GRP78 haploinsufficiency suppresses acinar-to-ductal metaplasia, signaling, and mutant
            <i>Kras</i>
            -driven pancreatic tumorigenesis in mice

Shen, Jiang-Cheng; Ha, Dat P.; Zhu, Genyuan; Rangel, Daisy F.; Kobielak, Agnieszka; Gill, Parkash S.; Groshen, Susan; Dubeau, Louis; Lee, Amy

doi:10.1073/pnas.1616060114

Cited by 40 publications

(28 citation statements)

References 64 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Furthermore, targeted heterozygous knockout of Grp78 in bone marrow suppressed blast numbers without affecting normal hematopoiesis (46). Recently, using the Pdx1 Cre -Ras G12D/þ -P53 fl/þ model for pancreatic ductal carcinoma, it was shown that epithelium-specific heterozygosity of Grp78 resulted in reduced tumorigenesis and increased survival of mice (47). Pancreatic ductal cells are known for their large translational capacity and dependence on the ER and thus on Grp78 levels.…”

Section: Discussionmentioning

confidence: 99%

Heterozygosity of Chaperone Grp78 Reduces Intestinal Stem Cell Regeneration Potential and Protects against Adenoma Formation

et al. 2018

Self Cite

View full text Add to dashboard Cite

Deletion of endoplasmic reticulum resident chaperone Grp78 results in activation of the unfolded protein response and causes rapid depletion of the entire intestinal epithelium. Whether modest reduction of Grp78 may affect stem cell fate without compromising intestinal integrity remains unknown. Here, we employ a model of epithelial-specific, heterozygous deletion by use of mice and organoids. We examine models of irradiation and tumorigenesis, both and Although we observed no phenotypic changes in heterozygous mice, heterozygous organoid growth was markedly reduced. Irradiation of heterozygous mice resulted in less frequent regeneration of crypts compared with nonrecombined (wild-type) mice, exposing reduced capacity for self-renewal upon genotoxic insult. We crossed mice to-mutant animals for adenoma studies and found that adenomagenesis in heterozygous- heterozygous mice was reduced compared with heterozygous controls (1.43 vs. 3.33; < 0.01). In conclusion, epithelium-specific heterozygosity compromises epithelial fitness under conditions requiring expansive growth such as adenomagenesis or regeneration after γ-irradiation. These results suggest that Grp78 may be a therapeutic target in prevention of intestinal neoplasms without affecting normal tissue. Heterozygous disruption of chaperone protein Grp78 reduces tissue regeneration and expansive growth and protects from tumor formation without affecting intestinal homeostasis. .

show abstract

Section: Discussionmentioning

confidence: 99%

Heterozygosity of Chaperone Grp78 Reduces Intestinal Stem Cell Regeneration Potential and Protects against Adenoma Formation

et al. 2018

Self Cite

View full text Add to dashboard Cite

show abstract

“…PKC mice showed detectable PDAC by 3 months and rapid subsequent tumor growth, associating with upregulation of Grp78 and the phosphorylated form of eukaryotic translation initiation factor 2 a (eIF2a) in the ductal cells, indicative of ER stress. 5 While homozygous knockout of Grp78 in the pancreas led to extensive fat infiltration and poorly developed acinar cells, heterozygous Grp78 knockout with 50% reduction in Grp78 level had no effect on pancreas development and function; thus, it is well suited for studying the role of Grp78 in PDAC and it also more closely mimics what can be achieved in the clinic with therapeutic agents.…”

Section: Role Of Grp78 In Pdac and Admmentioning

confidence: 99%

“…Through creation of the PKC78 C/¡ (Pdx-Cre;Kras G12D/C ; p53 C/¡ ;Grp78 C/¡ ) model, we established that Grp78 haploinsufficiency in the pancreas is sufficient to reduce proliferation, suppress activation of Akt, ribosomal protein S6 (S6), extracellular regulated MAP kinase (Erk), and signal transducer and activator of transcription 3 (Stat3), delay tumor growth and significantly prolong survival. 5 Previous studies have shown that acinar cells expressing mutant Kras G12D are induced to transdifferentiate through the process of ADM recently recognized as a key tumor initiation event of PDAC. 1 Importantly, we discovered that PKC78 C/¡ pancreata exhibited reduced ADM, as well as deficient ADM in acinar cells isolated from the heterozygous Grp78 pancreas in response to transforming growth factor a (TGFa) stimulation.…”

