Ovarian Cancer

Question 1

What are the steps in staging Ovary Cancer?

Answer 1

1) Obtain any free fluid for cytology can examination
2) If no free fluid, obtain Washings by instilling and recovering 50-100mls of saline.
- The fluid should irrigate the cul de sac, parabolic gutters and area beneath each diaphragm
3) Systematically, explore all intra-abdominal organs and surfaces. They should be visualized and palpated
- bowel
- liver
- GB
- diaphragm
- mesentery
- momentum
- entire peritoneum
4) Suspicious areas/adhesions should be biopsied. If there are no suspicious areas, multiple biopsies should be obtained from the peritoneum of the cul-de-sac, paracolic gutters, bladder, and intestinal mesentery
5) Diaphragm should be biopsied/scraped for cytology.
6) Omentum should be resected from the transverse colon
7) Retroperitoneum should be explored to evaluate pelvic LN. Suspicious LN should be removed and sent for frozen section. An ipsilateral dissection may be performed only for unilateral tumor
8) Para-aortic LN should be exposed and enlarged LN removed. Nodes superior to the inferior mesenteric artery should also be resected
9) In the absence of suspicious LN, pelvic and para-aortic LN should be sampled to exclude the possibility of microscopic stage III disease
10) A TAHBSO is performed

Question 2

What are the epithelial ovarian cancers?

Answer 2

= Adenocarcinomas.

They can be subclassified into:

• Serous
• Endometrioid
• Transitional cell (Brenner)
• Mucinous
• Clear Cell
• Mixed epithelial Tumors
• Undifferentiated
• Unclassified

Question 3

What are the risk factors for ovarian CA?

Answer 3

Age (mean age 59yo, decreases after 80yo)
FHx
- single first degree-relative with ovarian CA puts one at 3.6x risk, with lifetime risk of 5%
- BRCA 1 or BRCA 2
- HNPCC (MSH2 24% risk, MLH1 20%, MSH6 1%)
White race
Diet with high animal fat
Nulliparity or 1st birth after 35yo
Involuntary infertility
Late menopause
Early menarche

Question 4

Which subtype of ovarian cancer is strongly a/w endometriosis?

Answer 4

Clear cell

Question 5

Which mutation does clear cell ovarian CA carry in a significant proportion?

Answer 5

ARID1A mutations

Question 6

ARID1A mutations are found in which type of ovarian CA?

Answer 6

Clear Cell

Endometrioid

Question 7

What is a mixed ovarian CA?

Answer 7

Tumor consists of >1 histo type and minor component forms >10%

Question 8

What are the types of Ovarian CA?

Answer 8

Type 1:

• low grade, indolent
• low grade serous, Endometrioid, mucinous, cc, Malignant Brenner
• Mutations of KRAS, BRAF, ERBB2, PTEN, PIK3CA, ARID1A
• relatively genetically stable

Type 2:

• No clear precursor lesion
• High grade, aggressive
• high-grade serous, high-grade Endometrioid, malignant mixed mesodermal tumors (MMMT) and undifferentiated tumor
• freq a/w TP53 mutations

Question 9

What are some of the suspicious morphology on transvaginal US?

Answer 9

L.I.M.A.S

Large lesion
Multi-lobular cysts
Solid papillary projections
Irregular internal septa toons
Ascites

Question 10

What is considered optimal cytoreduction?

Answer 10

No residual tumor measuring >1cm at the end of the surgery

Question 11

What does CRS entail for ovarian CA?

Answer 11

TAHBSO
Pelvic and para-aortic LN sampling
Infra colic omentectomy
Pelvic and peritoneal biopsies
Pelvic and peritoneal Washings 
Appendectomy in case of mucinous histology

Question 12

Is this true? Why?

Neoadj –> surgery is better than CRS –> chemo?

Answer 12

Vergote NEJM 2010

N=632

Aim: to identify if neoadjuvant chemo –> interval debulking was inferior to primary debulking surgery–> chemo

Incl criteria:
- Stage IIIC/IV epithelial ovarian CA, fallopian-tube carcinoma, PPC

Largest residual tumor was 1cm or less in 40% of primary debulked patients, and in 80% with interval debulking
Postop adverse effects and mortality higher after primary debulking

Conclusion–> Neoadj chemo not inferior

Subset analysis:

• initial CRS better for Stage III, lower volume disease
• initial Neoadj chemo better with Stage IV disease

Question 13

Describe the FIGO staging broadly.

