Testicular

Question 1

Most common risk factor for testicular cancer?

Answer 1

cryptorchidism

Question 2

What is recommended prophylaxis for cryptorchidism?

Answer 2

orchiectomy, esp when intra-abdominal

Question 3

Relative risk of testicular cancer in 1st degree relatives

Answer 3

increases 6-10 fold

Question 4

What is intratubular germ cell neoplasia?

Answer 4

carcinoma in situ, risk of progression is 50% at 5 years if untreated

Question 5

Less common risk factors for testicular cancer?

Answer 5

Hypospadias
HIV (seminomas)
Testicular microlithiasis
Klinefelter & Down syndromes
exposure to exogenous estrogens in utero
peutz-Jegher syndrome and Carney complex (Sertoli cell)

Question 6

Common presentation for testicular cancer?

Answer 6

painless mass, heavy sensation in lower abd or perianal region

Question 7

What are the types of testicular tumors?

Answer 7

Germ cell (95%)
sex cord tumors
lymphoma, leukemia and plasmacytoma

Question 8

What are two types of germ cell tumors?

Answer 8

Seminoma and nonseminomas

Question 9

What is the most prevalent and specific cytogenetic abnormality in testicular cancer?

Answer 9

gain of 12p sequences; commonly i12p

Question 10

What are key histologic and serum characteristics of the different germ cell tumor subtypes?

Answer 10

Seminoma (pure) - AFP normal; bHCG: normal to mildly elevated; i12p (50%) “min b oma)
Spermatocystic seminoma: i12p (0%)
NSGCTs: i12p (80%)
-Embryonal: AFP & bHCG normal to mildly elevated “um bro could be both”
-Choriocarcinoma: AFP normal, bHCG > 1000 IU/L “human ““chorionic”” gonadotropin “
-Yolk sac: AFP > 100; bHCG normal “fetal yolk”
-Teratoma

Question 11

What are key serum tumor markers (STMs) and how are they broken up into mild, mod & high risk? What is their half-life

Answer 11

AFP (4-5 days) [ 10,000] “A is a 10 f partner”

b-HCG (18-36 hours) [ 50,000 “beta is two human butt cheegs”

LDH () [10x ULN) “L is 1.5 pieces of wood”

Question 12

Staging summary for testicular cancer?

Answer 12

Stage I: tumor only
Stage II: regional node involvement & mild STMs
Stage III: metastatic or high STMs
- IIIA: nonregional lymph nodes, pulm mets and/or mild STMs
- IIIB: nonregional lymph nodes, pulm mets and/or mod STMs
- IIIC: non pulm mets or marked STMs

Question 13

What are prognostic catergories for Seminoma?

Answer 13

No Poor

• Good: non pulmonary visceral mets; I-IIIB
• Int: non pulmonary visceral mets: IIIC

Question 14

What are prognositic catergories for NSGCT?

Answer 14

Good: I-IIIA
Int: IIIB
Poor: IIIC

Question 15

What is likelihood of cure in Stage I seminoma?

Answer 15

close to 100%

Question 16

What is criticial question when determining adjuvant therapy following resection for Stage I seminoma>

Answer 16

Is the patient compliant? - relapse rate of 15-20%; down to 5% if given chemo (carbo AUC 7 1-2 cycles or RT (20-25 Gy, PA-strip)

Question 17

What adjuvant therapy for Stage I Seminoma is preferred but withheld usually?

Answer 17

RT, due to secondary malignancies, 18.2% cumulative risk at 25 years; (PA-strip preffered field over hockey-stick and dog-leg)

Question 18

What is advantage of single dose of carbo (AUC 7) over RT for Stage I seminoma?

Answer 18

Less incidence of new contralateral GCT (0.2% vs 1.2%) 80% risk reduction

Question 19

What is relapse rate for Stage I Non-seminoma? How many are upstaged to Stage II following RPLND

Answer 19

30%

Question 20

Late recurrences for testicular cancer are common with and uncommon with?

Answer 20

common in seminoma and uncommon in non-seminoma

Question 21

What are two important factors in Stage I Non-seminoma that predict for relapse and favor adjuvant intervention?

Answer 21

presence of LVI (lymphovascular invasion) * (strongest)

embryonal component predominant

Question 22

What imaging modality is not recommended for NSGCTs

Answer 22

PET-CT

Question 23

What is recommended for adjuvant therapy in high risk Stage I Non-seminoma?

Answer 23

RPLND (preferred in US, avoid chemo toxicity, advantage of upstaging) versus chemo (BEP x 1-2, preferred in Europe due to low relapse rate of

Question 24

Key question for Stage I Non-seminoma s/p RPLND?

