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Title: Gestational Trophoblastic Disease (GTD) Gestational Trophoblastic Neoplasia (GTN )


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Gestational Trophoblastic Neoplasia (GTN)
  • Zohreh Yousefi Professor of Obstetrics and
    Gynecology,
  • Fellowship of Gynecology Oncology , Ghaem
    Hospital,
  • website www.zohrehyousefi.com

3
  • Danforth's
  • Williams Obstetrics, 23e
  • B erek and Hacker's Gynecologic Oncology
  • Up To Dat
  • GESTATIONAL TROPHOBLASTIC DISEASE
  • PATHOGENESIS
  • DIAGNOSIS
  • MANAGEMENT
  • GESTATIONAL TROPHOBLASTIC NEOPLASIA
  • TREATMENT
  • SUBSEQUENT PREGNANCY

4
  • Gestational trophoblastic disease (GTD) is term
  • group of tumors with abnormal trophoblast
    proliferation
  • produce human chorionic gonadotropin (hCG)

5
  • GTD histologically is divided into
  • benign
  • hydatidiform moles
  • ( complete and partial)
  • Malignant
  • Invasive mole

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  • Non -molar trophoblastic neoplasms
  •  
  • Choriocarcinoma
  • Placental site trophoblastic tumor
  • Epithelioid trophoblastic tumor

7
Gestational trophoblastic neoplasia (GTN )
  • Malignant forms of gestational trophoblastic
    disease
  • GT N is all GTD except hydatidiform mole
  •  
  • Weeks or years following any type of pregnancy
  • But frequently occur after a hydatidiform mole

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Hydatidiform mole
  •  
  • Microscopic (classic findings)
  • Absence embryonic elements
  • Trophoblastic proliferation
  • (cytotrophoblast and
    syncytiotrophoblast)
  • Stromal edema and hydropic degeneration
  • Absence of blood vessels

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Macroscopic of Hydatidiform mole
  • Hydropic villi Grapelike vesicles filled
    clear material
  • usually 1 to 3cm diameter
  • proliferation of the trophoblast

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  • Hydatidiform mole

    Complete mole Partial mole Partial mole
























































  • Partial mol ( fetal tissue)
  • Grossly placenta a mixture of normal and
  • hydropic
    villi
  • Fetus Severe growth restriction
  • Multiple congenital anomalies

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Risk Factors hydatidiform mole
  •  
  • Strongest risk factors are
  • Age and a
  • history of prior hydatidiform mole
  •  
  • Both extremes of reproductive age
  • adolescents twofold risk
  • Older than 40 tenfold risk

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  • history of Prior mole
  • the risk of another mole
  • Complete mole is 1.5 percent
  • Partial mole is 2.7 percent
  • Two prior molar pregnancies
  • the risk is 23 percent

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  • An ethnic predisposition
  • Diet (Deficiencies of protein or)
  • (Vitamin A deficiency)
  • animal fat
  • Smoking
  • Increased paternal age

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Pathogenesis
  • Abnormal fertilization process
  • Normal ovum with a duplicated haploid sperm
  • Inactive ovum chromosomes
  • Karyotype 46, XX
  • diploid and result from androgenesis
  • Partial moles triploid karyotype
  • 69, XXX, 69,XXY

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Clinical Findings
  • Because universal sonography in prenatal care
  • Typically diagnosed at a mean of 10 weeks
  •  
  • Vaginal bleeding
  • spotting to profuse hemorrhage
  • Moderate iron-deficiency anemia

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  • Exaggerated early pregnancy symptoms
  • Nausea and vomiting ( hyperemesis)
  • Abdominal cramp

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  • Abnormally enlarged and soft uterus uterine
    growth
  • Theca-lutein cysts (hCG) 25 to 60
  • (Torsion, infarction, rupture and hemorrhage)
  • Releases antiangiogenic factors that activate
    endothelial damage
  • Severe preeclampsia
  • hypoxic trophoblastic mass

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  • All hydatidiform moles secrete hCG
  •  
  • Thyrotrophic -like effects of hCG
  • hCG acts a thyrotrophic substance
  • Elevated serum free thyroxine (T4)
  • (TSH) levels to be decreased
  • thyroid hyper function
  • thyroid storm

