Inhibition of group 1 p21‐activated kinases suppresses pancreatic stellate cell activation and increases survival of mice with pancreatic cancer

Yeo, Dannel; Phillips, Phoebe A.; Baldwin, Graham S.; He, Hong; Nikfarjam, Mehrdad

doi:10.1002/ijc.30615

Cited by 33 publications

(27 citation statements)

References 47 publications

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“…Activated PSCs play a pivotal role in the pathologic processes of pancreatic diseases, and inhibition of PSCs activation, or even the transformation of activated PSCs into quiescence PSCs, has been found to be benecial to the treatment of pancreatic cancer and pancreatitis. [18][19][20] The activated PSCs are positive for a-SMA, collagen 1, so this two molecules are oen used as the marker of PSCs activation. 21 As shown in Fig.…”

Section: Inhibition Of Asic1a Suppresses the Activation Of Pscs Inducmentioning

confidence: 99%

Retracted Article: ASIC1a involves acidic microenvironment-induced activation and autophagy of pancreatic stellate cells

Wang

Pan

et al. 2018

RSC Adv.

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Section: Inhibition Of Asic1a Suppresses the Activation Of Pscs Inducmentioning

confidence: 99%

Retracted Article: ASIC1a involves acidic microenvironment-induced activation and autophagy of pancreatic stellate cells

Wang

Pan

et al. 2018

RSC Adv.

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“…α-SMA is an established marker for PSC activation [27], and its expression is negatively correlated with PDA survival [28]. We have previously reported that inhibition of PAK1 decreased proliferation and increased apoptosis of PSCs while suppressing SMA expression in PSCs [12]. Here for the first time we have detected the expression of -SMA by both Western blot and immunofluorescent staining in cells established from xenografts isolated from pancreatic cancer patients.…”

Section: Discussionmentioning

confidence: 83%

“…Inhibition of PAK1 synergistically with gemcitabine reduced the growth of pancreatic cancer cells in vitro and in vivo [10], and activation of PAK1 contributed to gemcitabine resistance of pancreatic cancer cells [11]. Inhibition of PAK1 also suppressed PSC activation and proliferation while promoting apoptosis, and deletion of stromal PAK1 increased survival of mice with PDA [12]. PAK4 promoted PDA cell proliferation and survival by activation of the NF-κB pathway [13], and inhibition of PAK4 increased the sensitivity of PDA cells to gemcitabine [14].…”

Section: Introductionmentioning

confidence: 99%

The PAK Inhibitor PF-3758309 Promotes the Inhibitory Effects of Multiple Chemotherapeutic Reagents on Patient-Derived Pancreatic Cancer Cell Lines

Wang¹,

Huynh²,

Wang³

et al. 2018

Preprint

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Pancreatic ductal adenocarcinoma (PDA) remains the most lethal malignancy due to lack of an effective treatment. P21-activated kinases (PAKs) play key roles in PDA growth, and the PAK inhibitor PF-3758309 synergistically reduced PDA growth with gemcitabine. The aim of this study was to determine the effect of PF-3758309 with multiple chemotherapeutic reagents on a panel of patient-derived PDA cell lines. Cells were treated with PF-3758309 plus or minus gemcitabine, 5-fluorouracil (5-FU) or abraxane, and cell proliferation was determined. Protein expression profiles were measured by Western blot. PDA cells were subcutaneously injected into the flanks of SCID mice which were then treated with PF-3758309, gemcitabine, PF-3758309 plus gemcitabine, or gemcitabine plus abraxane. Tumour growth was measured by volume and weight. PF-3758309 enhanced the inhibitory effects of 5-FU, gemcitabine and abraxane on a panel of patient-derived PDA cells, inhibited HIF-1 protein expression and reduced the protein levels of palladin and -SMA in these cells. The combination of PF-3758309 with gemcitabine maximally inhibited PDA growth in vivo, which was comparable to the combination of gemcitabine with abraxane. PF-3758309 enhanced the suppressive effects of multiple chemotherapeutic reagents on the growth of a panel of patient-derived PDA cell lines. The combination of PF-3758309 with gemcitabine provides a potential treatment option with less toxicity than gemcitabine plus abraxane.

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“…A recent study revealed the role of PAK1 in PSC modulation for the first time by showing that inhibition of PAK1 by FRAX597 (a potent group I PAK inhibitor) reduced the activation and proliferation of PSC and increased apoptosis in vitro . In an orthotopic pancreatic cancer mouse model, survival in the PAK1 knockout group was significantly increased compared to the PAK1 wildtype group, and depletion of PAK1 in the pancreatic stroma also reduced PAK1 expression and activity in the tumour[ 64 ]. Similarly, survival was prolonged in the group treated with FRAX597 plus gemcitabine in the same orthotopic pancreatic cancer model[ 59 ].…”

Section: Pak Signalling In Pancreatic Cancermentioning

confidence: 99%

“…The extensive desmoplastic reaction, which is a hallmark of pancreatic cancer, is reported to result in a dense stroma, deficient vascularization and inefficient drug delivery, eventually leading to chemo-resistance[ 96 , 97 ]. As mentioned above, PAK1 is responsible for PSC activation, leading to stromal fibrosis[ 64 ] in pancreatic cancer similar to its pivotal role in liver fibrogenic pathways[ 98 ].…”

Section: Paks and Chemo-resistance In Pancreatic Cancermentioning

confidence: 99%

p21-activated kinase signalling in pancreatic cancer: New insights into tumour biology and immune modulation

Wang

Baldwin

Nikfarjam

et al. 2018

WJG

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Pancreatic cancer is one of the most aggressive and lethal malignancies worldwide, with a very poor prognosis and a five-year survival rate less than 8%. This dismal outcome is largely due to delayed diagnosis, early distant dissemination and resistance to conventional chemo-therapies. Kras mutation is a well-defined hallmark of pancreatic cancer, with over 95% of cases harbouring Kras mutations that give rise to constitutively active forms of Kras. As important down-stream effectors of Kras, p21-activated kinases (PAKs) are involved in regulating cell proliferation, apoptosis, invasion/migration and chemo-resistance. Immunotherapy is now emerging as a promising treatment modality in the era of personalized anti-cancer therapeutics. In this review, basic knowledge of PAK structure and regulation is briefly summarised and the pivotal role of PAKs in Kras-driven pancreatic cancer is highlighted in terms of tumour biology and chemo-resistance. Finally, the involvement of PAKs in immune modulation in the tumour microenvironment is discussed and the potential advantages of targeting PAKs are explored.

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Inhibition of group 1 p21‐activated kinases suppresses pancreatic stellate cell activation and increases survival of mice with pancreatic cancer

Cited by 33 publications

References 47 publications

Retracted Article: ASIC1a involves acidic microenvironment-induced activation and autophagy of pancreatic stellate cells

Retracted Article: ASIC1a involves acidic microenvironment-induced activation and autophagy of pancreatic stellate cells

The PAK Inhibitor PF-3758309 Promotes the Inhibitory Effects of Multiple Chemotherapeutic Reagents on Patient-Derived Pancreatic Cancer Cell Lines

p21-activated kinase signalling in pancreatic cancer: New insights into tumour biology and immune modulation

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