Answer 13

I - Tumor confined to ovaries
II - Tumor involves 1 or both ovaries with pelvic extension
III - Tumor involves 1 or both ovaries with microscopically confirmed peritoneal mets outside the pelvis +/- regional LN Mets
IV- Distant mets beyond the peritoneal cavity

Question 14

Describe FIGO stage I

Answer 14

I = Tumor confined to the ovaries

IA = tumor limited to 1 ovary, capsule intact

• no tumor on ovarian surface
• no malignant cells in Ascites/peritoneal Washings

IB = Tumor limited to both ovaries, capsules intact.

• no tumor on ovary surface
• no malignant cells in Ascites/peritoneal Washings

IC: Tumor limited to one or both ovaries, with any of the following:

• Capsule ruptured
• tumor on ovarian surface
• positive malignant cells in the Ascites or positive peritoneal Washings

Question 15

Describe FIGO Stage II

Answer 15

Stage II - Tumor involves 1 or both ovaries with pelvic extension

IIA: extension +/- implants in uterus +/- tubes
- no malignant cells in Ascites or peritoneal Washings

IIB: Extension to other pelvic organ
- no malignant cells in the Ascites or peritoneal Washings

IIC: IIA/B with positive malignant cells in the Ascites or positive peritoneal Washings

Question 16

Describe FIGO Stage III

Answer 16

III = Tumor involves 1 or both ovaries with microscopically confirmed peritoneal mets outside the pelvis +/- regional LN mets

IIIA: microscopic peritoneal mets beyond the pelvis

IIIB: Macroscopic peritoneal mets beyond the pelvis, 2cm or less in greatest dimension

IIIC: Peritoneal mets beyond the pelvis >2cm in greatest dimension +/- regional LN mets

Question 17

What are the trials supporting intraperitoneal chemotherapy?

Answer 17

1) GOG 172 trial by Deborah Armstrong
- NEJM 2006
- RCT Phase 3; n=400
- 2 arms in Stage III Ovarian CA with 1cm or less residual mass:
(I) IV Pac + IV CDDP
(II) IP Pac + IP CDDP; IV Pac
- 40% in IP group completed therapy
- mPFS 18m (IV) vs 24m (IP)
- mOS 50m vs 66m (IP)

2) Meta-analysis by Hess in 2007
- 6 RCTs 1700 patients (ovarian Ca)
- pooled HR for PFS 0.8 and pooled HR for OS 0.8 (both p significant)

3) GOG 104
- IV CDDP/Cyclo vs IP CDDP/IV Cyclo
- 2nd look laparotomy
- pCR 36% vs 47%
- mOS 41m vs 49m

4) GOG 114
- initially 3 arms:
> IV CDDP/IV Cyclo
> IV CDDP/IV Pac
> IV Carbo AUC9/IP CDDP/IVPac
- IV CDDP/Cyclo taken off
- PFS 28m vs 23m (IP better)
- OS 60m vs 50m (IP better)

Question 18

What is the rationale for IP chemotherapy?

Answer 18

1) Major route of spread is within the peritoneal cavity
2) Ability to reduce tumor volume with debulking
3) Residual peritoneal tumor exposed to increased concentration of drug for prolonged period of time

Question 19

What are the limitations of IP chemo?

Answer 19

Poor tumor penetration of bulky disease

Less exposure of extra-peritoneal dz to drug

Question 20

What are the possible complications of IP chemo?

Answer 20

1) Obstruction to flow or inadequate distribution
2) Infection:
- peritonitis
- abdominal wall or catheter
3) Intestinal perforation

Question 21

What are the trials that support dose-dense scheduling in ovarian CA?

Answer 21

1) JGOG 3016
- 2 arms:
(A) IV Pac (180)/IV Carbo (AUC6) q21 days x 6#
(B) IV Pac (80) D1,D8,D15 + IV Carbo (AUC 6) D1 q21d x 6#
- 6yr update
- mOS 60m vs 100m
- mPFS 28m vs 17m

2) MITO 7
- 2 arms:
(A) IV Pac (175)/Carbo AUC6 q21d x 6#
(B) IV Pac (60) + IV Carbo AUC2 D1,8,15 q21d x6#
- 2 yr f/u
- mPFS 17m (A) and 18m (B)
- QOL scores better with dad
- G3/4 and FN rates lower in (B)

Question 22

What is the role of adjuvant chemotherapy for early stage epithelial ovarian cancer?