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Diagnosis
  • Amenorrhea followed by irregular bleeding
  • Spontaneous passage of molar tissue
  • High values Serum ß-HCG measurement
  • confirming the diagnosis
  • IHC stain positively for p57

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  • Sonography
  • Echogenic uterine mass with
  • anechoic cystic spaces
  • without a fetus or amnionic sac
  • The appearance as snowstorm

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Transvaginal sonogram demonstrating the snow
storm appearance.
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Mis-diagnosis
  • Incomplete abortion
  • missed abortion
  • Cystic degeneration
  • uterine leiomyoma
  •  

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  • which of the following symptoms will a highly
    intelligent physician assistant immediately
    consider hydatidiform mole?
  • pelvic pain at night during the first trimester
  • significantly elevated BP in the first trimester
  • significant bloody vaginal discharge  in the
    first trimester
  • nausea and vomiting in the first trimester

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  • Answer is B

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Management
  • Termination of Molar Pregnancy
  • Evacuation and Curettage
  • Hysterectomy (rarely and select cases
  • no desired future
    pregnancy )
  • Chest radiograph
  • Initiate effective contraception
  • OCP or MPA poor compliance

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  • Serum hCG levels
  • 48 hours of evacuation (baseline)
  • Weekly until undetectable Weekly until
  • normal for 3 consecutive weeks
  • monthly until normal for at least 6
    consecutive months
  • Median time for resolution is 9 weeks
    for complete

  • 7 weeks for partial
  • Hysterectomy reduces the incidence of
    malignant sequelae
  • does not eliminate follow-up

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hCG change
  • HM 84-100
    days
  • Spontaneous abortion 19 days
  • Normal delivery 12 days
  • Ectopic pregnancy 8-9 days

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  • After molar evacuation
  • risk factors for malignant squeal
  • 15 - 20 complete moles
  • 1 - 5 partial moles
  •  
  • 1 5 of HM become invasion moles
  • 2.5 progress into
    choriocarcinoma

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Twin Pregnancy (Normal Fetus and Coexistent
Complete Mole)
  • Diagnosis is difficult
  • (early pregnancy ultrasound)
  • A single partial molar pregnancy with
    abnormal fetus Distinguished

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  • A few cases the diagnosis is not suspected
  • until examination of the placenta
  • following delivery

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  • Amniocentesis ( fetal karyotype )
  • diploid or triploid
  • If fetal karyotype is normal
  • Major fetal malformations are excluded by
    ultrasound
  •  
  • Chest X-ray performed
  • Serum hCG values
  •  
  • If there is no evidence of metastatic disease
  • to allow the pregnancy
  •  

33
Possible risk for developing
  • Subsequent GTN
  • Preterm delivery
  • Preeclampsia
  • Sever hemorrhage

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Persistent GTD
  • Persistently elevated serum hCG level
  • Irregular vaginal bleeding
  • Persistent theca lute in cysts
  • (2 to 4 months regress spontaneously)
  • Uterine sub involution
  • Risk factors for GTN

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Risk factors of GTN
  • Older age
  • ß-hCG levels gt 100,000 mIU/mL
  • Large uterine size for-gestational age
  • Theca-lutein cysts gt 6 cm
  • Earlier recognition and evacuation of molar
    pregnancies
  • not lower risk neoplasia

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Criteria for Diagnosis of Gestational
Trophoblastic Neoplasia
  • Criteria for the diagnosis of postmolar GTN
  • 1. Plateau or rise of serum ß-hCG level
  • 2. Detectable serum ß-hCG level for
  • 6 months or more
  • 3. Histological criteria for choriocarcinoma
  • 4-Irregular bleeding ,uterine sub involution

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Plateau of serum ß-hCG level ( 10 percent) for
four easurements during a period of 3 weeks or
longer days 1, 7, 14, 21 Rise of serum ß-hCG
level gt 10 percent during three weekly
consecutive , during a period of 2 weeks or
moredays 1, 7, 14

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Diagnosis
  • Sonography Abdomino pelvic
  • or trans vaginal
    sonography
  • Radiograph of chest
  • Chest CT scan
  • Brain CT scan or
  • MRI

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SPESIAL
  • 1-Selective angiography of abdominal and pelvic
    or hepatic (if indicated )
  • 2-Whole body PET Less commonly (occult disease
    )
  • 3-Stool guaiac tests
  • If positive test is or if gastrointestinal
    symptoms
  • be routinely performed in persistent GTN
  • 4- complete radiographic evaluation
  • of the gastrointestinal tract

