2006
DOI: 10.1073/pnas.0601273103
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Both p16 Ink4a and the p19 Arf -p53 pathway constrain progression of pancreatic adenocarcinoma in the mouse

Abstract: Activating KRAS mutations and p16 Ink4a inactivation are near universal events in human pancreatic ductal adenocarcinoma (PDAC). In mouse models, Kras G12D initiates formation of premalignant pancreatic ductal lesions, and loss of either Ink4a͞Arf (p16 Ink4a ͞p19 Arf ) or p53 enables their malignant progression. As recent mouse modeling studies have suggested a less prominent role for p16 Ink4a in constraining malignant progression, we sought to assess the pathological and genomic impact of inactivation of p16… Show more

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Cited by 542 publications
(542 citation statements)
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“…These data were confirmed using the CKIH mice (Pdx1-Cre/ LSL-Kras G12D /Ink4a/Arf F/+ ) (Supplementary Figure S2b). Similarly to the original study, 27 CKIH mice developed PDA with a longer latency of 227 days compared with the 66 days of CKI mice (Supplementary Figure S2c; n = 19 and 9, respectively, Po0.0001), and combination with TA mice shortened the latency of CKIH mice from 227 to 169 days for CKIHTA (Figure 1g; n = 9 and 8, respectively, P = 0.035). Altogether, with similar clinical representation across the various PDA models, these data reveal that, as reported for the PDA mouse model carrying a loss of TP53, TAp73 functions as a potent barrier to PDA progression.…”
Section: Resultssupporting
confidence: 75%
See 1 more Smart Citation
“…These data were confirmed using the CKIH mice (Pdx1-Cre/ LSL-Kras G12D /Ink4a/Arf F/+ ) (Supplementary Figure S2b). Similarly to the original study, 27 CKIH mice developed PDA with a longer latency of 227 days compared with the 66 days of CKI mice (Supplementary Figure S2c; n = 19 and 9, respectively, Po0.0001), and combination with TA mice shortened the latency of CKIH mice from 227 to 169 days for CKIHTA (Figure 1g; n = 9 and 8, respectively, P = 0.035). Altogether, with similar clinical representation across the various PDA models, these data reveal that, as reported for the PDA mouse model carrying a loss of TP53, TAp73 functions as a potent barrier to PDA progression.…”
Section: Resultssupporting
confidence: 75%
“…Interestingly, PDA developed in this homozygous-null TAp73 model showed similar histology as well as close progression kinetic to that observed in TP53 − / − background, with a median lethality of 50 days. 27 These data suggest that while both act in limiting PDA development, p53 and TAp73 showed no compensatory activity in this physiological context. These data were confirmed using the CKIH mice (Pdx1-Cre/ LSL-Kras G12D /Ink4a/Arf F/+ ) (Supplementary Figure S2b).…”
Section: Resultsmentioning
confidence: 84%
“…Notably, even introducing a single null Ink4a/Arf allele accelerated Myc-initiated lymphomagenesis, and lymphomas generated in Ink4a/Arf +/-mice invariably were rendered functionally null via LOH, whereas mammary tumors arising in Ink4a/Arf +/-mice in our study routinely retained the wild-type allele. Likewise, both Ras-initiated melanomas (42) and pancreatic cancers (43) are accelerated when either Ink4a/Arf-encoded gene product is deleted, and this is especially so in the setting of combined Ink4a/Arf deficiency. Differences in the transgenes (Wnt vs. Myc/Ras) and/or tissues analyzed in each study may explain the distinct consequences of Ink4a/Arf loss in these models.…”
Section: Discussionmentioning
confidence: 99%
“…Pancreatic carcinomas constitute the paradigm of tumors presenting p16 Ink4a inactivation, with 98% of cases showing a loss of p16 Ink4a function (Moore et al, 2001a, b;Fukushima et al, 2002;Bardeesy et al, 2006). In these tumors, several mechanisms whereby the p16 Ink4a gene is inactivated have been described, including homozygotic deletions, loss of heterozygosity, point mutations and promoter methylation (Herman et al, 1995;Rutter et al, 2003;Paulson et al, 2008;Andujar et al, 2010).…”
Section: Other Functions Attributed To P16 Ink4amentioning
confidence: 99%