Answer 22

Cochrane Database by Winter-Roach. 1st published in 2009. 2 updates, latest in 2015
6RCTs (including ICON 1); >1200 patients
>95% with Stage I Ovarian CA
10yr OS HR 0.72
10yr PFS HR 0.67

Effective in prolonging survival in early stage disease. But uncertain benefit in low, and intermediate-risk early stage disease

Question 23

Tell me about ICON5/GOG 182

Answer 23

5-arm study, to evaluate if incorporation of an additional cytotoxic agent improves OS and PFS in advanced epithelial Ovarian Ca and PPC who received Pac/Carbo.

Stage III/IV, n>4000
80% competed 8#

5arms:
A) Pac/Carbo
B) Pac/Carbo/Gem
C) Pac/Carbo/Liposomal Doxorubicin
D) Carbo+Topotecan --> Carbo/Pac
E) Carbo+Gem --> Pac/Carbo

No improvements in PFS/OS

Question 24

What is the role of Docetaxel in the treatment of Ovarian CA?

Answer 24

JNCI 2004, Vasey et al.

2 arms, 6# each:
A) Docetaxel (75)/ Carbo (AUC5)
B) Paclitaxel (175)/ Carbo (AUC5)
Responding patients get 3# more mono therapy Carbo

F/u 2 years
Similar PFS 15m, and OS of 60+%
Docetaxel with less overall and G2 neurotoxicity 10% vs 30%
Docetaxel with greater G3/4 neutropenia 94% vs 84%

Possible alternative

Question 25

What is the role of Liposomal Doxorubicin in ovarian CA?

Answer 25

MITO-2

Stage IC-IV ovarian CA
2 arms:
A) Pac (175)/Carbo AUC 5
B) PLD (30)/Carbo AUC 5

N=820
f/u 3 years
Median PFS 19m vs 17m (PLD vs Pac) p0.6
Median OS 60m vs 50m (PLD vs Pac) p0.3
Similar RR

Question 26

What predicts OS for surgery at 1st relapse?

Answer 26

Need to fulfill 2 out of 3.

1) Complete resection at 1st surgery
2) Good PS
3) Absence of Ascites

Question 27

Tell me about DESKTOP III

Answer 27

Prospective RCT evaluating role of surgery at relapse.

2 arms:
A) Chemo –> Surgery
B) Chemo alone
Choice of chemo is physician -determined

Question 28

What are the DESKTOP trials?

Answer 28

DESKTOP I =
- exploratory study based on retrospective analysis
- n=267
- complete resection was a/w prolonged survival in recurrent ovarian CA
- identified criteria panel: PS, FIGO stage at Dx, residual tumor after primary surgery, absence of Ascites.
> Able to predict complete resection in 80%

DESKTOP 2:
- to verify the DESKTOP I score.

DESKTOP 3:
Not out yet
Prospective RCT evaluating value of surgery at relapse 
2 arms:
- Chemo--> Surgery
- chemo alone 
Choice of chemo is physician dependent

Question 29

What are the trials using Bevacizumab?

Answer 29

Upfront:

• ICON 7
• GOG 218

Recurrent disease:

• OCEANS (platinum-sensitive)
• AURELIA (platinum-resistant)

Question 30

Tell me about ICON 7

Answer 30

N=1500
All stages

2 arms:

• Pac(175)/Carbo (AUC 5 or 6)/Bev (7.5mg/kg) + Bev
• Pac(175)/Carbo (AUC5/6)

Entire population: no significant diff in PFS/OS

High risk:
- PFS 20m vs 16m
- OS 39m vs 34m
High risk: Stage 3c sub optimally debulked; Stage 4, no debulking surgery (total 1/3 of population)

Question 31

Tell me about GOG 218

Answer 31

N=1800
Stage III/IV

3 arms:
(A): Pac(175)/Carbo(AUC6)
(B): Pac(175)/Carbo(AUC6)/Bev(15mg/kg) –> Placebo
(C): Pac (175)/Carbo(AUC6)/Bev (15mg/kg)–>Bev (15mg/kg)

Median PFS: 11m vs 12m vs 15m
Median OS: 41m vs 39m vs 44m

Question 32

What are the other anti-angiogenics that you know about in the treatment of ovarian ca?

