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Management of Testicular Cancer

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Title: Management of Testicular Cancer


1
Management of Testicular Cancer
  • Hassan G. TAAN
  • Urology Resident
  • AUBMC
  • Moderator Prof. Rami Nasr

2
  • Testicular cancer 1 male neoplasms , 5
    urological tumours, incidence 3-10 /100,000 per
    year in West
  • Risk factors cryptorchidism, Klinefelters
    syndrome, family history, contralateral tumor,
    and infertility
  • Germ cell tumors constitutes 95 of testicular
    tumors
  • Testicular tumours show excellent cure rates.
  • proper staging
  • chemotherapeutic combinations
  • early treatment-based radiotherapy and surgery
  • strict follow-up salvage therapies

3
STAGING Of TESTICULAR CANCER
4
Staging AJCC (American Joint Comittee on Cancer)
  • Stage 0 CIS
  • Stage I T1-4/N0/M0
  • IA T1
  • IB T2-4
  • IS ANY T, S1-3
  • Stage II T1-4/N1-3/M0
  • IIA N1
  • IIB N2
  • IIC N3
  • Stage III T1-4/N1-3/M1

5
Tumour Markers
  • Alpha-fetoprotein
  • Trophoblasts
  • Major serum binding protein produced by foetal
    yolk sac, liver, GIT
  • Negligible amounts after 1 year of age
  • T1/2 4-6 days
  • Beta-human chorionic gonadotrophin
  • Syncytiotrophoblasts
  • Secreted by placenta for maintanence of corpus
    luteum
  • T1/224 hours
  • LDH
  • tumour burden

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7
GERM CELL TUMORS
  • Seminoma
  • Typical/Classic (82 85 of seminomas)
  • Spermatocytic (2 12 of seminomas)extremely
    low metastatic
    potential. Mengt50years
  • Anaplastic previously classified as separate
    entity that was believed to be more
    aggressive/lethal due to greater mitotic
    activity. However, mitotic index is not
    associated with worse prognosis, so term no
    longer used
  • Nonseminomatous Germ Cell Tumors
  • Embryonal cell carcinoma
  • Yolk sac tumor
  • Teratoma
  • Choriocarcinoma
  • Mixed Tumors
  • Intratubular germ cell neoplasia (CIS)

8
  • Frequency of Histologic causes
  • GCT constitute 90 95 of all primary
    testicular malignancies
  • Seminoma 30 60
  • Embryonal carcinoma 3- 4 in pure
    form (present in 40 of NSGCTs)
  • Teratoma 5 10
  • Pure choriocarcinoma 1
  • Mixed GCTs 60

9
PATTERNS OF SPREAD OF GCTs
  • Right testis
  • - Interaortocaval nodes at level of
    2nd vertebral body
  • Left testis
  • Left paraaortic and preaortic nodes
    (bounded by left ureter, left renal vein, aorta
    and origin of IMA)
  • Cross-over Right to left (but NOT left to
    right)
  • Epididymis external iliac chain
  • Inguinal node mets may occur if
  • Scrotal involvement of primary tumor
  • Prior inguinal or scrotal surgery
  • Retrograde lymphatic spread from
    massive retroperitoneal LN deposits

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11
STAGE I SEMINOMA
  • The overall CSS rate under surveillance
    97-100 for seminoma stage I .
  • The drawback of surveillance intensive
    follow-up, repeated imaging of the
    retroperitoneal lymph nodes, for at least 5 years
    after orchidectomy
  • There was no significant difference between one
    cycle of carboplatin compared to adjuvant
    radiotherapy, with regard to recurrence rate,
    time to recurrence, and survival after a median
    follow-up of 4 years
  • Adjuvant radiotherapy to a para-aortic field or
    to a hockeystick field , with moderate doses
    (total 20-24 Gy), will reduce the relapse rate to
    1-3

12
SURVEILLANCE FOR STAGE I SEMINOMA
  • H PE ,serum tumor markers (bhCG, LDH, AFP) every
    3-4 months the first year, every 6 months the
    second year, then annually thereafter
  • Imaging Chest radiography each visit CT scan of
    the pelvis annually for 3 years if status post
    para-aortic radiotherapy

13
STAGE IIA-B SEMINOMA
  • 15 to 20 percent of seminoma patients have CS II
    disease, 70 of whom have CS IIA-B. Dog-leg
    radiotherapy using 25 to 30 Gy is employed at
    most centers
  • Long-term disease-free survival rates are 92 to
    100 for CS IIA and 87 to 90 for CS IIB , with
    in-field recurrences reported in 0 to 2 and 0
    to 7 of cases, respectively
  • Relapses are cured in virtually all cases with
    first-line chemotherapy, and disease-specific
    survival approaches 100
  • Induction chemotherapy using first-line regimens
    (BEP3 or EP4) is an accepted alternative to
    dog-leg radiotherapy for patients with bulky
    (gt3 cm) and/or multiple retroperitoneal masses
    because the risk of relapse is lower than with
    dog-leg radiotherapy (15 and 30 of CS IIA and
    IIB patients in one center)

14
Surveillance for stage IIa/b seminoma
  • H PE and serum tumor markers every 3-4 months in
    years 1-3, every 6 months in year 4, and then
    annually thereafter
  • Imaging Radiography each visit CT scan of the
    abdomen and pelvis during month 4 of the first
    year

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16
STAGE IIC AND III
  • Patients with CS IIC and III seminoma are treated
    with induction chemotherapy
  • Ninety percent of patients with advanced seminoma
    are classified as good risk and should receive
    either BEP3 or EP4 chemotherapy
  • Complete radiographic responses are reported in
    70 to 90 of patients, and the 5-year overall
    survival is 91
  • With BEP4 chemotherapy, the 5-year overall and
    progression-free survival is 79 and 75,
    respectively

