Smoking

Pesticides

Asbestos

periodontal disease

Heavy alcohol consumption {+6 drinks/day}

Elevated BMI {>35}

Low vitamin D

Chronic pancreatitis.

Diabetes Mellitus type II, even prediabetes

New-onset Diabetes

Genetics

Premalignant tumors of the pancreas [mucinous cystic neoplasms, IPMs]

Germline 

BRCA 1,2, PALB2 carrier

ATM

HNPCC

MMR def

CDKN2A/p16

STK11/LKB1 carrier Peutz Jeger syndrome

Li Fraumani

PRSS1 [Heriditary pancreatitis]

FDR

Somatic

KRAS G12D,G12V,G12C..

TP53--mutated >50% of the times

CDKN2A(p16)

SMAD(DPC4)

MLL3

BRCA 2 can occur somatically as well.

MMR/MLH1/MSH2/MSI high 1-2%

Resectable Pancreatic Cancer (10-15%) 

• T1-3,N0-1,M0 • Stage I, IIa, IIb

- Standard of care is upfront surgical resection or neoadjuvant therapy 

- No standard neoadjuvant approach (most centers use gemcitabine nab-paclitaxel or (m)FOLFIRINOX w/wo subsequent CRT, If BRCA 1/2 or PALB2 mutated--gem+cis, (m)FOLFIRINOX w/wo subsequent CRT with cape/FU/or gem with RT

-  (m)FOLFIRINOXfor ECOG 0-1

- Don't do upfront Sx if high-risk features (equivocal or indeterminate imaging findings, markedly elevated CA 19-9, Large primary tumors, large regional LN's, excessive weight loss, extreme pain)

- Multiple options for adjuvant therapy 

- Gemcitabine x 6 months 2007-2016 [m OS 25?35?37? mo)

- Gemcitabine + Capecitabine 2017* [m OS 28 mo)

- mFOLFIRINOX 2018* --m OS 54 months PRODIGE 24 --ECOG 0-1

- Gemcitabine + nab-paclitaxel 2023 ---m OS 40.5 -41.8

Consider chemoradiation after 4-6 months of chemotherapy for patients with R1 resections

Gemcitabine nab-paclitaxel or (m)FOLFIRINOX w/wo subsequent CRT with cape/FU/or gem RT

If BRCA 1/2 or PALB2 mutated--gem+cis, (m)FOLFIRINOX w/wo subsequent CRT with cape/FU/or gem with RT.

--> Standard of care is chemotherapy with options dependent on performance status: 

 Gemcitabine/nab-p, (m) FOLFIRINOX, NALIRIFOX

BRCA1/2, PALB2 mutations- (m) FOLFIRINOX, gem+cis

--> Int PS 2--include gem, Cape, gem+abraxane

--> Poor PS 3-- gem, FU, cape

--> Delivering radiation after induction chemotherapy does not improve median survival over chemotherapy alone but does improve PFS • At 5 years, the survival rate is higher for those undergoing radiation (10% vs 4%)  

Targeted therapies, CPI for TMP>=10 can be considered in certain circumstances.

• Gemcitabine/nab-paclitaxel for KPS > 70% 

• nal-IRIFOX superior to Gem/nab-p*

• FOLFIRINOX reserved for patients with PS 0-1 

OS same 11.1 mo with nal-IRIFOX and FOLFIRINOX 

--> Int PS 2--include gem, Cape, gem+abraxane, FOLFOX, CAPOX

--> Poor PS 3--BSC

 • Performance status is clearly linked to survival 

• Combination therapy in poor PS patients appears to be detrimental

Targeted therapies, CPI for TMP>=10 can be considered in certain circumstances.

--> CT/MRI dedicated Pancreatic protocol

--> Endoscopic Ultrasound* • Tissue acquisition for localized disease*

--> Image-guided biopsy of accessible metastatic site

--> ERCP +/- stent in setting of jaundice 

NCCN Guidelines for Pancreatic Adenocarcinoma recommend that clinicians consider germline testing for all patients with pancreatic cancer and molecular analysis for those with metastatic disease

Staging Studies

--> Thin Cut (3mm) abdominopelvic CT Scan - Clear Demonstration of Relationship of Tumor to Portal Vein, SMV, SMA - Potential to Demonstrate Metastatic Disease to Liver or Peritoneum - Image Lung Bases [if regular CT was done before]

• Serum tumor markers – CA 19-9 (10% of patients are non-producers) – CEA – CA 125 

• CT scan of the chest 

• Laparoscopy – Limited to Special Cases --do it for clearly resectable tumors.

