. The mean age at diagnosis is 48 years Age (year) Incidence of cervical cancer <20 0.1/100,000 20-24 1.5/100,000 30-85 11-15.8/100.000
  • 5. Pathogenesis • Human papillomavirus (HPV) is central to the development of cervical neoplasia and can be detected in 99.7% of cervical cancers. • There are four major steps in cervical cancer development: 1) Oncogenic HPV infection of the metaplastic epithelium at the cervical transformation zone 2) Persistence of the HPV infection 3) Progression of a clone of epithelial cells from persistent viral infection to precancer 4) Development of carcinoma and invasion through the basement membrane
  • 6. Pathogenesis • Most HPV infections are transient. When HPV infection persists, the time from initial infection to development of high grade cervical intraepithelial neoplasia and, finally, invasive cancer takes an average of 15 years, although more rapid courses have been reported • Among the more than 40 genital mucosal HPV types identified, approximately 15 are known to be oncogenic. Subtypes. HPV 16 and 18 are found in over 70 percent of all cervical cancers.
  • 7. Risk factors Most of these factors are associated with an increased risk of acquiring or having compromised immune response to infection with human papillomavirus (HPV), the etiologic agent of most cervical cancers. These include: • Early onset of sexual activity • Multiple sexual partners • A high-risk sexual partner (e.g., a partner with multiple sexual partners or known human papillomavirus infection) • History of sexually transmitted infections (e.g., Chlamydia trachomatis, genital herpes) • History of vulvar or vaginal squamous intraepithelial neoplasia or cancer
  • 8. Risk factors • Immunosuppression (e.g. AIDS) • Low socioeconomic status • Others: Non-white women Early age at first birth (< 20 years old) and increasing parity (>3 or more) Smoking (SCC of the cervix only) Oral contraceptive use Cervical cancer is less common in sexual partners of circumcised males
  • 9. Routes of Spread: Cervical cancer can spread by: • Direct extension: may involve uterine corpus, vagina, parametria, peritoneal cavity, bladder, or rectum. Ovarian involvement by direct extension of cervical cancer is rare; (0.5% in SCC and 1.7% of adenocarcinomas) • Lymphatic spread • Hematogenous dissemination: the most common sites are the lungs, liver, and bone
  • 10.
  • 11. Clinical manifestation: • Asymptomatic – abnormal cervical smear • Vaginal bleeding • Postcoital bleeding • Abnormal vaginal discharge In advanced disease • Pelvic or lower back pain, which may radiate along the posterior side of the lower extremities • Bowel or urinary symptoms, such as pressure-related complaints, hematuria, hematochezia, or vaginal passage of urine or stool
  • 12. FIGO staging of carcinoma of the cervix uteri Stage 0: preinvasive carcinoma, CIS Stage I: carcinoma strictly confined to the cervix (extension to the corpus should be disregarded) stage Ia - Preclinical carcinoma of the cervix, i.e. those diagnosed only by microscopy o Stage Ia1: lesion < 3 mm invasion & < 7 mm in width o Stage Ia2: lesion 3-5 mm invasion & < 7 mm in width. Stage Ib - lesion invasion > 5mm & / or diameter > 7 mm o Stage Ib1: lesion < 4 cm o Stage Ib2: lesion > 4 cm Stage II: the carcinoma extend beyond the cervix but has not extend onto the pelvic wall. The carcinoma involve the vagina, but not the lower one-third Stage IIa - No obvious parametrial involvement (extension to the upper two third of the vagina) Stage IIb - Obvious parametrial involvement
  • 13.
  • 14. Stage III: the carcinoma has extended to the pelvic wall. On rectal exam, there is no cancer-free space between the tumor & the pelvic wall. The tumor involved the lower third of the vagina. All cases of hydronephrosis or nonfunctioning kidney Stage IIIa - Tumor extend to the lower third of the vagina (no extension to the pelvic wall) Stage IIIb - Extension onto the pelvic wall &/or hydronephrosis or non-functioning kidney Stage IV: the carcinoma has extended beyond the true pelvis or has clinically involved the mucosa of the bladder or rectum. Stage Iva - Spread to adjacent organs Stage IVb - Spread to distant organs
  • 15. Diagnosis: Examination • Pelvic examination – speculum, bimanual, and rectovaginal examination for palpation and inspection of the primary tumor, uterus, vagina, and parametria • Examination for distant metastases – palpation of groin and supraclavicular lymph nodes Cervical biopsy: the diagnosis of cervical cancer is made based upon histologic evaluation of a cervical biopsy • Colposcopy with directed cervical biopsy • Endocervical curettage • Conization
  • 16. Diagnosis • Imaging studies - X rays, CT,MRI, PET…etc • Lab: CBC,KFT, LFT, UA…etc.