Answer 32

Oral TKI

• pazopanib
• cediranib
• Nintedanib

Angiopoeitin inhibitor
- Trebananib

VEGF “Trap”

Question 33

Is there any benefit with Pazopanib?

Answer 33

AGO-OVAR 16 trial

Investigated as a form of maintenance therapy.
Advanced EOC
- 1st line surgery + Chemo, if no PD and tumor Oral Pazopanib 800 mg daily
> Placebo

Primary endpoint PFS favors Pazopanib
- 18m vs 12m HR 0.8
OS data not mature, but no early detrimental effect

Question 34

Tell me about ICON 6

Answer 34

ICON 6 trial tests Cediranib in platinum-sensitive R-EOC

Platinum-sensitive relapsed EOC
TFI >6 months following 1st line

3arms:

• chemo + placebo–> Placebo
• Concurrent chemo+ Cediranib –> placebo
• Concurrent chemo+ Cediranib –> Cediranib

Chemo agents: Platinum/Taxol; Platinum/Gem; Carboplatin

Cediranib maintenance improves PFS by 3months 12.5vs 9.4
Improves O by 2.7m
- 20m vs 18m

Question 35

What other conditions causes raised CA 125?

Answer 35

Ovarian cancer 
- 85% elevated in advanced disease
- 50% elevated in early disease
Breast cancer
Lung cancer
Colon cancer
Pancreatic cancer

Non-malignant conditions:

• endometriosis
• pelvic inflammatory disease
• ovarian cysts

Question 36

When do we consider a colonoscopy +/- OGD in the management of suspected ovarian CA?

Answer 36

Particularly when CA 125/CEA ratio is 25 or less

Question 37

What to do with Stage I ovarian CA patients?

Answer 37

IA/IB Grade 1 = Observe
IA/IB Grade 2 = Observe or IV Taxane/Carbo 3#-6#
IA/IB Grade 3 or clear cell = IV Taxane/Carbo 3#-6#

IC = IV Taxane/Carbo 3#-6#

Question 38

What are the toxicities of IP chemotherapy?

Answer 38

Increased myelosuppression
Renal toxicities
Abdominal pain
Neuropathy
GI toxicities
Metabolic toxicities
Hepatic toxicities

Question 39

What is VEGF expression in ovarian Cancer like?

Answer 39

Often over expressed

A/w poorer prognosis

Question 40

Explain about the following molecular genetics of ovarian cancer.

• TP53
• BAX
• VEGF
• PTEN

Answer 40

1) TP53:
- mutated in ~50% of pts with ovarian cancer

2) BAX:
- pro-apoptotic Gene and overexpression is a/w increased responsiveness to chemotherapy and better prognosis

3) VEGF
- often over expressed and is a/w poor prognosis

4) PTEN
- PTEN and KRAS mutations are more common in mucinous or Endometrioid tumors

Question 41

Majority of inherited disease in the Jewish population is due to one of the 3 founder mutations in BRCA1 and BRCA2. What are they?

Answer 41

185delAG

5382insC

617delT

Question 42

Oral contraceptive use for 5 or more years is a/w what percentage decrease in the incidence of ovarian cancer?

Answer 42

50%

Question 43

Tell me about sex cord-stromal tumors

Answer 43

Granulosa cell tumors most common subtype

They comprise only ~5% of all ovarian neoplasms

Peak incidence >50yo

Granules a cell tumors may secrete estrogen and be a/w endometrial hyperplasia and endometrial ca

Majority Dx in stage I, with 10-yr survival rates of 75%-95%
Late relapses may occur
Patients with advanced-stage dz fare more poorly

Most such patients will be offered chemotherapy, traditionally with BEP or other regimens used in germ cell tumors

Question 44

Explain about the following molecular genetics of ovarian cancer.

• TP53
• BAX
• VEGF
• PTEN

Answer 44

1) TP53:
- mutated in ~50% of pts with ovarian cancer

2) BAX:
- pro-apoptotic Gene and overexpression is a/w increased responsiveness to chemotherapy and better prognosis

3) VEGF
- often over expressed and is a/w poor prognosis

4) PTEN
- PTEN and KRAS mutations are more common in mucinous or Endometrioid tumors

Question 45

What is the OCEANS trial about?