17
Surveillance for stage IIc, III seminoma
  • H PE and serum tumor markers every 2 months the
    first year, every 3 months the second year, every
    4 months the third year, every 6 months the
    fourth year, and then annually thereafter
  • Imaging Chest radiography each visit CT scan of
    the abdomen and pelvis during month 4 of the
    first year status post surgery (otherwise, every
    3 months until stable) PET scan as clinically
    indicated

18
Follow Up - Seminoma
19
Relapses
  • Surveillance/Radiotherapy
  • BEP x 3
  • Chemotherapy cohort
  • VIP x 4 (vinblastine, ifosfamide and cisplatin)
    or
  • TIP x 4 (paclitaxol, ifosfamide and cisplatin)

20
Prognostic factors for occult metastatic disease
in testicular cancer
21
Impact on fertility and fertility-associated
issues
  • In patients in the reproductive age group,
    pre-treatment fertility
  • assessment (testosterone, LH and FSH
    levels) should be performed, and semen analysis
    and cryopreservation should be offered.
  • If cryopreservation is desired, it should
    preferably be performed before orchidectomy, but
    in any case prior to chemotherapy treatment
  • In cases of bilateral orchidectomy or low
    testosterone levels after treatment of TIN,
    life-long testosterone supplementation is
    necessary
  • Patients with unilateral or bilateral
    orchidectomy should be offered a
  • testicular prosthesis

22
Non Sminoma Germ Cell Tumors
  • Approximately one third of NSGCT patients have CS
    I with normal postorchiectomy levels of serum
    tumor markers
  • The optimal management of these patients
    continues to generate controversy because the
    long-term survival associated with surveillance,
    RPLND, and primary chemotherapy approaches 100
  • Up to 30 of NSGCT patients with clinical stage I
    (CS1) disease have subclinical metastases and
    will relapse if surveillance alone is applied
    after orchidectomy.

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24
Surveillance In NSGCT CS1
  • Close surveillance after orchidectomy in CS1
    NSGCT patients showed a
  • cumulative relapse rate of 30, with 80
    of relapses occurring during the first 12 months
    of follow-up, 12 during the second year and 6
    during the third year, decreasing to 1 during
    the fourth and fifth years
  • 35 of relapsing patients have normal levels of
    serum tumour markers
  • at relapse. 60 of relapses are in the
    retroperitoneum
  • Despite very close follow-up, 11 of relapsing
    patients presented with large-volume recurrent
    disease.
  • surveillance within an experienced surveillance
    programme may be offered to patients with
    non-risk stratified clinical stage I non-seminoma
    as long as they are compliant and informed about
    the expected recurrence rate as well as the
    salvage treatment

25
Follow Up Surveillance Stage I NSGCT
26
Primary chemotherapy In NSGCT CS1
  • Several studies involving two courses of
    chemotherapy with cisplatin, etoposide and
    bleomycin (PEB) as primary treatment for
    high-risk patients (having 50 risk of relapse)
    have been reported .
  • In these series, involving gt 200 patients, some
    with a median follow-up of nearly 8 years , a
    relapse rate of only 2.7 was reported, with very
    little long-term toxicity
  • Two cycles of cisplatin-based adjuvant
    chemotherapy do not seem to adversely affect
    fertility or sexual activity
  • slow-growing retroperitoneal teratomas after
    primary chemotherapy

27
Retroperitoneal lymph node dissection
  • If RPLND done, 30 have lymph node involvement,
    pathological stage II (PS2) disease . RPLND -gt
    -ve L.N (PS1), 10 of the PS1 patients relapse
    at distant sites.
  • The main predictor of relapse in CS1 NSGCT
    managed by surveillance, for having PS2 disease
    and for relapse in PS1 after RPLND-? vascular
    invasion in the primary tumour .
  • Patients without vascular invasion constitute
    50-70 of the CS1 population, and these patients
    have only a 15-20 risk of relapse on
    surveillance, VS 50 relapse rate in patients
    with vascular invasion

28
  • The risk of relapse for PS1 patients is lt 10 for
    those without vascular invasion and 30 for
    those with vascular invasion
  • If two (or more) courses of cisplatin-based
    chemotherapy are given adjuvant to RPLND in PS2
    cases, the relapse rate is reduced to lt 2,
    including teratoma relapse .
  • The risk of retroperitoneal relapse after a
    properly performed nerve-sparing RPLND is very
    low (lt 2), as is the risk of ejaculatory
    disturbance or other significant side-effects

29
  • In a randomised comparison of RPLND with one
    course of PEB chemotherapy, adjuvant chemotherapy
    significantly increased the 2-year
    recurrence-free survival to 99.41 as opposed to
    surgery, which had a 2-year recurrence-free
    survival of 92.37
  • It was also found that one adjuvant PEB reduced
    the number of recurrences to 3.2 in the
    high-risk and to 1.4 in the low-risk patients

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31
CS1S with (persistently) elevated serum tumour
markers
  • If the marker level increases after orchidectomy,
    the patient has residual disease. If RPLND is
    performed, up to 87 of these patients have
    pathological finding in the nodes .
  • An U/S of the contralateral testicle must be
    performed, if this was not done initially.
  • The treatment of true CS1S patients is still
    controversial. They may be treated with three
    courses of primary PEB chemotherapy and with
    follow-up as for CS1B patients (high risk) after
    primary chemotherapy, or by RPLND .
  • The presence of vascular invasion may strengthen
    the indication for primary
  • chemotherapy as most CS1S with vascular
    invasion will need chemotherapy sooner or later

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