Testicular Cancer

Question 1

Risk factors for developing testis cancer including germ cell neoplasia in situ (GCNIS)?

Answer 1

history of UDT/cryptorchidism (4-6x, reduced by 2-3 x if orchidopexy prior to puberty)

family history

personal history of testis cancer

Question 2

Risk of occult systemic disease for stage one testis cancer is lowest for :

Answer 2

pure seminoma vs. NSGCT

Question 3

Pure seminomas are more sensitive to chemotherapy and radiation relative to NSGCT?

Answer 3

YES

Question 4

The most undifferentiated type of NSGCT is?

Answer 4

embryonal carcinoma AND has totipotential capacity (differentiate into other NSGCT - yolk sac, choriocarcinoma, teratoma)

Question 5

Why is presence of teratoma important for management?

Answer 5

Although histologically benign, may contain genetic anomalies found in malignant GCT → uncontrollable growth and invasion or transformation into somatic-type malignancies

universally resistant to chemo and radiation

ONLY curable by surgical resection

Question 6

What are the testis cancer tumor markers and their associated histologies?

Answer 6

alpha fetoprotein (AFP) → yolk sac and embryonal (chorio and seminoma do NOT produce) → ½ life 5-7 days

human chorionic gonadotropin (hCG) → chorio and embryonal and syncytiotrophoblastic cells in seminoma → ½ life 24-36 h

lactate dehydrogenase (LDH) → nonspecific, best for estimating disease bulk

Question 7

Staging for testis cancer is based on:

Answer 7

pathologic stage of tumor

post orchiectomy tumor markers

staging by PE and imaging

Question 8

Testis TNM

Answer 8

Question 9

Testis TNM stage:

Answer 9

Question 10

Testis Risk Categories:

Answer 10

Question 11

A solid mass on PE or imaging is:

Answer 11

GUIDELINE STATEMENT 1

malignant neoplasm until proven otherwise

Question 12

When finding solid mass on PE or imaging, what is first step?

Answer 12

GUIDELINE STATEMENT 2

serum tumor. markers (AFP, hCG, and LDH) prior to any treatment

Question 13

Prior to intervention for testicular mass, patients should be counseled:

Answer 13

GUIDELINE STATMENT 3

risk of hypogonadism and infertility

offered sperm banking (consider prior to orchiectomy if unclear status of contralateral or known subfertility)

Question 14

What type of scrotal imaging should be used?

Answer 14

GUIDELINE STATEMENT 4

scrotal ultrasound with doppler (for unilateral or bilateral masses)

Question 15

What workup is required for testicular microlithiasis?

Answer 15

GUIDELINE STATEMENT 5

testicular microlithiasis in absence of solid mass and risk factors doe snot confer and increased risk of malignant neoplasm and doesn’t require further evaluation

Question 16

Patient with normal tumor markers (hCG and AFP) and indeterminate findings on PE or US, what is next step?

Answer 16

GUIDELINE STATEMENT 6

Repeat imaging 6-8 weeks

(< 2 cm 50-80% are not cancer → benign tumors, infarcts, Leydig cell nodules)

Question 17

In initial workup of testicular lesion, any other imaging modalities besides US?

Answer 17

GUIDELINE STATEMENT 7

MRI should NOT be used in initial eval and dx of testicular lesion suspicious for neoplasm

Question 18

Lesion determined by US and PE suspicious for malignancy, next steps after tumor markers?

Answer 18

GUIDELINE STATEMENT 8

with normal contralateral testis

inguinal orchiectomy (testis sparing not recommended, trans-scrotal discouraged)

GUIDELINE STATEMENT 9

testicular prosthesis should be discussed prior to orchiectomy

Question 19

What is recommended when a patient underwent a scrotal orchiectomy and found to have a testis neoplasm?

Answer 19

GUIDELINE STATEMENT 10

increased risk of recurrence and may be considered for adjunctive tx (excision of scar or RT) for local control

Question 20

Discuss role of testis sparing surgery, considerations, and surgical considerations?

