Clinical Significance of the Genetic Landscape of Pancreatic Cancer and Implications for Identification of Potential Long-term Survivors

Yachida, Shinichi; White, Catherine M.; Naito, Yoshiki; Zhong, Yi; Brosnan, Jacqueline A.; Macgregor-Das, Anne M.; Morgan, Richard A.; Saunders, Tyler; Laheru, Daniel A.; Herman, Joseph M.; Hruban, Ralph H.; Klein, Alison P.; Jones, Siân; Velculescu, Victor E.; Wolfgang, Christopher L.; Iacobuzio‐Donahue, Christine A.

doi:10.1158/1078-0432.ccr-12-1215

Cited by 237 publications

(226 citation statements)

References 31 publications

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“…These observations should support a genetic progression model of pancreatic carcinogenesis leading to invasive cancer 5, 6, 7, 8, 9, 10. Recently, the estimated lifetime of clonal evolution during PC development and progression based on a computational model using many autopsy cases has been reported 11, 12. This model suggested an average of 11.7 years from the initiating carcinogenesis until development of the parental clone, an average of 6.8 years to the development of metastatic subclones within the primary PC, and an average of 2.7 years until death of the case (Figure 1).…”

Section: Opportunity To Diagnose ‘Early Pancreatic Cancer’mentioning

confidence: 66%

Early diagnosis of pancreatic cancer: Current trends and concerns

Hanada

Amano

Abe

2017

Annals of Gastroent Surgery

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Early detection of pancreatic cancer (PC) is essential for a better prognosis. Some recent studies have demonstrated that a slight dilatation of the main pancreatic duct (MPD) and small cystic lesions were detected initially in most cases diagnosed at an early stage. Detecting these abnormal findings in cases with high risk factors through an effective screening system including image diagnosis, some biological markers, or familial cancer registrations should contribute to early diagnosis of PC. It has been reported that endoscopic ultrasonography (EUS) is essential for detecting tumors <10 mm with a favorable prognosis. Additionally, EUS‐guided fine‐needle aspiration biopsy is useful for confirming final histological diagnosis. For the diagnosis of stage 0 PC, local irregular stenosis of MPD should be an important initial abnormal sign detected by EUS or magnetic resonance cholangiopancreatography. Cytodiagnosis multiple times using pancreatic juice obtained by endoscopic nasopancreatic drainage should be essential for the final diagnosis. Recently, activities of regional networks between specialist doctors in medical centers and general practitioners for early diagnosis of PC have been reported in Japan. In the future, these activities may play an important role in the early diagnosis of PC.

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Section: Opportunity To Diagnose ‘Early Pancreatic Cancer’mentioning

confidence: 66%

Early diagnosis of pancreatic cancer: Current trends and concerns

Hanada

Amano

Abe

2017

Annals of Gastroent Surgery

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“…In particular, the genetic landscape of PDAC is notable for four frequently mutated genes, classifiable as "driver" genes, including K-RAS, TP53, CDKN2A/p16INK4a, and SMAD4/DPC4. These four genes are well recognized as contributing to the carcinogenesis and maintenance of PDAC, and the simultaneous determination of their status provides important information regarding disease progression and survival 16 . DNA extracted from frozen samples was successfully amplified in 100% of all the original human tumors and CAM tumors specimens, for each studied exon.…”

Section: Mutation Analysismentioning

confidence: 99%

“…We used 20 ng of genomic DNA, as template in nested PCR reactions to amplify DNA fragments corresponding to exons 1 and 2 of K-RAS, TP53 exons 5-9, CDKN2A/p16INK4a exons 1 and 2, and DPC4/SMAD4 exons 0-11. The PCR protocol and the sets of primers have been described in detail previously 16,48 . PCR products were purified using a presequencing kit (Amersham Biosciences, Roosendaal, The Netherlands) and sequenced with both forward and reverse primers using the BigDyeTM Terminator v3.1 Cycle Sequencing Kit (Applied Biosystems, Foster City, CA), with the ABI PRISMTM 3100 Genetic analyzer (Applied Biosystems).…”

Section: Mutation Analysismentioning

confidence: 99%

“…Additional IHC studies were performed using antibodies to Cdkn2A (clone E6H4, MTM Laboratories, Heidelberg, Germany), p53 (Bp-53-11, Ventana) and Smad4 (clone B8, Santa Cruz Biotechnology, Santa Cruz, CA) proteins, as reported previously 16 . Nuclear labeling of Cdkn2A was scored as intact (positive, indicating the presence of an intact gene) or lost (negative, indicating a deletion, inactivating mutation or promoter hypermethylation); p53 immunolabeling was considered abnormal when it showed nuclear accumulation of this protein in ≥ 30% of the neoplastic cells compared to adjacent normal cells, or if the neoplastic cells showed a virtual absence of immunolabeling compared to immediately adjacent normal cells suggesting the presence of an intragenic deletion, nonsense or frameshift mutation; nuclear labeling of Smad4 was scored as intact (positive, indicating the presence of an intact gene) or lost (negative, indicating a deletion or inactivating mutation of the gene has occurred).…”