Section: Role Of Grp78 In Pdac and Admmentioning

confidence: 99%

“…7,8 Our mouse models revealed that Grp78 haploinsufficiency in acinar cells reduced Egfr expression and hampered the activation of Erk, Akt, Stat3 and b-catenin signaling in the PKC model. 5 It is possible that GRP78 is needed for processing or stabilizing of EGFR and various client proteins required for kinase signaling facilitating ADM. As an essential chaperone, GRP78 may also be needed for the reprogramming of the repertoire of proteins from the acinar into ductal cell signature.…”

Section: Potential Grp Regulatory Mechanisms On Metaplasiamentioning

confidence: 99%

See 1 more Smart Citation

New role of endoplasmic reticulum chaperones in regulating metaplasia during tumorigenesis

Shen

Rangel

et al. 2017

Molecular & Cellular Oncology

Self Cite

View full text Add to dashboard Cite

Metaplasia is emerging as a key process in tumorigenesis. We discovered that 2 essential endoplasmic reticulum (ER) chaperones, 78-kilodalton glucose-regulated protein (GRP78) and 94-kilodalton glucose-regulated protein (GRP94) have a role in metaplasia. Grp78 haploinsufficiency in the mouse pancreas impairs acinar-to-ductal metaplasia, whereas in the uterus, Grp94 loss induces squamous cell metaplasia; both resulting in tumor suppression.

show abstract

“…To survive the pressure created by the tumor microenvironment, including hypoxia and nutrient deprivation, tumor cells utilize the UPR pathways (Avril et al ., 2017; Chevet et al ., 2015; Lee, 2007; Ma and Hendershot, 2004). Multiple components of the UPR have been linked to advanced tumor stage and chemoresistance in cancer (Lee, 2014; Roller and Maddalo, 2013; Shen et al ., 2017; Wang and Kaufman, 2014). For example, overexpression of PDIA5 in chronic myeloid leukemia shows increased resistance to imatinib (Chevet et al ., 2015).…”

Section: Introductionmentioning

confidence: 99%

GRP78‐mediated antioxidant response and ABC transporter activity confers chemoresistance to pancreatic cancer cells

et al. 2018

View full text Add to dashboard Cite

Chemoresistance is a major therapeutic challenge that plays a role in the poor statistical outcomes in pancreatic cancer. Unfolded protein response (UPR) is one of the homeostasis mechanisms in cancer cells that have been correlated with chemoresistance in a number of cancers including pancreatic cancer. In this study, we show that modulating glucose regulatory protein 78 (GRP78), the master regulator of the UPR, can have a profound effect on multiple pathways that mediate chemoresistance. Our study showed for the first time that silencing GRP78 can diminish efflux activity of ATP‐binding cassette (ABC) transporters, and it can decrease the antioxidant response resulting in an accumulation of reactive oxygen species (ROS). We also show that these effects can be mediated by the activity of specificity protein 1 (SP1), a transcription factor overexpressed in pancreatic cancer. Thus, inhibition of SP1 negatively affects the UPR, deregulates the antioxidant response of NRF2, as well as ABC transporter activity by inhibiting GRP78‐mediated ER homeostasis. Sp1 and NRF2 have been classified as nononcogene addiction genes and thus are imperative to understanding the molecular mechanism of resistance. These finding have huge clinical relevance as both Sp1 and GRP78 are overexpressed in pancreatic cancer patients and increased expression of these proteins is indicative of poor prognosis. Understanding how these proteins may regulate chemoresistance phenotype of this aggressive cancer may pave the way for development of efficacious therapy for this devastating disease.

show abstract

GRP78 haploinsufficiency suppresses acinar-to-ductal metaplasia, signaling, and mutant Kras -driven pancreatic tumorigenesis in mice

Cited by 40 publications

References 64 publications

Heterozygosity of Chaperone Grp78 Reduces Intestinal Stem Cell Regeneration Potential and Protects against Adenoma Formation

Heterozygosity of Chaperone Grp78 Reduces Intestinal Stem Cell Regeneration Potential and Protects against Adenoma Formation

New role of endoplasmic reticulum chaperones in regulating metaplasia during tumorigenesis

GRP78‐mediated antioxidant response and ABC transporter activity confers chemoresistance to pancreatic cancer cells

Contact Info

Product

Resources

About