Answer 20

GUDIELINE STATMENT 11A

tss through inguinal incision in pts wishing to preserve gonadal fx with masses < 2 cm and (1) equivocal US/PE and negative hCG and AFP (2) congenital, acquired or functionally solitary testis, or (3) b/l synchronous tumors

GUIDELINE STATMENT 11B

counseled regarding (1) high risk of local recurrence (2) need for monitoring with PE/US (3) role of adjuvant RT to testis to reduce local recurrence (4) impact of RT ons perm and testosterone (5) risk of testicular atrophy and need for tRT and/or subfertility/infertility

GUIDELINE STATMENT 11C

in addition to suspicious mass, multiple bx of ipsi testis normal parenchyma (GCNIS) should be obtained and evaluated by GU pathologist

Question 21

In patients with hx of GCT or GCNIS the risk of second primary tumor in contralateral testis is:

Answer 21

GUIDELINE STATEMENT 12

Rare but significant increase risk

(2%overall, 70% metachronous, 30% synchronous)

Question 22

In patient with GCNIS on testis biopsy or malignant neoplasm after TSS, what are recommendations and options:

Answer 22

GUIDELINE STATEMENT 13A

with GCNIS or s/p TSS → inform patients of r/b of surveillance, radiation, or orchiectomy

GUIDELINE STATEMENT 13B

recommend surveillance in pts who prioritize preservation of fertility and testicular androgen production

GUIDELINE STATEMENT 13C

recommend RT (18-20 Gy) or orchiectomy in patients who prioritize reduction of cancer risk taking into account the less risk of hypogonadism with RT

Question 23

Discuss utility of serum tumor markers in treatment planning:

Answer 23

GUIDELINE STATEMENT 14

Nadir makers should be repeated at appropriate T ½ time interval after orchiectomy for staging and risk stratification

GUIDELINE STATEMENT 15

for pts with elevated AFP or hCG post orchiectomy, clinicians should monitor tumor markers to establish nadir levels before treatment only if nadir would influence treatment

Question 24

In metastatic GCT (Stage IIC or III) planning for chemo what is the regimen based on?

Answer 24

GUIDELINE STATEMENT 16

IGCCCG risk stratification based on serum tumor markers (hCG, AFP, LDH) prior to chemo, staging imaging studies, and tumor histology from orchiectomy. Any post-pubertal male, should be treated as an adult

Question 25

Describe Good Prognosis risk category for Seminoma and Non-Seminoma GCT:

Answer 25

Non-Seminoma

Testis/retroperitoneal primary, no non-pulmonary visceral mets, good markers

(AFP < 1000, hCG < 5000, LDH < 1.5 x norm)

56% of non-seminomas

5 yr PFS 89%

5 yr OS 92%

Seminoma

any primary site, no non-pulmonary visceral mets, normal AFP, any hCG, any LDH

90% seminomas

5 y PFS 82%

5 y OS 86%

Question 26

Describe Intermediate Prognosis for Seminoma and Non-Seminoma GCT:

Answer 26

Non-Seminoma

testis/retroperitoneal primary, no non-pulmonary visceral mets, intermediate markers

(AFP > ,1000 < 10,000, hCG > 5,000 and < 50,000, and LDH > 1.5 x N and < 10 x N)

28% non-seminomas

5 y PFS 75%

5 yr OS 80%

Seminoma

any primary site, non-pulmonary visceral mets, normal AFP, any hCG, any LDH

10% seminomas

5 y PFS 67%

5 y OS 72%

Question 27

Describe Poor Prognosis for Seminoma and Non-Seminoma GCT:

Answer 27

Non-Seminoma

mediastinal primary, non-pulmonary visceral mets, poor markers

(AFP > 10,000, hCG > 50,000, LDH >10 x N)

16% of non-seminomas

5 y PFS 41%

5 y Survival 48%

Seminoma

No patients classified as poor

Question 28

Post orchiectomy elevated (AFP and hCG - 3 x normal), what should be done before treatments?

Answer 28

GUIDELINE STATEMENT 17

A rising trend should be confirmed before management decisions are made as false positive elevations may occur

Question 29

Patients with newly diagnosed GCT, what imaging should be done?

Answer 29

GUIDELINE STATEMENT 18

CT scan A/P with IV contrast or MRI (if CT contra)

GUIDELINE STATEMENT 19A

Chest imaging

GUIDELINE STATMENT 19B

In setting rising of post-orchiectomy markers, mets on CT A/P, CXR or PE, A CHEST CT

GUIDELINE STATMENT 19C

Stage 1 seminoma, CXR (superior specificity) over Chest CT

GUIDELINE STATEMENT 19D

NSGCT Chest CT over CXR (especially if recommended adjuvant tx)

GUIDELINE STATEMENT 20

Newly dx GCT, do NOT obtain PET for staging

Question 30

In newly dx GCT, how do you guide management decisions?