Answer 45

Aim: Tested the efficacy & safety of Bev+Gem/Carbo cf Gem/Carbo in platinum-sensitive recurrent ovarian, primary peritoneal, or Fallopian tube cancer

N=500
2 arms:
A) Gem/Carbo/Bev-->Bev 
- 6-10cycles, then Bev maintenance till PD
- Gem 1000 mg/m2 D1,8; AUC 4 D1 q21d
- Bev 15mg/kg D1
B) Gem/Carbo/Placebo--> Placebo

Median PFS 12m vs 8m
Objective RR 80% vs 60%
Duration of response 10m vs 7m

Sig S/e with Bev:
G3 or higher HTN 17% vs 1%
Proteinuria 9%

Question 46

Tell me about GOG 158

Answer 46

Done by Ozols et al, JCO 2003

Aim: to establish that Pac/Carbo is non-inferior to Pac/CDDP

N=800
Optimally debulked, advanced ovarian CA 
2 arms:
A) CDDP (75)+CI Pac (135) 
B) Carbo (AUC 7.5)+Pac (175) over 3 hours 

A: more common GI, Renal, Metabolic tox, G4 leukopenia
B: More thrombocytopenia

Med PFS: 19m vs 21m
Med OS: 49m vs 57m

Question 47

What is the evidence to suggest that primary chemotherapy is non-inferior to primary surgery?

Answer 47

1) Vergote NEJM 2010
- n= 670
- majority with Stage IIIC or IV
- >5cm in 75% met lesions; >10cm in 60%
- 2 arms:
A) CRS –> Chemo
B) Chemo –> CRS

2) CHORUS study Lancet 2015
- n=550, Stage III/IV ovarian CA
- 2arms:
(1) Primary surgery –> 6# of chemotherapy
(2) 3#chemo –> Surgery –> 3# chemo

Chemo options:
A) Pac (175) + Carbo (AUC 5/6) or
B) alternative Carboplatin combination regimen
C) Carboplatin mono therapy

Med OS 23m in primary surgery group vs 24m in primary chemo group.

HR 0.9 in favor of primary chemo

Conclusion: Survival with primary chemo on-inferior to primary surgery

Criticisms:
- poor surgery quality
» 27% did not receive Bilateral oophrectomy
» 24% did not receive hysterectomy
» more than 80% did not receive upper abdominal surgeries
» median time was 120min surgery time, and optimum cytoreduction achieved only in 40%
- ?pt population. Authors attributed poor surgical outcomes to poor PS/older age

Question 48

How many cycles of chemo can we give before surgery ?

Can we give more than 3? Why.

Answer 48

Bristow et al Gynecologic Oncology 2006

Meta-analysis
Stage III/IV ovarian Ca patients

Mean median OS 24.5m
Each 10% increase in maximal Cytoreduction was a/w 2m increase in median survival time.
Each incremental increase in pre-op chemo cycles was a/w decrease in median survival Time of 4months.

Question 49

What is Unresectable disease for ovarian cancer?

Answer 49

Diffuse and/or deep infiltration of small bowel mesentery
Diffuse carcinomatosis involving stomach and/or large parts of the small/large bowel
Infiltration of duodenum and/or parts of pancreas
Involvement of large vessels of the hepatoduodenal ligament, celiac trunk or behind the ports hepatis
Involvement of liver parenchyma

Question 50

What are the molecular alterations a/w high grade serous and low grade serous ovarian CA?

Answer 50

High grade serous (70% of ovarian CA)

• Chromosomal instability
• p53
• BRCA 1/2

Low grade serous

• BRAF
• KRAS

Question 51

What are the molecular alterations a/w endometrioid ovarian CA?

Answer 51

pTEN
Beta-Catenin
KRAS
ARID1A

Question 52

What are the molecular alterations a/w cc ovarian CA?

Answer 52

ARID1A
HNF1beta
IL6-STAT-HIF
PI3K/AKT/mTOR

Question 53

What are the molecular alterations a/w Mucinous ovarian CA?

Answer 53

KRAS

HER2

Question 54

By how much is one’s risk of ovarian CA lowered by undergoing risk-reducing Salpingo-Oophrectomy, assuming the person is a carrier of BRCA1 or 2 mutations

Answer 54

~80%

- confirmed by meta-analysis of 10 studies

Question 55

Why 6# and not 3# of adjuvant chemotherapy?

