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Copyright ©2014 Baishideng Publishing Group Inc.
World J Gastroenterol. Jun 28, 2014; 20(24): 7830-7848
Published online Jun 28, 2014. doi: 10.3748/wjg.v20.i24.7830
Table 1 Histomorphologic subtypes of pancreatic cancer related to their genetic/epigenetics and possible prognostic characteristics
Variant (source)MorphologyGenetics/epigeneticsPrognosis
MCWell defined pushing border, syncytial growth pattern, and poorly differentiated cancer cellsGermline or somatic mutations as well as epigenetic silencing by promoter methylation of mismatch repair genes MLH1 and MSH2BetterMC: Overall 2- and 5-yr survival rate of 29% and 13%[23]CC: 2-yr and 5-yr survival rate of 70% and 57%[153]
CCSuspension of well-differentiated cancer cells in extracellular mucin pools (at least 80%)Unknown
ACCombination of glandular and squamous (at least 30%) componentsK-RAS2 mutations, inactivation of CDKN2A/p16, SMAD4/DPC4 and TP53WorseAC/UC: Median survival of 5 mo after resection[154,155]
UCNoncohesive cancer, lacking histological features of differentiationK-RAS2 gene mutations, loss of E-cadherin protein expression (promoter hypermethylation)
Expression of L1CAM, COX2, and EGFR
Subtype with osteoclast-like giant cells shows mutations like noninvasive precursor lesions
Table 2 Activated and deactivated key genes in pancreatic cancer according to hallmark of cancer, frequency as well as to kind of possible genetic and epigenetic alteration
Gene symbol (source)Associated function according the hallmarks of cancer1[35,36]FrequencyType of genetic alterationEvidence for epigenetic regulation (reference)
Activation
K-RAS2[131]a, f, g> 90Point mutation
AKT2[162,163]a, j, g10-20Amplification
BRAF[164]a, b, g5Point mutation
Deactivation
CDKN2A/p16[165]b, d, i95Homozygous deletion, intragenic mutationYes[166]
TP53[167-169]b, d, i, h50-70Intragenic mutation an one allele and loss in the other allele
SMAD4/DPC4[170,171]b, c, f55Homozygous deletion, intragenic mutation
MLH1[23,172]h3-15Heterozygote mutationsYes[34]
BRCA2[173]a7Heterozygote mutations
STK11/LKB1[174]i5Homozygous deletion, intragenic mutation
TGFBR2[175]a, f4Homozygous deletion, homozygous frameshift mutation
MAP2K4[176,177]a2Homozygous deletion, missense mutation
Table 3 Overview of DNA hyper-/hypomethylation involved in pancreatic cancer
DNA modificationMaterial
Gene affectedRef.
Cancer samplesCell linesOther
DNA hyper-methylationp16[166]
RASSF1A[178]
MDFI, hsa-miR-9-1, ZNF415, CNTNAP2, ELOVL4[179]
SOX15[180]
HOP hoemobox (HOPX)[181]
KLF10[182]
hMLH1[183]
miR-34a/b/c[184]
SPARC[185]
FoxE1, NPTX2, CLDN5, P16, TFPI-2, SPARC, ppENK[186]
SFRP[187]
AsPC1, Hs766T, MiaPaCa2, Panc1UCHL1, NPTX2, SARP2, CLDN5, reprimo, LHX1, WNT7A, FOXE1, TJP2, CDH3, ST14[30,159]
AsPC1, BxPC3, CFPAC1, Panc1NPTX2[188]
Panc1, SW1990miR-132[121]
BxPC3, Capan2, CFPAC1, HPACI, HPAFII, MiaPaCa2, Panc1, PL45FOXA1/2[81]
MiaPaCa2ARID1B[189]1
Panc1NPTX2[190]1
AsPC1, BxPC3, Panc1, MIA PaCa-2Dkk3[191]
BXPC3, HPAFII, HPAC, hTERT-HPDE, Panc1Cldn18[192]
BxPC3, CFPAC1, Panc1, SW1990TNFRSF10C[193]
Pancreatic juiceNeuronal pentraxin II (NPTX2)[194]
Pancreatobiliary fluidUCHL1, RUNX3[195]
PanINp16[196]
IPMNsBNIP3, PTCHD2, SOX17, NXPH1, EBF3, SPARC, SARP2, TSLC1, RELN, TFPI2, CLDN5, UCHL1[157,197]
Blood, brush cytologyNPTX2[198,199]
DNA hypo-methylationVAV1[79]
Claudin4, lipocalin2, 14-3-3 sigma, trefoil factor 2, S100A4, mesothelin, prostate stem cell antigen[78]
MUC4[77]
SW1990ABCB1/MDR1, ABCC1/MRP1, ABCG2/BCRP[200]
Table 4 Overview of miRNAs associated with specific targets/functions in pancreatic cancer
miRNA/functionCell linesTarget gene(s)Cellular effectsRef.