Answer 30

GUIDELINE STATEMENT 21

assign of TNM category

(image chest, A/P, post orchiectomy nadir AFP, hCG, and LDH)

GUIDELINE STATEMENT 22

Imaging w/in 4 weeks

Markers w/in 10days

Question 31

Management decisions for newly dx GCT should be made with whom and based on which histology?

Answer 31

GUIDELINE STATEMENT 23

Multidisciplinary team (urology, med onc, rad onc, pathology, radiology)

GUIDELINE STATEMENT 24

Expert review of pathology in clinical scenarios where treatment decisions impacted

(review of expert alters subtype in 4-6%, 27% pathology reports revised)

Question 32

In newly dx patients post orchiectomy with normal STM and equivocal findings on imaging for mets, how do you decide on tx?

Answer 32

GUIDELINE STATEMENT 25

Consider repeating imaging 6-8 weeks to clarify extent of dz before tx

Question 33

Recommended tx for Seminoma GCT stage 1:

Answer 33

GUIDELINE STATEMENT 26

Surveillance after orchiectomy (<20% recurrence)

adjuvant RT and carboplatin-based chemo are less preferred (3-9% recurrence)

Question 34

Recommended tx for pts w/Seminoma GCT and Stage IIa/b with LN < 3 cm? For IIB w/LN > 3 cm?

Answer 34

GUIDELINE STATEMENT 27

IIA/B LN < 3 cm: recommend RT(dog leg up to 30 Gy) or multi-agent cisplatin-based chemo (4 cycles EP or 3 cycles BEP) based on SDM

IIB LN >3 cm: chemotherapy recommended

Question 35

Long term chemotherapy for GCT a/e:

Answer 35

cardiovascular, gastrointestinal, hematologic, infertility, secondary malignancy, neurologic, renal, pulmonary

Question 36

Recommended tx for patients with NSGCT with elevated or rising post orchiectomy serum AFP and hCG:

Answer 36

GUIDELINE STATEMENT 28

risk appropriate multi-agent chemotherapy

Question 37

Recommended treatment for Stage 1A NSGCT:

Answer 37

Reminder: IA pT1N0M0S0(beyond seminiferous tubules, still in testicle)

GUIDELINE STATEMENT 29

Surveillance preferred

RPLND or BEP x 1 (decline surveillance or non-compliance)

Question 38

What are independent risk factors for relapse in NSGCT?

Answer 38

LVI and embryonal carcinoma

Question 39

Recommended treatment for Stage 1B NSGCT:

Answer 39

Reminder IB: pT2-T4N0M0S0

GUIDELINE STATEMENT 30

surveillance, RPLND, or 1-2 BEP based on SDM

Question 40

Patients with stage 1 NSGCT and any secondary somatic malignancy (teratoma with malignant transformation) in primary tumor, what is recommended tx:

Answer 40

GUIDELINE STATEMENT 31

RPLND

(teratoma has capacity to de-differentiate into somatic malignancy including sarcomas and carcinomas)

Question 41

Patient with stage IIA NSGCT and S0, recommended tx:

Answer 41

Reminder IIA: any pTN1 (<5 nodes, < 2 cm) M0 S0 or S1 (in this question S0)

GUIDELINE STATEMENT 32

RPLND (benefit avoid chemo/remove teratoma) or chemotherapy

Question 42

Patient with stage IIB NSGCT and S0, recommended tx:

Answer 42

Reminder: Stage IIB: Any pT, N2 (1 but <5 nodes with >2cm <5 cm, OR grown outside LN, OR > 5 nodes), M0S0 (this case) or S1

GUIDELINE STATEMENT 33

Risk-appropriate BEP vs. possible RPLND (select patients, S0)

Question 43

Who should perform RPLND and how?

Answer 43

GUIDELINE STATMENT 34

referral to experience surgery at high volume center

GUIDELINE STATEMENT 35

experience and expertise with MIS can consider, acknowledge lack of long-term oncologic data

Question 44

Describe an RPLND with curative intent:

Answer 44

GUIDELINE STATEMENT 36

*full b/l template with pts with suspicious LN on CT or intra-op or teratoma

*full b/l or modified template may be performed in clinically neg nodes

*right modified template may omit para-aortic LN below IMA (omission para-aortic LN above IMA controversial)

*left modified template may omit paracaval, precaval, and retrocaval LN (omission of interaortocaval LN controversial)

*nerve-sparing should be offered to preserve ejaculatory function

*nerve-sparing should NOT compromise quality of dissection

*complete retroaortic and/or retrocaval LND w/dissection and division of lumbar vessels should be performed within planned template