  • 17. Treatment Surgical Management of Early Invasive Cancer of the Cervix Stage Comment Rx Stage Ia1 < 3 mm invasion No lymph vascular space invasion Conization (or) Simple hysterectomy (abdominal or vaginal) Stage Ia1 < 3 mm invasion With lymph vascular space invasion Trachelectomy + pelvic LNDs (or) Simple hysterectomy or modified radical hysterectomy + pelvic LNDs
  • 18. Treatment Stage Ia2 >3-5 mm invasion & <7 mm in diameter Radical trachelectomy + pelvic LNDs (or) Modified radical hysterectomy + pelvic LNDs Stage Ib1 Lesion <2 cm Modified radical hysterectomy with pelvic lymphadenectomy Stage Ib1 Lesion > 2 cm Radical hysterectomy with pelvic lymphadenectomy
  • 19. Complicationof radical hysterectomy: Acute / subacute Complications • Ureterovaginal / vesicovaginal fistula (2-3%) • Pulmonary embolus (1-2%) • Blood loss • Febrile morbidity (25-50%): atelectasis, pelvic cellulitis, urinary tract infection, wound infection, pelvic abscess, and phlebitis • Postoperative bladder dysfunction • Lymphocyst formation Chronic Complications • Bladder hypotonic • Ureteral strictures • Compromised sexual activity, decreased lubrication, & shortened vagina
  • 20. Treatment For more advanced disease (> stage 1B1): Chemoradiation Compared with surgery, chemoradiation resulted in: • Higher incidence of sexual dysfunction • Higher incidence of bowel dysfunction • A higher incidence of urinary incontinence • Ovarian failure — women treated with surgery may be at risk for premature ovarian failure possibly due to impairment of ovarian perfusion. Pelvic RT (with or without concomitant chemotherapy) uniformly results in ovarian failure due to the doses required for curative intent therapy.
  • 21. Comparison of surgery versus radiations for stage Ib / IIa cancer of the cervix Surgery Radiation Serious complicat ions - Urologic fistula 3% - Intestinal & urologic fistula & stricture in 1.4-5.3% Vagina - Initially shortened, but may lengthen with regular intercourse - Fibrosis & possible stenosis particularly in postmenopausal women Ovaries - may be conserved - Destroyed Chronic effects - Bladder atony in 3% - Radiation fibrosis of bladder & bowel in 6- 8%
  • 22. Anatomic structure Simple hysterectomy Modified radical Radical Uterus Removed Removed Removed Ovaries Optional removal Optional removal Optional removal Cervix Removed Removed Removed Vaginal margin None 1-2 cm margin > 2-3 cm margin Ureters Not mobilized Dissected through broad ligament Dissected through broad ligament Cardinal ligaments Divided at uterine border Divided where ureter transit the broad ligament Divided at pelvic sidewall Uterosacral ligaments Divided at cervical border Partially resected Divided near sacral origin Bladder Mobilized to base of cervix Mobilized to upper vagina Mobilized to middle vagina Rectum Not mobilized Mobilized below cervix Mobilized below middle vagina
  • 23. Treatment • Women who are not surgical candidates due to poor functional status – chemoradiation • Women who wish to preserve fertility – For women of reproductive age who wish to preserve their fertility and have a lesion size ≤2 cm and no lymph node metastases Trachelectomy +/- PLNs may be offered
  • 24. Prognosis The major prognostic factors affecting survival among women with cervical cancer are stage, nodal status, tumor volume, depth of cervical stromal invasion, and lymphovascular space invasion (LVSI). Disease stage is the most important prognostic factor Stage 5-years Survival rate Ia 95% Ib 80% II 64% III 38% IV 14%
  • 25. Recurrent Disease • Following treatment of early stage cervical cancer, distant metastases or multiple recurrence sites develop in 15 to 61 percent of cases, usually within the first two years of completing treatment. • Recurrent cervical cancer presents as disease isolated to the pelvis (locoregional recurrence) or with disease involving other organs or outside the pelvis • Treatment depends on the mode of primary therapy & the site of the recurrence, e.g.: Patient who have initial treatment by surgery should be considered for radiotherapy Patient who had radiotherapy should be considered for surgery provided the recurrence is central & there is no evidence of distal recurrence
  • 26. Screening and Prevention • Cervical smear: the rate of cervical cancer has declined significantly in settings in which cervical cancer screening is employed • HPV vaccine