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Katlanmamış Protein Yanıtı Sinyal Yolunun IRE1α Kolunun Baskılanmasının PANC-1 Pankreatik Duktal Adenokarsinoma Hücrelerinin Tümörijenik Özellikleri Üzerindeki Etkilerinin İncelenmesi

Yıl 2022, , 11 - 18, 11.04.2022
https://doi.org/10.22312/sdusbed.1003140

Öz

Amaç: Pankreas kanseri pankreas dokusundaki hücrelerden orijin alan bir grup malignite olarak ifade edilmektedir. Gelişen bu malignite pankreas duktal adenokarsinomu (PDAC) olarak adlandırılmaktadır. PDAC gelişen hastaların sağ kalım oranları oldukça düşüktür ve dünya genelinde kansere bağlı ölümlerin dördüncü en sık nedenidir. PDAC tümörlerini çevreleyen mikroortamın hipoksik koşulları ve besinden yoksun şartlarının hücrelerde artmış bazal ER stresini uyardığı rapor edilmiştir. Hücrelerde ER stresi yanıtlarını kontrol eden Katlanmamış Protein Yanıtı (UPR) adı verilen ve birincil amacı ER homeostazisini yeniden kurmak olan evrimsel olarak korunmuş bir sinyal iletim yolu geliştirmiştir. Son yıllardaki çalışmalar UPR sinyal yolunun karsinogenez sürecine katkıda bulunduğunu ortaya koymuştur. ER stresi ve UPR aktivitesindeki değişimlerin ovaryum, prostat, meme ve pankreas kanseri de dahil olmak üzere birçok kanser türünün gelişimi ile doğrudan ilişkili olduğu rapor edilmiştir. Çalışmamızda UPR’nin regülasyonunda görev alan üç önemli efektör proteininden biri olan IRE1α’nın seçici bir inhibitörü olan MKC-3946 ile inhibisyonunun PANC-1 hücrelerinin tümörijenik özellikleri üzerindeki etkileri araştırılmıştır.

Materyal-Metot: MKC-3946’ün biyokimyasal etkinliği immünoblotlama ile değerlendirilmiştir. MKC-3946’ün PANC-1 hücrelerinin tümörijenik yeteneği üzerindeki etkileri WST-1 temelli hücre proliferasyon ölçümü, koloni oluşturma tahlili, yara iyileşme tahlili ile incelenmiştir.

Bulgular: MKC-3946 uygulaması PANC-1 hücrelerinin tümörijenik özelliklerini anlamlı düzeyde baskılamıştır.

Sonuç: IRE1α’nın farmakolojik olarak hedeflenmesi, pankreas kanserine yönelik olarak yeni bir terapötik bakış açısı sağlayabilir.

Destekleyen Kurum

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Proje Numarası

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Teşekkür

Teşekkür Bu çalışmadaki bazı analizlerin gerçekleştirilmesinde kullanılan cihazlar ile destek veren Süleyman Demirel Üniversitesi Yenilikçi Teknolojiler Uygulama ve Araştırma Merkezi (YETEM)'ne katkılarından dolayı teşekkür ederiz. Laboratuvarımıza hücre hattı desteğinde bulunan Dr. İbrahim Aydın CANDAN’a teşekkür ederiz.