*ipsilateral gonadal vessels removed in ALL patients

*cephalad extent is crus of diaphragm to level of RA, caudad extent crossing of ureter over ipsilateral common iliac

Question 45

After primary RPLND, what is recommended mgmt based on staging features:

Answer 45

GUIDELINE STATEMENT 37

Surveillance or chemo with stage II (not pure teratoma)

pN1 and/or pN1-3 pure teratoma → surveillance

pN2-3 → multi-agent chemotherapy (BEP)

Question 46

What is surveillance protocol for Stage I seminoma:

Answer 46

GUIDELINE STATEMENT 38

H&P, cross-sectional imaging of abd +/- pelvis q 4-6 mo x 2 y, q6-12 mo yrs 3-5

routine chest and STM as indicated clinically

Question 47

What is surveillance protocol for Stage I NSGCT:

Answer 47

GUIDELINE STATEMENT 39

After Orchiectomy: H&P and STM (AFP, hCG, +/- LDH) q2-3 mo x 1 year, q 2-4 mo in year 2, q 4-6 mo in year 3, q 6-12 mo years 4-5, >5 if indicated

GUIDELINE STATEMENT 40

CXR + CT A +/- P q 3-6 mo year 1 (start 3 mo), q 4-12 mo in year 2, once year 3-5

Men with higher risk of relapse should be imaged at shorter intervals (e.g. LVI)

Question 48

Patients who relapse should be treated according to what? Stage 1 GCT on surveillance have what risk of relapse > 5 years?

Answer 48

GUIDELINE STATMENT 41

pts with relapse on surveillance should be fully restaged and treated based on new TMN-s status

GUIDELINE STATEMENT 42

Stage I GCT on surveillance < 1% late relapse after 5 y, annual serologic and radiographic assessment should be performed as indicated based on clinical concerns

Question 49

How should survivors of GCT be monitored for hormonal status and long term sequelae of treatment?

Answer 49

GUIDELINE STATEMENT 43

monitor for s/s hypogonadism, if present serum AM testosterone and LH

GUIDELINE STATEMENT 44

survivors s/p chemo and/or RT → elevated risk CVD, establish PCP to manage modifiable risk factors (diet, exercise, smoking, lipids, BP, glucose)

GUIDELINE STATEMENT 45

survivors s/p chemo and/or RT → elevated risk secondary malignancy, establish PCP for checkups and cancer screening

Question 50

What are important questions to ask a young man who presents with scrotal swelling?

Answer 50

urethral discharge/unprotected sex

dysuria/hematuria

back pain (myalgia)

hx of UDT

Shortness of breath

trauma

constitutional sxs (weight loss/night sweats)

headache

pain

Question 51

What are important aspect of physical exam with suspected testicular mass?

Answer 51

lung exam

testis/spermatic cord

hydrocele

gynecomastia

inguinal exam

abdominal exam

Question 52

what are all possible elements of post orchiectomy workup and why?

Answer 52

MRI brain if headache or neuro sxs

sperm banking if not done prior

repeat STM

CT A/P

CXR (ok if CT A/P normal and STM normal after orchiectomy) vs. CT (poor prognostic features or sob)

Bone scan: clinical features warrant ALP + scan (pain, fracture?)

Question 53

what is the primary mechanism of spread of testicular tumors?

Answer 53

lymphatic

Question 54

what is important testing to conduct prior to chemo, if lung mets or pulm sxs/hx?

Answer 54

PFTs

If abnormal avoid Bleomycin

Question 55

What are short term and long term a/e of Bleomycin?

Answer 55

Pulmonary fibrosis

Raynaud’s

Question 56

What are short term and long term a/e of Etoposide?

Answer 56

Myelosuppression

Question 57

What are short term and long term a/e of Cisplatin?

Answer 57

Neurotoxicity

Nephrotoxicity

Ototoxicity

Question 58

Describe risks and concerns for consent for post-chemo RPLND?

Answer 58

risks retrograde ejaculation, vascular injury, blood txfn, possible grafting of vessels, nephrectomy. chylous ascites, ileus, bowel/ureteral injury

*minimize perioperative FiO2 and fluid overload (Bleo)

Question 59

Describe operative steps of RPLND?