* PET imaging is not routinely recommended or approved for pancreatic cancer staging 

 High tumor marker with no CT evidence of metastatic disease 

 Patients who had sx and high tumor marker and you cant tell if it is recurrence (Locally recurrent disease) or just fibrosis in surgical bed.

Multiphase CT scan 

1. Non-Contrast Phase [images right after injecting contrast]

2. Arterial / Late Arterial Phase (a.k.a. Pancreatic Parenchymal Phase) Timing: ~35–50 seconds after IV contrast--You see pancreatic tumors (PDAC appears hypoenhancing). It helps with optimal visualization of arterial anatomy: SMA/ Celiac artery/ Common/proper hepatic artery----Helps assess arterial invasion, which determines resectability

3. Portal Venous Phase Timing: ~60–70 seconds-- Evaluate venous involvement- SMV/ Portal vein/ Splenic vein. It detect liver metastases and lymphadenopathy

4. Optional Delayed Phase (90–120 seconds)

Used for: Characterizing cystic lesions, Evaluating enhancement washout, Checking pancreatic duct strictures or delayed duct filling

You can do multiphase imaging with MRI of the pancreas, and it is commonly done. It is not identical to CT pancreas protocol, but MRI has its own multiphase contrast-enhanced sequences.

CT preferred.

* Simple Contrast CT is single phase (almost always portal venous phase around 60–70 seconds).

ONIVYDE is a topoisomerase inhibitor. [Topoisomerases  relieve DNA supercoiling ]

WARNING: SEVERE NEUTROPENIA and SEVERE DIARRHEA

The most common adverse reactions (≥ 20%) of ONIVYDE: diarrhea, nausea, vomiting, fatigue/asthenia, decreased appetite, stomatitis, and pyrexia. The most common laboratory abnormalities (≥ 10% Grade 3 or 4) were lymphopenia and neutropenia.

--> Interstitial lung disease (ILD)

--> Severe hypersensitivity reaction.

- Recommended dose of ONIVYDE is 70 mg/m2 intravenous infusion over 90 minutes every two weeks. 

- Recommended starting dose of ONIVYDE in patients homozygous for UGT1A1*28 is 50 mg/m2 every two weeks. 

- There is no recommended dose of ONIVYDE for patients with serum bilirubin above the upper limit of normal.

DNA synthesis inhibition

The most common adverse reactions for the single agent (≥20%) are nausea/vomiting, myelosuppression, hepatic transaminitis, proteinuria, fever, hematuria, rash, dyspnea, and peripheral edema.

--> Schedule-dependent toxicity: Increased toxicity with infusion time greater than 60 minutes or dosing more frequently than once weekly.

--> Myelosuppression

--> Pulmonary toxicity and respiratory failure: Discontinue Gemcitabine Injection immediately for unexplained new or worsening dyspnea or evidence of severe pulmonary toxicity

--> Hemolytic-uremic syndrome (HUS): Monitor renal function prior to initiation and during therapy. Discontinue Gemcitabine Injection for HUS or severe renal impairment. (5.4) 

--> Hepatoxicity 

--> Exacerbation of radiationtherapy toxicity: May cause severe and lifethreatening toxicity when administered during or within 7 days of radiation therapy.

--> Capillary leak syndrome: Discontinue Gemcitabine Injection. 

Recommended Dose Reductions for Gemcitabine Injection for Myelosuppression in Pancreatic Cancer and Non-Small Cell Lung Cancer 

ANC ≥ to 1000 and Platelet count and ≥ to 100,000 No dose modifications.

ANC ≥ 500-999 and Platelet count 50 K-99.99k-- 75% of full dose

ANC < 500 and Platelet count < 50,000 Hold 

Metastatic pancreatic with BRCA 1/2 germline mutation who recieved Gem/Cis or FFX x 16 weeks with stable or response--can add olaparib maintainence. 

PFS 7.4 months Olaparib 3.8 months Placebo

18.9 months Olaparib 18.1 months Placebo 

POLO Trial