Section: Mutation Analysismentioning

confidence: 99%

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Development of bioluminescent chick chorioallantoic membrane (CAM) models from primary pancreatic cancer cells: A platform for drug testing

León

Rovithi

Avan³

et al. 2017

Pancreatology

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The aim of the present study was to develop chick-embryo chorioallantoic membrane (CAM) bioluminescent tumor models employing low passage cell cultures obtained from primary pancreatic ductal adenocarcinoma (PDAC) cells. Primary PDAC cells transduced with lentivirus expressingFirefly-luciferase (Fluc) were established and inoculated onto the CAM membrane, with >80% engraftment. Fluc signal reliably correlated with tumor growth. Tumor features were evaluated by immunohistochemistry and genetic analyses, including analysis of mutations and mRNA expression of PDAC pivotal genes, as well as microRNA (miRNA) profiling. These studies showed that CAM tumors had histopathological and genetic characteristic comparable to the original tumors. We subsequently tested the modulation of key miRNAs and the activity of gemcitabine and crizotinib on CAM tumors, showing that combination treatment resulted in 63% inhibition of tumor growth as compared to control (p < 0.01). These results were associated with reduced expression of miR-21 and increased expression of miR-155. Our study provides the first evidence that transduced primary PDAC cells can form tumors on the CAM, retaining several histopathological and (epi)genetic characteristics of original tumors. Moreover, our results support the use of these models for drug testing, providing insights on molecular mechanisms underlying antitumor activity of new drugs/combinations.With less than 7% of patients alive five years after diagnosis, pancreatic ductal adenocarcinoma (PDAC) exhibits one of the poorest prognoses of all solid tumors. Despite extensive clinical efforts, the outcome of this malignancy has not improved in the last decade, and PDAC is expected to become the second deadliest cancer, after lung cancer, by 2030 1,2 .Gaining more insight into the mechanisms that delineate tumor progression in PDAC could ultimately provide more successful therapeutic approaches. To this end, genetically engineered mouse models (GEMMs) have provided a powerful tool, developing tumors that recapitulate both the underlying biology and the dense desmoplastic reaction of PDACs. This stromal reaction has been considered for years as one of the mediators of resistance to chemotherapy 3 . However, experimental and clinical evidence demonstrated that anti-stromal approaches may favour PDAC aggressiveness, reinforcing the need to critically revisit the complexity of cancer-stroma interactions for translational and pharmacological implications 4 . Recent studies suggested that early passages of primary PDAC cells and "avatar" mice can mimic the genetic diversity that characterizes the human disease and might be better predictors of drug activity, including the standard treatment with gemcitabine 5,6 .Despite several studies used such in vivo models in order to promote drug development and selection, their costs and complexity impaired the translation of these results in the clinical setting. Novel, cost-effective models that similarly mimic tumor biology and provide faster information on the activ...

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“…Yachida et al [111] demonstrated that among patients with stage I/II disease who had two driver gene alterations, the median disease-free and median overall survival was longer. Also, these patients were significantly more likely to develop oligometastatic failure.…”

Section: The Role Of Geneticsmentioning

confidence: 99%

Improving Survival of Pancreatic Cancer. What Have We Learnt?

Singh

Chaudhary

2015

Indian J Surg

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Pancreatic adenocarcinoma still ranks high among cancer-related deaths worldwide. In spite of substantial strides in preoperative staging, surgery, perioperative care, and adjuvant treatment, the survival still remains dismal. A number of patient-, disease-, and surgeon-related factors play a role in deciding the eventual outcome of the patient. The aim of this commentary is to review the current knowledge of various factors and the recent advances that impact the survival of patients with pancreatic adenocarcinoma. A search of scientific literature using Embase and MEDLINE, for the years 1985-2015, was carried out for search terms Bpancreatic cancer^and Bsurvival.^Further search was based on the various specific prognostic factors that contribute towards survival of patients with pancreatic cancer found in the literature. Most of the studies used for this review include those that deal with pancreatic head cancers, some include patients with pancreatic cancers in all locations while very few included patients with tumors of body and tail only. In spite of significant developments in pre-and perioperative management, increased rates of margin-negative resections, and use of adjuvant treatment, the survival rates of pancreatic cancer patients remains poor. A paradigm shift with more effective adjuvant regimen and genetic interventions may help change the outcomes of patients with pancreatic cancer.

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Clinical Significance of the Genetic Landscape of Pancreatic Cancer and Implications for Identification of Potential Long-term Survivors

Cited by 237 publications

References 31 publications

Early diagnosis of pancreatic cancer: Current trends and concerns

Early diagnosis of pancreatic cancer: Current trends and concerns

Development of bioluminescent chick chorioallantoic membrane (CAM) models from primary pancreatic cancer cells: A platform for drug testing

Improving Survival of Pancreatic Cancer. What Have We Learnt?

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