Answer 59

1. Transabdominal midline incision (xiphoid to below umbilicus)
   
   1. (can do robotic if can justify)
2. Incise posterior peritoneum from ileocecal valve to ligament of Treitz
3. Mobilize right colon, small bowel, and duodenum off RP to expose great vessels with clear exposure of renal veins; IMV can be divided to facilitate mobilization of left colon mesentery if necessary
4. Split and roll technique with ligation/division of all lumbar vessels to allow complete mobilization of great vessels to facilitate a complete dissection; L3 most important for ejaculation (sympathetic chains just above common iliacs
5. Complete resection of remainder of right spermatic cord
6. Nerve sparing can be attempted if no compromised of oncologic principles/complete resection, but not required

Question 60

Describe template for post chemo RPLND:

Answer 60

lateral → right and left ureter

Inferior → ureter crossing iliac

Superior → renal vessels (suprahilar not routinely required)

Question 61

How do you diagnose chylous ascites?

Answer 61

CT A/P shows fluid ascites, air in small and large bowel

JP triglycerides elevated (like 1000)

Question 62

What are the management steps for chylous ascites?

Answer 62

1st line: diuretic with fluid & salt restriction and low fat diet with medium chain fatty acid supplement

2nd line: if persistent for weeks, NPO/TPN

Question 63

What do you do for 3 cm RP mass after RPLND for NSGCTin patient with known teratoma?

Answer 63

High dose chemo/BMT

VeIP (etoposide, ifosfamide, cisplatin, mesna)

TIP (paclitaxel, ifosfamide, cisplatin, mesna)

Question 64

What is treatment for stage Ib (pT2N0M0S0) seminoma?

Answer 64

Surveilance, XRT or chemo - Carboplatin 1 (preferred) or 2 cycles

Question 65

What are the side effects of carboplatin?

Answer 65

short term myelosuppression

long term secondary malignancy and heart disease

Question 66

What are side effects of RT?

Answer 66

short term: nausea, emesis, diarrhea, leukopenia

long term: dyspepsia, PUD, oligospermia, secondary malignancy

Question 67

Patient with recurrent seminoma s/p EP x 4, with residual RP mass (originally 6 cm now 4 cm). Next steps? If positive, next steps?

Answer 67

PET scan (CT PET)

> 6 weeks after completion chemo

Next steps:

RPLND vs. Surveillance (controversy, both acceptable per NCCN)

Question 68

What are common presentations in testicular carcinoma?

Answer 68

1. Painless testicular enlargement–most common
2. Testicular mass–firm lump or nodule
3. Testicular pain–heaviness, aching, acute pain~10%
4. Gynecomastia–%5
5. Abdominal mass or pain
6. Respiratory problems

Question 69

When performing orchiectomy for testicular mass, when would you recommend biopsy of contralateral side?

Answer 69

US abnormal

UDT or poor spermatogenesis

Marked atrophy (volume <12)

Question 70

Half lives of STM?

Answer 70

BhCG 24-46 h (check 1 week)

AFP 5-7 days (check 4 weeks)

LDH 4 days

Question 71

Treatment options for IB seminoma?

Answer 71

1. Surveillance: best option with low risk (tumor size < 4 cm, no rete testis invasion, recurrence as low as 6%); need compliance, concern for radiation (CTs)
2. EBRT: seminoma very radiosensitivity, long term radiation toxicity < 2% (cardiac disease doubled, risk secondary malignancy); para aortic field and ipsi nodes (“dog leg”) 20 Gy in 10 fx; relapse 1-3%
3. Single dose carboplatin: noncompliant patients; equivalent relapse to RT, short term a/e thrombocytopenia and GI toxicity

Question 72

Describe surveillance for IB seminoma post orchiectomy? After RT or chemo?

Answer 72

Orchiectomy:

HPI: 1 year: q3-6 mo, 2-3 year: q6-12 mo, 4-5 year: 1 x year

A/P CT: at 3, 6, 12 mo, 2-3 year q 6-12 mo, 4-5 year: q 12-24 mo

CXR: if clinically indicated, sxs consider CT

Chemo/RT

HPI: 1-2 year: q6-12 mo, 3-5 year 1 x year

A/P CT: 1-3 year: q1 x year, 4-5 year not indicated

CXR: if clinically indicated, sxs consider CT

Question 73

Tx of IIA seminoma? And IIB?

Answer 73

IIA:

Traditional (preferred): EBRT to para-aortic and ipsi iliac PLN → 30 Gy

OR

Primary chemotherapy: EP x 4 or BEP x 3 for multiple positive LN

IIB:

Preferred: Primary chemotherapy: EP x 4 or BEP x 3

RT in non-bulky cases include para-aortic and ipsi iliac LN → 36 Gy

Question 74

For stage IIC or III seminoma what determines tx?