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GTN CLASSIFICATION
  • Invasive Mole
  • Almost all invasive moles arise from partial or
    complete moles
  • Deep penetration into the myometrium
  • or peritoneum
  • Involvement of vaginal vault

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Invasive hydatidiform mole infiltrating the
myometrium
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Choriocarcinoma
  • Most common follow a term pregnancy
  • or miscarriage
  • Rapidly growing both myometrium
  • and blood
    vessels
  • Blood-borne metastases

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  • differentiation between
  • invasive mole and choriocarcinoma
  • if we see villi, it must be invasion mole
  • if we cant see villi, it is choriocarcinoma
  •  
  •  

44
Common Sites for Metastatic Gestational
Trophoblastic Tumors
Site Per cent
Lung 60-95
Vagina 40-50
Vulva/cervix 10-15
Brain 5-15
Liver 5-15
Kidney 0-5
Spleen 0-5
Gastrointestinal 0-5
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Symptoms
  • Metastatic symptoms
  • Profuse vaginal bleeding
  • Vaginal or cervical metastasis
  • (bluish nodule in vaginal)
  • Abdominal pain (intra-abdominal hemorrhage)
  • Cough, hemoptysis
  • Headache, nausea, vomit, paralysis or coma
  • Urologic hemorrhage

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Lung metastasis
  • Four principal pulmunary radiologic patterns
  • Snowstorm pattern (Alveolar pattern )
  • Discrete rounded densities
  • Plural effusion
  • Embolic pattern

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Brain metastasis
  • Plasma CSF /hCG level ratio is normally
  • gt60 1
  • In patients with CNS metastases lt60 1
  • Falsely lowered plasma CSF /hCG level
  • First -trimester abortions
  • In the absence of lung or vaginal metastasis
  • Risk of cerebral and hepatic spread
  • is exceedingly low

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  • Generally in GTN
  • Serum hCG levels combined Clinical
    findings
  •  
  • Rather than a histological specimen
  • Diagnose and treat this malignancy

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Follow-up of GTN patients ß-subunit until hCG
  • Weekly until normal for 3 consecutive
    weeks
  • monthly until normal for at least 3
    consecutive months
  • at 1-month interval for 1 year
  • at 1- month interval for 2 years in high
    stage
  • at yearly interval for many years
  • (increased risk of late recurrence)
  •  

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  • Be careful
  • hCG
  • Pelvic examination
  • Chest X-ray
  • unusual rise of serum hCG
  • Rule out Normal pregnancy
  • Ectopic pregnancy
  • False-Positive hCG

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  • False-Positive hCG
  • Quiescent GTN
  • Phantom hCG
  • Pituitary hCG
  • Non-gynecologic tumors secreted -hCG

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Quiescent GTN
  • Constant, low level of hCG lt100 IU/L
  • Without evidence of a primary or metastatic
    malignancy
  • Persisting for periods 3 months to 16 years
  • Slow-growing
  • Oral contraceptive pills
  • and avoid pregnancy until
  • hCG has been undetectable for six months
  • 20 percent will eventually have recurrent
    active
  •  
  • H hCG assay is critical

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H CG variants
  •  
  • Hyperglycosylated hCG (H -hCG)
  • hCG produced by syncytiotrophoblasts
  • (H -hCG) synthesized by cytotrophoblast
  • (H -hCG) absolute marker of ongoing invasion
  • hCG-H is detectable gt1 ng/ml active GTN
  • To discriminate quiescent disease

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Phantom hCG
  •  False positive serum hCG
  • Send the serum to two laboratories
  • Using different commercial assays
  • If negative in one or both
  • false positive hCG
  • Presence of hCG in serum but not urine

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  • Heterothallic antibodies may results
  • false-positive
  • False positive are at risk for recurrent
  • Risk for other false positives, such as
  • CA-125 and thyroid antibodies

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Pituitary hCG
  •  
  • Secreted LH and hCG pulsatile and
    paralleled
  • Higher levels of h CG in postmenopausal
  • than premenopausal Cross-reactivity with
    LH
  • Pituitary production hCG ranges from
  • 1 to 32 mIU/mL 
  • HRT or BSO or OCP after 23 weeks
  • Suppress hCG Pituitary production

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  • Staging of GTN
  •  
  • WHO Scoring System

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Staging
  • International staging of WHO may be summarized as
    follows
  • ? lesion localized in uterus, no metastasis
  • ? lesion extends beyond uterus, but still
    confined to internal genitalias
  • ? pulmonary lesion
  • ? metastasis to other distant sites.