Function as oncogene-10aAsPC1, Capan1, Capan2, MiaPaCa2, Panc1, Patu8988T, Patu8988S, Patu8902HOXB1, 3Metastasis ↑[201]
-21AsPC1, BxPC3, Capan1, Capan2, CFPAC1, Hs776T, H48N, KP-1N, KP-2, KP-3, MiaPaCa2, NOR-P1, Panc1, SUIT-2, SW1990HOXA1Invasion ↑[202]
AsPC1, Capan1, Capan2, CFPAC1, H48N, HS766T, KP-1N, KP-2, KP-3, MiaPaCa2, NOR-P1, Panc1, SUIT-2, SW1990Proliferation ↑, invasion ↑, chemoresistance ↑[203]
BxPC3Proliferation ↑[204]
Capan1, HS766T, MiaPaCa2, MPanc96, Panc1, PL45, SW1990PTEN, RECKAfter miRNA inhibition: cell cycle arrest ↑, apoptosis ↑[205]
-132, -212Panc1Rb1Proliferation ↑[206]
-155Capan2, MiaPaCa2, MCF7, MEFs, 293TTP53INP1Apoptosis ↓[207]
-194, -200b, -200c, -429AsPC1, A818, BxPC3, Capan1, Capan2, HPAFII, MiaPaCa2, MPanc96, Panc1, Patu8902, Patu8988T, Patu8988S, PT45, Suit 007, Su.86.86, Sut00281EP300Metastasis ↑[208]
-197AsPC1, Panc1p120 cateninEMT ↑[209]
-210Panc1, MiaPaCa2, SUIT-2Migration ↓, vimentin ↓, snai-1 ↓, membraneous β-catenin ↑[210]
-221Capan1, HS766T, MiaPaCa2, MPanc96, Panc1, PL45, SW1990p27Chemosensitivity ↑[205]
-224, -486AsPC1, A818, BxPC3, Capan1, Capan2, HPAFII, Su 86.86, MPanc96, MiaPaCa2, Panc1, Patu8902, Patu8988T, PT45, Patu8988S, Suit 007, Suit 00281CD40Invasion ↑, metastasis ↑[211]
Function as tumor suppressor-301aBxPC3, Hs766TBimProliferation ↑,[212]
-320cAsPC1, Panc12SMARCC1Chemoresistance ↑[213]
-421SW1990, Panc1DPC4/Smad4Proliferation ↑, colony formation ↑[214]
-491-5pAsPC1, Capan1, MiaPaCa2, SW1990Bcl-XL, TP53Proliferation ↓, apoptosis ↑, STAT3 ↓, PI-3K/Akt ↓[215]
let-7let-7aBxPC3, Capan1, Capan2, human HPNE (human pancreatic nestin-positive) cells MiaPaCa2, Panc1Proliferation ↓, K-RAS ↓, MAPK ↓[216]
AsPC1RASK-RAS ↓, radiosensitivity ↑[217]
-22BxPC3SP1, ESR1Tumourigenesis ↓[218]
-26aSW1990, Panc1HMGA1Proliferation ↓, invasion ↓, migration ↓, apoptosis ↑[219]
-34BxPC3, MiaPaCa2Bcl-2, Notch-1/2Clonogenicity ↓, invasion ↓, apoptosis ↑, cell cycle arrest ↑, chemosensitivity ↑, radiosensitivity ↑, CSC ↓[220]
-34aPanc1Cell cycle arrest ↑, apoptosis ↑, migration ↓, E2F3 ↓, Bcl-2 ↓, c-myc ↓, cyclin D1 ↓[221]
-34bAsPC1, MiaPaCa2Notch-1Proliferation, apoptosis[222]
Smad3Progression in vivo[223]3
-107MiaPaCa2, Panc1CDK6Proliferation ↓[224]
-126AsPC1, BxPC3, KLM-1, MiaPaCa2, Panc1ADAM9Migration ↓, invasion ↓, E-cadherin ↑[225]
-132BxPC3, HPAFII, HPAC, Panc1Proliferation ↓, colony formation ↓, Akt ↓[121]