Answer 74

Risk factors

Good risk: any primary site, no non-pulm visceral mets, normal AFP, any hCG or LDH

Intermediate risk: any primary site, non-pulmonary visceral mets, normal AFP, any hCG or LDH

Poor risk: no seminoma is poor risk

Question 75

Treatment for good risk IIC or III seminoma? intermediate risk?

Answer 75

Good risk: Primary chemo EP x 4 or BEP x 3

Intermediate risk: BEP x 4 or VIP x 4 or clinical trial

Question 76

How do you manage post-chemo residual mass for seminoma?

Answer 76

Likely fibrosis or necrosis

< 3 cm → surveillance

>3 cm → PET scan > 6 weeks after chemo, if + RPLND or chemo (conventional dose VeIP or TIP, or high dose chemo)

Question 77

risk factors for testicular carcinoma?

Answer 77

gonadal dysgenesis

h/o prior testis tumor

CIS or intraepithelial germ cell neoplasia

UDT (intra-abd → seminoma, inguinal after pexy → NSGCT)

HIV

FHx

Infertility with Klinefelter’s

Hypospadias

Question 78

Name primary GCT (relative frequency) and non-GCT?

Answer 78

Primary Germ Cell Tumors: seminoma (60%), embryonal carcinoma (20%), teratocarcinoma (15%), teratoma (5%), chorio (1%), yolk sac (<1%)

Non Germ Cell Tumors: only 10% malignant, orchiectomy and surveillance: Leydig cell tumor, Sertoli cell tumor

Question 79

Describe path of testicular carcinoma spread?

Answer 79

Primarily via Lymphatics

RP node mets → cisterna chyli → thoracic duct → supra-diaphragmatic nodes → extra-nodal/distant mets

**exception is chorio or yolk sac which can demonstrate hematogenous spread

Question 80

Describe nodal spread pattern for right testis tumor? left testis tumor?

Answer 80

Right: Interaortocaval → precaval → preaortic → right common iliac → right external iliac

Left: paraaortic → preaortic → left common iliac → interaortocaval → precaval → paracaval

*lymphatic spread goes from right to left in RP

Question 81

What are treatment options for stage IB NSGCT?

Answer 81

1. Surveillance (only pT2)
   
   1. Patient needs to be very compliant with rigorous surveillance
   2. >50% embryonal may increase risk of relapse and make surveillance inferior to tx
   3. LVI most important factor to predict occult mets
   4. SWENOTECA trial, all men stage I NSGCT no LVI underwent surveillance, BPE x 1, or BEP x 2, recurrence 12%, 1%, 0%
2. Chemo
   
   1. 1 cycle BEP or 2 cycles (teratoma resistant, risk of infertility, secondary cancer, cardiac dz)
3. NS-RPLND (appropriate for stage I and IIA

Question 82

Risk of teratoma at RPLND? if in orchiectomy and if not?

Answer 82

In orchiectomy: 2-19%

Not in orchiectomy: 5-7%

Question 83

What are the types of RPLND? Templates?

Answer 83

1. Standard: includes full b/l dissection from above the RV to below aortic bifurcation, anejaculation approached 100% since sympathetic ganglia were sacrificed
   
   1. Superior: L adrenal, renal veins, below SMA
   2. Inferior: aortic bifurcation, IMA is sacrificed
   3. Medial: to contralateral ureter
   4. Lateral: renal hilum, ureter, iliac bifurcation
2. Limited: area overlying aorta below IMA spared, most post-ganglionic sympathetics preserved, ejaculation 80-90% pts
   
   1. Superior: L adrenal, renal veins, below SMA
   2. Inferior: above IMA (IMA spared)
   3. Medial: lateral to aorta
   4. Lateral: renal hilum, ureter, iliac bifurcation
3. NS-RPLND: preserves branches sympathetic chain over aorta, 100% ejaculation; not usually recommended for grossly pos nodes, usually performed in combo with limited dissection

Question 84

What percentage of IB are upstaged to stage II on RPLND?

Answer 84

30%

Question 85

If LN are grossly positive on RPNLD (stage IIB: >2 cm < 5 cm) what intraoperative template adjustment is made?

Answer 85

bilateral suprahilar dissections extending 4-6 cm above renal arteries to expose crura of diaphragm, IMV ligated, SMA identified and preserved, cisterna chyli is clipped

Superior: first hepatic vein (IVC)

Inferiorly: renal arteries

Laterally: medial aspect of adrenal glands

If nodes + near IMA → extend to lower aorta and contralateral common iliac (retrograde lymph spread)

If nodes + superior to IMA → lower aorta preserved

Question 86

Potential complications of RPLND?

