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Gestational Trophoblastic Disease
:GTD
 Dr Mebanshanbor Garod
 (MS General Surgery, FMAS,
 FEBS Surgical Oncology)

 Surgical Oncology Dept.,
 NEIGRIHMS, Shillong
A spectrum of interrelated conditions
originating from placenta:
Pre malignant conditions:
 Complete (CHM) and
 Partial hydatidiform moles moles (PHM)
 Invasive Mole
Malignant conditions:
 Choriocarcinoma
 Placental Site Throphoblastic Tumor (PSTT)
 Epitheloid trophoblastic tumor (ETT)
Persistent GTD (aka GTN) rises from
cytotrophoblast and syncitial cells of villous
trphoblast ,produces hCG
PSTT & ETT originates from intermediate
cells of extra villous trophoblast & sparsely
produce hCG
1 in 1500 pregnancy
Very young <16 years; advanced maternal
age >45 years.
20% will develop malignant sequelae.
1. CLINICAL; Usually during the first trimester of
pregnancy
 most common symptom: abnormal bleeding
 hyperemesis gravidarum
 uterine enlargement greater than expected for
gestational age (CHM)
 absent fetal heart sounds
2. USG “snowstorm” appearance, cystic
enlargement of the ovaries in 2nd trimester
(CHM)
3. hCG>I00000 mIU/ml
Rule out complictions (preeclampsia,
anemia etc)
Hysterectomy Vs Suction curettage
Increasing hCG levels :
• Increase of three values > 10% over 2 weeks or
• Plateau (four values ± 10% over 3 weeks )
• hCG > 20000 IU/l after >4 weeks after evacution
Histologic diagnoses of Choriocarcinoma
or invasive mole from uterine currettage
Clinical or radiographic evidence of
metastases
CC occurs in approximately 1 in 20,000–
40,000 pregnancies
 50% after term pregnancies
25% after molar pregnancies
 remainder after other gestational events
PSTT/ETT can develop after any type of
pregnancy
CC & PSTT/ETT:
Diagnosis tricky: months to years after
pregnancy as symptoms are non specific
Urine/serum hCG not always elevated
1. hCG
2. HISTOPATH: D&C for hyditaform mole
3. USG Pelvis
4. CT Chest: Persistent GTD or CC
(suspicious CXR findings)
5. MRI Brain: neurological symptoms or
lung mets on CT
STaGE I
1. Hysterectomy
2. Single agent Chemotherpy: MTX-F or Act
D
Stable hCG for three consecutive weeks
Re-elevated hCG
Not falling at least once within 18 days of
first treatment
All patients treated with combination
chemotherapy
Selective use of Radiation therapy and
surgery
 three drug doublet regimen TE/TP
Paclitaxel etoposide and cisplatin
Little application
Selected patients with cerebral mets
WBI (3000 cGY)
Hysterectomy : heavy bleeding, large bulky
intrauterine masses, sigificant pelvic
sepsis
Unresponsive solitary masses in the
liver/spleen/kidneys
Persistent lung nodules: solitary, limited to
one lung, hCG < 1000
 Stage I: TAH, Pelvic LN sampling
 Other stages & Metastatic disease: multi
agent CT , EP/EMA
FIGO scoring system : determine the risk of
resistance.
FIGO
1. 0-6: single agent MTX/FA or ACT-D
6 weeks maintenance after normalisation of HCG
2. >/ 7 multi agent CT EMA/CO
6 weeks maintenance therapy/8 weeks with poor pgronostic factors
(liver/brain mets)
3. Ultra high risk : EP/EMA or TE/TP
• Surgery : isolated foci of chemo-resistant disease
• PSTT/ETT
 Stage I: TAH, Pelvic LN sampling
 Other stages & Metastatic disease: multi agent CT , EP/EMA

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Gestational trophoblastic neoplasia

  • 1. Gestational Trophoblastic Disease :GTD  Dr Mebanshanbor Garod  (MS General Surgery, FMAS,  FEBS Surgical Oncology)   Surgical Oncology Dept.,  NEIGRIHMS, Shillong
  • 2. A spectrum of interrelated conditions originating from placenta: Pre malignant conditions:  Complete (CHM) and  Partial hydatidiform moles moles (PHM)  Invasive Mole Malignant conditions:  Choriocarcinoma  Placental Site Throphoblastic Tumor (PSTT)  Epitheloid trophoblastic tumor (ETT)
  • 3. Persistent GTD (aka GTN) rises from cytotrophoblast and syncitial cells of villous trphoblast ,produces hCG PSTT & ETT originates from intermediate cells of extra villous trophoblast & sparsely produce hCG
  • 4. 1 in 1500 pregnancy Very young <16 years; advanced maternal age >45 years. 20% will develop malignant sequelae.
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  • 6. 1. CLINICAL; Usually during the first trimester of pregnancy  most common symptom: abnormal bleeding  hyperemesis gravidarum  uterine enlargement greater than expected for gestational age (CHM)  absent fetal heart sounds 2. USG “snowstorm” appearance, cystic enlargement of the ovaries in 2nd trimester (CHM) 3. hCG>I00000 mIU/ml
  • 7. Rule out complictions (preeclampsia, anemia etc) Hysterectomy Vs Suction curettage
  • 8. Increasing hCG levels : • Increase of three values > 10% over 2 weeks or • Plateau (four values ± 10% over 3 weeks ) • hCG > 20000 IU/l after >4 weeks after evacution Histologic diagnoses of Choriocarcinoma or invasive mole from uterine currettage Clinical or radiographic evidence of metastases
  • 9. CC occurs in approximately 1 in 20,000– 40,000 pregnancies  50% after term pregnancies 25% after molar pregnancies  remainder after other gestational events PSTT/ETT can develop after any type of pregnancy
  • 10. CC & PSTT/ETT: Diagnosis tricky: months to years after pregnancy as symptoms are non specific Urine/serum hCG not always elevated
  • 11. 1. hCG 2. HISTOPATH: D&C for hyditaform mole 3. USG Pelvis 4. CT Chest: Persistent GTD or CC (suspicious CXR findings) 5. MRI Brain: neurological symptoms or lung mets on CT
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  • 14. STaGE I 1. Hysterectomy 2. Single agent Chemotherpy: MTX-F or Act D
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  • 18. Stable hCG for three consecutive weeks Re-elevated hCG Not falling at least once within 18 days of first treatment
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  • 20. All patients treated with combination chemotherapy Selective use of Radiation therapy and surgery
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  • 22.  three drug doublet regimen TE/TP Paclitaxel etoposide and cisplatin
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  • 24. Little application Selected patients with cerebral mets WBI (3000 cGY)
  • 25. Hysterectomy : heavy bleeding, large bulky intrauterine masses, sigificant pelvic sepsis Unresponsive solitary masses in the liver/spleen/kidneys Persistent lung nodules: solitary, limited to one lung, hCG < 1000
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  • 27.  Stage I: TAH, Pelvic LN sampling  Other stages & Metastatic disease: multi agent CT , EP/EMA
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  • 29. FIGO scoring system : determine the risk of resistance. FIGO 1. 0-6: single agent MTX/FA or ACT-D 6 weeks maintenance after normalisation of HCG 2. >/ 7 multi agent CT EMA/CO 6 weeks maintenance therapy/8 weeks with poor pgronostic factors (liver/brain mets) 3. Ultra high risk : EP/EMA or TE/TP
  • 30. • Surgery : isolated foci of chemo-resistant disease • PSTT/ETT  Stage I: TAH, Pelvic LN sampling  Other stages & Metastatic disease: multi agent CT , EP/EMA