Answer 24

Compliance; if yes surveillance; if no BEP x 2 for pN1 or pN2 disease and BEP x3-4 for pN3 disease

Question 25

Most common complication of nerve sparing RPLND?

Answer 25

infertility due to retrograde ejaculation

Question 26

Post-orchiectomy adjuvant therapy for Stage I Non-seminoma with positive STMs?

Answer 26

BEP x 3 or EP x 4

Question 27

What does Stage II germ cell tumor imply and how is therapy different from Stage I?

Answer 27

Retroperitoneal node involvement; surveillance is not an option

Question 28

What is recommended for adjuvant therapy in Stage II seminoma?

Answer 28

IIA: RT (30-35Gy - preffered), or chemo
IIB: Chemo (BEP x 3 - preffered) or RT
IIC: Chemo only (BEP x 3, or EP x 4)

Question 29

Only situation where single agent carboplatin (AUC 7) is an option?

Answer 29

Stage I Seminoma

Question 30

What regimen did BEP replace? Advantage

Answer 30

PVB; not as good in bulky disease and the vinblastine can result in considerable neuromuscular toxicity

Question 31

BEP 3 versus 4 cycles

Answer 31

4 cycles is reserved for Seminoma Int risk and Non-Seminoma Int or Poor risk.; 3 is good for good risk, good?

Question 32

What determines choice between BEP and EP?

Answer 32

Pulmonary function (older); or atheletes

Question 33

Rule of thumb for residual masses in testicular germ cell tumors?

Answer 33

NSGCTs: always resect
Seminoma: resect based on size criteria of > 3; if well delineated or positive PET after 6 weeks (preferred method)

Question 34

What is recommended for adjuvant therapy in STM negative Stage II Non-seminoma post-orchiectomy?

Answer 34

• similar to seminoma except RPLND replaces RT
  IIA: RPLND or chemo
  IIB: Chemo (BEP x 3 - preffered) or RPLND
  IIC: Chemo only (BEP x 3, or EP x 4)

Question 35

For Stage IIA STM negative Non Seminoma; s/p adjuvant RPLND; if residual disease is present, what determines adjuvant plan?

Answer 35

Node status:

• pN1: surviellance
• pN2: BEP or EP x2 over surviellance
• PN3: BEP x 3 or EP x 4

Question 36

For Stage IIC STM negative Non Seminoma; s/p adjuvant chemo; if residual disease is present, what determines adjuvant plan?

Answer 36

residual mass > 1 cm: RPLND

if

Question 37

For Stage II STM positive Non Seminoma what is adjuvant recommendation?

Answer 37

BEP x3 or EP x 4

Question 38

Why do some providers recommend RPLND after chemotherapy for Stage II or III NSGCTs regardless of response?

Answer 38

Growing teratoma syndrome (teratoma’s are relatively resistent to chemotherapy): presents with clinical discordance, dropping STMs and stable or increasing mass

Question 39

For post-chemo NSGCTs patients with positive STMs or residual mass with viable tumor (not fibrosis or teratoma), what is given?

Answer 39

2 cycles of: 
EP, 
VIP (etop/ ifos/ cis), 
VeIP (vinblas/ ifos/ cis), 
TIP (paclitaxel/ ifos/ cis)

Question 40

For Stage III disease what regimen shows similar efficacy to BEP x 4 cycles but increased hematologic and GU toxicity? In what scenario is this regimen preffered?

Answer 40

VIP

-lung disease

Question 41

What non-invasive method can help differentiate teratoma from fibrosis?

Answer 41

None; only through surgical resection with path analysis

Question 42

What is strongest predictor of fibrosis for residual pulmonary disease in Stage III NSGCTs?

Answer 42

necrosis in retroperitoneum on RPLND prior to thoractomy (89% of cases on retrosepctive multicenter study of 215 patients)

Question 43

For GCTs that relapse within 4 weeks of receiving a cisplatin based therapy or during therapy are classified as? What are there options then?
What is 2 years out?

Answer 43

platinum refractory or absolutely refractory
- GEMOX based or HDCT
platinum resistant
- paclitaxel or ifosfamide based

Question 44

Extragonadal seminomas have what prognosis and are managed how?

Answer 44

Prognosis similar to gonadal primaries and managed similarly.

Question 45

Extragondal germ cell turmor are usually what subtype?

Answer 45

non-seminoma; pure seminoma is extremely rare

Question 46

Extragonadal non-seminoma have what prognosis and are managed how?

Answer 46

worse than gonadal counterparts; mediastinal are worst, automatically poor prognosis despite marker and disease burden

Question 47

What malignancy is reported with mediastinal non-seminomas?

Answer 47

leukemia, esp megakaryocytic lineage