Answer 86

1. IVC laceration: proximal and distal control, oversew with 4-0 Prolene, hold pressure, if cannot control, consult vascular
2. IMA injury: ligate if necessary since collateral circulation (marginal artery of Drummond)
   
   1. IMA supplies distal half of transverse colon, descending colon, sigmoid, and rectum
   2. SMA supplies proximal half of transverse colon, ascending colon, and small bowel
3. Cisterna Chyle laceration: located right of L1-L2, ligate if recognized intraop, unrecognized will result in chylous ascites
   
   1. Dx by paracentesis, NPO, TPN or low fat, high protein, medium chain triglycerides diet, possible somatostatin analogues

Question 87

NSGCT stage IA, IB without risk factors, IIA, IIB treated with primary RPLND, what is tx for various nodal stages?

Answer 87

N0 → surveillance

N1 → surveillance (preferred) or chemotherapy (EP x 2)

N2 0→ chemotherapy (preferred - EP x 2) or surveillance

N3 → chemotherapy (BEP x 3 or EP x 4)

Question 88

NSGCT IIA/IIB s/o RPLND, WITHOUT adjuvant chemo surveillance?

Answer 88

H&P and markers: 1 year: q2 mo, 2 year

Question 89

NSGCT IIA/IIB s/o RPLND, WITH adjuvant chemo surveillance?

Answer 89

Question 90

NSGCT Stage I s/p RPLND or chemo, surveillance?

Answer 90

Question 91

NSGCT Stage 1 primary active surveillance w/o risk factors?

Answer 91

Risk factors: LVI, invasion of spermatic cord or scrotum, embryonal

Question 92

NSGCT Stage 1 primary active surveillance w/ risk factors?

Answer 92

Risk factors: LVI, invasion of spermatic cord or scrotum, embryonal

Question 93

NSGCT II/III after complete response to chemo +/- RPLND?

Answer 93

Question 94

What can cause AFP elevation?

Answer 94

hepatoma, pancreas carcinoma, bronchogenic carcinoma

elevated in fetal yolk sac tumor, embryonal, teratocarcinoma

infants < 1 yo

Liver dysfunction (hepatitis, cirrhosis)

Question 95

What can cause bhCG elevation?

Answer 95

chorio, seminoma, teratocarcinoma, embryonal

cross reacts with FSH, LH, TSH

marijuana users

Question 96

What can cause LDH elevation?

Answer 96

seminoma and non-seminoma

Isoenzyme 1 is most useful

monitor treatment when AFP and bhCG normalized

useful for “bulky” seminoma

Question 97

Stage IIC NSGCT, how do you determine the number of chemo cycles?

Answer 97

1. Good risk: treat with EP x 4 or BEP x 3

AFP < 1,000, HCG < 5,000, LDH < 1.5 X N (S0 or S1)

2. Intermediate risk: treat BEP x 4

AFP 1,000-10,000, HCG 5,000-50,000, LDH 1.5-10 x N (S2)

3. High risk: treat BEP x 4 or VIP x 4

AFP > 10,000, HCG >50,000, LDH 10 x N (S3)

Mediastinal primary

Question 98

Potential complications and treatment from RPLND?

Answer 98

1. ARDS → bleomycin → increases w/ increased FIO2 and over-hydration
   
   1. Ventilate patients with RA and do not use FIO2 > 25-30%
   2. Use colloid to crystalloid ratio 2:1
   3. Prefer RBC over crystalloid
2. Mass invades duodenum → perform duodenal resection
3. IMA is encased in tumor → divide IMA as long as marginal artery intact
4. Ureter is encased or invaded by tumor → nephroureterectomy
5. Tumor invades aorta, IVC, lilac vessels → excise and replace affected vessels, perform vascular patch
6. Psoas muscle involved by tumor → resect psoas fascia and affected muscle
7. Tumor thrombus present in IVC below renal veins → ligate vena cava below renal veins, pts will develop temporary lower extremity edema
8. Tumor invades the wall of IVC below the renal veins → legate the vena cava below renal veins, pts will develop temporary lower extremity edema
9. Sigmoid mesentery is adherent to mass → resect the mesentery and mesenteric vessels, make sure the marginal artery and vein remain intact

Question 99

What chemotherapy regimens are used in salvage setting for testicular cancer?