Answer 55

1) GOG 157
Chan et al 2010 Gynecol Oncol

N=400
70% with Stage I disease, 30% ccOvarian, 25% endometrioid, 20% serous, 7% Mucinous, 15% others

Results:
- THose with serous tumors had a significantly lower risk of recurrence after 6# cf to 3# HR 0.3 in contrast to non-serous.
==========
2) Jeffrey Bell et al. GOG study.
N=460
Stage IAG3, STage IBG3, cc, IC, completely resected stage II Epithelial ovarian CA
2 arms: 3# vs 6# of IV Pac/Carbo AUC7.5 Q21 days
70% stage I
RESULTS:
- G3/4 neurotoxicity in 2% vs 11% (6#)
- 6# caused more severe anemia and granulocytopenia.
- RR for 6# was 24% lower, HR 0.76,
- 5y RR 20% (6#) vs 25%(3#)
- overall death rate similar

Question 56

Tell me about the GOG 182-ICON5 study

Answer 56

Copeland Gyneol Onco 2003
Bookman et al.

Aim: To improve on the efficacy of standard platinum/Taxanes therapy by incorporating newer cytotoxic agents in sequential doublet and triplet combinations.

Newer agents studied: Gemcitabine, Liposomal doxorubicin, Topotecan

5 groups:

1) Pac/Carbo
2) Pac/Carbo/Gem
3) Pac/Carbo/Doxorubicin Liposomal
4) Carbo/Topotecan –> Carbo/Pac
5) Carbo/Gem –> Pac/Carbo

N>4000

RESULTS:
- no improvements in PFS/OS a/w any experimental regimen

CONCLUSION:
Addition of a 3rd cytotoxic agent did not provide any PFS/OS benefit after optimal/suboptimal cytoreduction

Question 57

What is the evidence for Docetaxel-Carbo = Pac-Carbo?

Answer 57

JNCI 2004 Vasey et al.

N>1000
Stage IC-IV epithelial ovarian/primary peritoneal CA

2 arms, Q21days x6#:

1) Docetaxel (75)/Carboplatin AUC 5
2) Paclitaxel (175)/Carboplatin AUC 5
* In responding patients, additional 3# of Carboplatin alone was permitted. *

RESULTS:
PFS ~15m
2y OS ~65%
RR similar
Docetaxel/Carbo a/w substantially less overall and G2/higher neurotoxicity cf to Pac/Carbo.
Docetaxel/Carbo gives more 3/4 neutopenia

Question 58

What is the MITO-2 about?

Answer 58

Sandro Pignata JCO 2011

Aim: To test if Liposomal Doxorubicin/Carbo was more effective than standard chemotherapy.

Stage IC-IV
N=800

2 arms:
1) Carbo AUC 5/Pac (175)
2) Carbo AUC 5/PLD (30)
Q21days X 6#

RESULTS:
Med PFS 19m vs 17m (Pac/Carbo) (Trend)
Med OS 60m vs 50m (Pac/Carbo) (trend)

Conclusion: Superiority not proven.
Pac/Carbo still remains as first line

Question 59

What is the Calypso trial about?

Answer 59

Wagner BJC 2012

Recurrence of cancer >6/12 after 1st or 2nd line therapy
N=1000

2 arms:
1) Carbo/Doxil
2) Pac/Carb
6 cycles each

RESULTS:
Med survival times 31m (Carbo/Doxil) vs 33m (Carbo/Pac)

Question 60

How is maximal cytoreduction a/w Survival?

Answer 60

Each 10% increase in maximal cytoreduction was a/w 2m increase in median survival time.

Evidence comes from Robert Bristow et al, meta-analysis

Question 61

Tell me about the CHORUS trial

Answer 61

Sean Kehoe et al.
Non-inferiority trial

Stage III/IV ovarian CA. N=550
2 arms:
1) primary surgery –>6#chemo
2) 3# chemo–> surgery–> 3#chemo

Chemo:
Pac (175) /Carbo AUC 5/6; or
Alternative Carboplatin combination; or
Carboplatin monotherapy.

RESULTS:

• med OS 22.5m (Sx first) vs 24m (chemo first)
• G3/4 post-op adverse events and deaths within 28days after surgery were more common in the primary-surgery group.

CONCLUSION:
Survival with primary chemo is non-inferior to primary surgery

Question 62

What are the 3 criteria to predict OS in choosing a patient to op on recurrence.

Answer 62

2 out of 3

1) Complete resection at 1st surgery
2) Good PS
3) Absence of Ascites