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IIa
IIb
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IIIalt3cm or locate in half lung IIIb disease
beyond IIIa
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Who Orgnaization prognostic scoring system for
gestational trophoblastic neoplasia
Prognostic factor 0 1 2 4
Age lt39 gt39 _ -
Antecedent pregnancy Hydatidiform Abortion , ectipic Term pregnancy -
Interval (months) lt4 4-6 7-12 gt12
hCG level (IU/liter) lt10 10-10 10-10 gt10
ABO blood groups (female/male) O/A B A/O AB
Largest tumor (cm) lt3 3-5 gt5 _
Site of metastasis _ Spleen, kidney Gastrointestinal tract, liver Brain
Number of metastases _ 1-3 4-8 gt8
Prior chemotherapy _ _ Single drug Multiple drugs
The total score is obtained by adding the
individual scores for each prognostic factor .
Total score lt4 , low risk 5-7 , intermediate
risk gt8 , high risk . Interval between
antecedent pregnancy and start of chemotherapy.
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  • According to the FIGO staging of gestational
    trophoblastic tumors
  • a lady with choriocarcinoma having
  • lung metastasis will belong to which stage

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protocol for treatment of GTD
  • Clinically staging( FIGO)
  • WHO scoring
  • Again, it is stressed that the diagnosis of
  • GTN made by persistently elevated serum
  • ß-hCG without confirmation by pathological
    tissue study

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Choice of treatment
  • Chemotherapy ( highly sensitive )
  • Surgery ( unresponsive or drug
    fails )
  • Irradiation (brain and liver ) 

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  • Chemotherapy are best management
  • Protocols Single-agent for
  • low-risk Methotrexate
  • Combination for high-risk disease
    EMA-CO
  • Early-stage GTN is typically cured
  • Later -stage disease usually responds
  • to chemotherapy
  •  

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Surgery in malignant GTN
  • Hysterectomy
  • Laparoscopy
  • Craniotomy (brain hemorrhage)
  • Thoracotomy
  • (solitary nodules in drug-resistant disease )
  • selective resection of lesion in uterus or
    liver

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Main causes of death
  • Hemorrhage
  • Infection
  • Metastasis

71
Placental Site Trophoblastic Tumor (PSST)
  • PSTT or non-trophoblastic malignancy
  • Uncommon tumor arises from implantation
    site-intermediate trophoblast
  • Secrete (hPL) from intermediate cells
  • Relatively small amounts of hCG
  • hCG free ß-subunit is more than one third of hCG
    (30)

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  • Typically local myometrial invasion
  • Rare systemic metastases
  • Treatment of ( PSST) is preferred hysterectomy
  • Because resistant to chemotherapy
  • For higher-risk than stage I
  • combination chemotherapy given

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Epithelioid Trophoblastic Tumor
  • This rare tumor
  • Intermediate trophoblast -type
  • Grossly a nodular fashion
  • Primary treatment is hysterectomy
  • Relatively resistant to chemotherapy
  • Approximately a fourth this neoplasm
  • will have metastatic disease,
  • combination chemotherapy

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SUBSEQUENT PREGNANCY
  • Pregnancy outcomes are usually normal
  • May develop
  • 1-Repeat molar gestation 2-percent
  • 2-Spontaneous abortions
  • 3-Congenital anomalies
  • 4-Ovarian failure (chemotherapy)
  • 5-Secondary tumors including
  • leukemia
  • colon cancer, melanoma
  • and breast cancer

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After Termination of Subsequent Pregnancy
  • Sonographic evaluation in early pregnancy
  • pathological evaluation placenta after delivery
  • serum ß-hCG level is measured 6 weeks
    postpartum

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Conclusion
  • The possibility of metastatic GTN should be
    considered
  • In any woman of the reproductive age
  • Presenting with metastatic disease
  • Or
  • an unknown primary site of malignancy

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