-143AsPC1, BxPC3, Capan2, HPAFII, MiaPaCa2, Panc1COX-2Proliferation ↓, MEK/MAPK ↓[226]
Panc1ARHGEF1 (GEF1), ARHGEF2 (GEF2), K-RASMigration ↓, invasion ↓, metastasis ↓, E-cadherin ↑[227]
-148aIMIM-PC2CDC25BProliferation ↓, colony formation ↓[228]
-148bAsPC1, BxPC3, MiaPaCa2, Panc1, SW1990AMPKα1Proliferation ↓, apoptosis ↑, cell cycle arrest ↑, invasion ↓, chemosensitivity ↑, tumourigenicity ↓[229]
-150Colo357, HPAF, Panc10.05MUC4Proliferation ↓, clonogenicity ↓, migration ↓, invasion ↓, cellular adhesion ↑[230]
-200AsPC1, BxPC3, Colo357, HPAC, MiaPaCa2, L3.6pl, Panc12EMT ↓ (ZEB1 ↓, slug ↓, vimentin ↓)[231]
-375Proliferation ↓, cell cycle arrest ↑, apoptosis ↑[232]3
-548dPanc1Proliferation ↓, apoptosis ↑, cell cycle arrest ↑[233]
Table 5 Overview of Epigenetic mechanisms - see text for details and references
MechanismEnzymeSubclasses/componentsEffect on target gene expression
DNA (de-) methylationDNMTDNMT1 (methylation maintenance)
DNMT3A and -3B (de novo methylation)
DNA de-methylaseNot known
Histone (de-) acetylationHATe.g., CBP, p300
Histone methylationHDACClass I (HDACs-1-3, -8), class IIa (HDACs-4, -5, -7, -9), class IIb (HDACs-6, -10), class III (SIRT1-7), class IV (HDAC-11)
PcG→ H3-K27-me3PRC1: CBX-2, 4, or 9, PHC-1, 2, or 3, BMI1, RING1A/B or RNF2
→ H3-K27-me3 maintenance
PRC2: EZH2, SUZ12, EED
de novo H3-K27-me3 maintenance
TrxG → H3-K4-me3Several members
Post-transcriptionalmiRNAs2578 mature miRNA (miRBase v20)
Table 6 Trials using epigenetic agents in pancreatic cancer
CompoundCombinationPhaseEndpointClincialTrials.govTreatment
DNMT inhibitors
Azacitidine+ GemcitabineIMTDNCT01167816
AzacitidineIIPFSNCT018458052
DecitabineVarious stages of development for solid tumors3
ZebularinePreclinical
HDAC inhibitors
Vorinostat+ MarizomibIMTDNCT00667082[234]
Vorinostat+ RadiationI/IIMTD, PFSNCT00948688
+ 5-FU
Vorinostat+ RadiationIMTDNCT00983268
+ Capecitabine
Vorinostat+ RadiationI/IIMTDNCT00831493
BelinostatVarious stages of development for solid tumors
EntinostatIMTDNCT00020579[235]
Entinostat13-cis retinoic acidIMTD
Panobinostat+ BortezomibIIPFSNCT01056601[236]1
HAT inhibitors
CurcuminIISurvivalNCT00094445[147]1
Curcumin+ GemcitabineIITTPNCT001928421
Curcumin+ GemcitabineIIINCT004864601
+ Celecoxib
CurcuminIMTD-[237]
Curcumin+ GemcitabineIMTD-[238]
Curcumin+ GemcitabineI/IIMTD-[239]