Answer 99

1. VeIP (VP-16, Ifosfamide, Cisplatin) → mesna to protect bladder from Ifosfamide, 30% durable responses
2. TIP (Paclitaxel, Ifosfamide, Cisplatin) → mesna to protect bladder from Ifosfamide, 25% durable responses
3. Gemcitabine/Ifosfamide/Cisplatin → small study reporting 54% response rate
4. High dose chemotherapy → with autologous peripheral blood derived stem cell support, unfavorable prognosis group (incomplete previous response, high markers, high volume, extratesticular primary, late relapse)
   
   1. 2 cycles of high dose Carboplatin plus Etoposide, w/ or w/o Cyclophosphamide (or Ifosfamide) → 20% durable responses

Question 100

Follow up regimen after salvage chemotherapy for testicular cancer?

Answer 100

CXR and markers q3 mo x 2 years, then q6 mo x 3

CT A/P q 6 mo

Question 101

How do you manage post chemotherapy residual mass for NSGCT? Seminoma?

Answer 101

NSGCT → residual mass should be excised as completely as possible if > 1 cm

Markers have to normalize before RPLND, if elevated → further chemotherapy

Seminoma → residual mass > 3 cm and normal markers → PET CT vs. surveillance → Indeterminate → repeat PET 6-8 weeks vs. bx → Positive → RPLND vs. bx

Question 102

If there is mixed pathology seminoma and nonseminoma, how do you treat?

Answer 102

NSGCT recommendations

Question 103

what are primary landing sites for left and right testicular tumors?

Answer 103

Left → para-aortic → preaortic

Right → interaortocaval → precaval → right iliac

Question 104

describe the nerve sparing elements of RPLND? why important?

Answer 104

prevent anejaculation or other ejaculatory dysfunction

ID and preserve sympathetic trunks (L1-4) as they course posterior to the IVC on the right and anterior to aorta on the left, they coalesce just inferior to the IMA at inferior hypogastric plexus

Question 105

What are treatment options for scrotal contamination in testis cancer?

Answer 105

1. Stage 1 pure seminoma → extend RP radiation to include ipsi scrotum and inguinal nodes (risk of azoospermia)
2. Stage 1 NSGCT → widely excise previous scar and spermatic cord at time of RPLND, or separate procedure if no RPLND, perform formal hemiscrotectomy in case of gross contamination but ill not eliminate risk of relapse
3. Advanced dz → tx with full dose platinum chemo → examine inguinal nodes at f/up

**contamination increased recurrence but not OS

Question 106

Which nodal status is chemo indicated for post RPLND Stage IA/B or IIA/B treated with primary RPLND? Which regimens?

Answer 106

Question 107

Follow up post primary RPLND in need of adjuvant chemotherapy?

Answer 107

CXR and markers q3 mo x 2 years, the q 6 mo x 3 years

CT scan q 6 mo

Question 108

Treatments for clinical stage IIA NSGCT with negative markers?

Answer 108

Primary NS-RPLND

OR

Primary chemotherapy EP x 4 or BEP x 3

Question 109

Treatments for clinical stage IIB NSGCT with negative markers?

Answer 109

Question 110

Treatments for clinical stage IIA NSGCT with persistent markers elevation?

Answer 110

Primary chemotherapy → BEP x 3, EP x 4

Question 111

Treatments for clinical stage IIB NSGCT with positive markers?

Answer 111

Primary chemotherapy: BEP x 3, EP x 4

Question 112

Primary chemotherapy for early clinical stages with persistent marker elevation:

Answer 112

Question 113

What is growing teratoma syndrome?

Answer 113

RP masses that contain teratomas enlarge (sometimes quickly) in the face of normal STM. Usually benign, but warrant surgical excision, if left alone may spread and compromise vital organ function (bowel, ureters, vessels) by local invasion

Question 114

Why can testis tumors cause gynecomastia?

Answer 114

NSGCT can produce elevated levels of estradiol

Leydig cell tumors promote peripheral conversion of testosterone to estrogen (but will not cause elevation in STM)

Question 115

What if you remove a testicular tumor in a patient with clinical symptoms (e.g. gynecomastia), elevated STM, and a supraclavicular node, and the pathology shows scar and no active malignancy?

Answer 115

“burned” out testis tumor or extragonadal

Must perform excisional bx or FNA of supraclavicular node

Question 116

Describe risk classification post-orchiectomy for NSGCT and seminoma

Answer 116

Question 117

Post orchiectomy for NSGCT, with NED, with isolated bHCG elevation, what can be the cause?

Answer 117

Elevated LH

Single testicle → low testosterone → anterior pituitary increased LH which has cross reactivity with bhCG

Give testosterone injection and retest (if goes down, no further action)