Kaynakça

  • [1] Sarantis P, Koustas E, Papadimitropoulou A, Papavassiliou AG, Karamouzis M V. Pancreatic ductal adenocarcinoma: Treatment hurdles, tumor microenvironment and immunotherapy. World J Gastrointest Oncol. 2020;12(2):173–81.
  • [2] Kleeff J, Korc M, Apte M, Vecchia CL, Johnson CD, Biankin AV, Neale RE, Tempero M, Tuveson DA, Ralph Hruban H.. Pancreatic cancer. Nat Rev Dis Primers. 2016;2:16022.
  • [3] Ansari D, Gustafsson A, Andersson R. Update on the management of pancreatic cancer: Surgery is not enough. World J Gastroenterol. 2015;21(11):3157–65.
  • [4] Adamska A, Domenichini A, Falasca M. Pancreatic ductal adenocarcinoma: Current and evolving therapies. Int J Mol Sci. 2017;18(7).
  • [5] Mayo SC, Nathan H, Cameron JL, Olino K, Edil BH, Herman JM, et al. Conditional survival in patients with pancreatic ductal adenocarcinoma resected with curative intent. Cancer. 2012;118(10):2674–81.
  • [6] Kong B, Cheng T, Wu W, Regel I, Raulefs S, Friess H, et al. Hypoxia-induced endoplasmic reticulum stress characterizes a necrotic phenotype of pancreatic cancer. Oncotarget. 2015;6(31):32154–60.
  • [7] Hetz C, Zhang K, Kaufman RJ. Mechanisms, regulation and functions of the unfolded protein response. Nat Rev Mol Cell Biol. 2020;21(8):421-438.
  • [8] X-X Li, H-S Zhang, Y-M Xu, R-J Zhang, Y Chen, L Fan, Y-Q Qin, Y Liu ML& JF. Knockdown of IRE1α inhibits colonic tumorigenesis through decreasing β-catenin and IRE1α targeting suppresses colon cancer cells. Oncogene 2017;36:1-9.
  • [9] Adams BM, Oster ME, Herbert DN. Protein quality control in the endoplasmic reticulum. 2019; 38(3):317-329.
  • [10] Zhang K, Kaufman RJ. Signaling the unfolded protein response from the endoplasmic reticulum. J Biol Chem. 2004;279(25):25935–8.
  • [11] Calfon M, Zeng H, Urano F, Till JH, Hubbard SR, Harding HP, Clark SC. IRE1 couples endoplasmic reticulum load to secretory capacity by processing the XBP-1 mRNA. Nature 2002;15:92-96.
  • [12] Hollien J, Weissman JS. Decay of endoplasmic reticulum-localized mRNAs during the unfolded protein response. Science 2006;313(5783):104–7.
  • [13] Heather P. Harding YZ& DR. Protein translation and folding are coupled by an endoplasmic-reticulum-resident kinase. Nature 1999; 397:271-274.
  • [14] Vattem KM, Wek RC. Reinitiation involving upstream ORFs regulates ATF4 mRNA translation in mammalian cells. Proc Natl Acad Sci U S A. 2004;101(31):11269–74.
  • [15] Logue SE, McGrath EP, Cleary P, Greene S, Mnich K, Almanza A, et al. Inhibition of IRE1 RNase activity modulates the tumor cell secretome and enhances response to chemotherapy. Nat Commun 2018;9(1). [16] Talty A, Deegan S, Ljujic M, Mnich K, Naicker SD, Quandt D, et al. Inhibition of IRE1α RNase activity reduces NLRP3 inflammasome assembly and processing of pro-IL1β. Cell Death Dis. 2019;10(9).
  • [17] Dejeans N, Barroso K, Fernandez-Zapico ME, Samali A, Chevet E. Novel roles of the unfolded protein response in the control of tumor development and aggressiveness. Semin Cancer Cell 2015;33:67-73.
  • [18] Papaioannou A, Chevet E. Driving Cancer Tumorigenesis and Metastasis Through UPR Signaling. Top Microbiol Immunol 2018;414:159-192.
  • [19] Siwecka N, Rozpȩdek W, Pytel D, Wawrzynkiewicz A, Dziki A, Dziki Ł, et al. Dual role of endoplasmic reticulum stress-mediated unfolded protein response signaling pathway in carcinogenesis. Int J Mol Sci. 2019;20(18).
  • [20] Erzurumlu Y, Ballar P. Androgen Mediated Regulation of Endoplasmic Reticulum-Associated Degradation and its Effects on Prostate Cancer. Sci Rep 2017;7:1–12.
  • [21] Volkmann K, Lucas JL, Vuga D, Wang X, Brumm D, Stiles C, et al. Potent and selective inhibitors of the inositol-requiring enzyme 1 endoribonuclease. J Biol Chem 2011;286(14):12743–55. [22] Mimura N, Fulciniti M, Gorgun G, Tai YT, Cirstea D, Santo L, Hu Y, Fabre C, Minami J, Ohguchi H, Kiziltepe T, Ikeda H, Kawano Y, French M, Blumenthal M, Tam V, Kertesz NL, Malyankar UM, Hokenson M, Pham T, Zeng Q, Patterson JB, Richardson PG, Munshi NC, Anderson KC. Blockade of XBP1 splicing by inhibition of IRE1α is a promising therapeutic option in multiple myeloma. Blood 2012;119(24):5772-81.
  • [23] Hinshaw DC, Shevde LA. The tumor microenvironment innately modulates cancer progression. Cancer Res. 2019;79(18):4557–67.

Investigation of the Effects of Suppression of the IRE1α Arm of the Unfolded Protein Response Signaling Pathway on Tumorigenic Characteristics of PANC-1 Pancreatic Ductal Adenocarcinoma Cells

Yıl 2022, , 11 - 18, 11.04.2022
https://doi.org/10.22312/sdusbed.1003140

Öz

Objective: Pancreatic cancer is mean as a group of malignancies originating from cells in the pancreatic tissue. This developing malignancy is named pancreatic ductal adenocarcinoma (PDAC). The survival rate of patients who develop PDAC is very low and is the fourth most common cause of cancer-related death worldwide. Hypoxic and nutrient-deprived conditions of the microenvironment surrounding PDAC tumors have been reported to induce increased basal ER stress in cells. Cells are developed an evolutionarily conserved signal transduction pathway called the Unfolded Protein Response (UPR) that controls ER stress responses in cells, which primary purpose is to restore ER homeostasis. Recent studies have revealed that the UPR signaling pathway contributes to the carcinogenesis process. It has been reported that changes in ER stress and UPR activity are directly related to the development of many types of cancer, including ovarian, prostate, breast, and pancreatic cancer. In our study, the effects of inhibition of IRE1α, one of the three important effector proteins involved in the regulation of the UPR, with a selective inhibitor, MKC-3946, on the tumorigenic properties of PANC-1 cells were investigated.

Material-Method: The biochemical efficiency of MKC-3946 was evaluated by immunoblotting. The effects of MKC-3946 on the tumorigenic ability of PANC-1 cells were investigated by WST-1-based cell proliferation measurement, colony formation assay and wound healing assay.

Results: MKC-3946 treatment significantly suppressed the tumorigenic properties of PANC-1 cells.

Conclusion: Pharmacological targeting of the IRE1α in pancreatic cancer may provide a new therapeutic perspective.

Proje Numarası

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Kaynakça

  • [1] Sarantis P, Koustas E, Papadimitropoulou A, Papavassiliou AG, Karamouzis M V. Pancreatic ductal adenocarcinoma: Treatment hurdles, tumor microenvironment and immunotherapy. World J Gastrointest Oncol. 2020;12(2):173–81.
  • [2] Kleeff J, Korc M, Apte M, Vecchia CL, Johnson CD, Biankin AV, Neale RE, Tempero M, Tuveson DA, Ralph Hruban H.. Pancreatic cancer. Nat Rev Dis Primers. 2016;2:16022.
  • [3] Ansari D, Gustafsson A, Andersson R. Update on the management of pancreatic cancer: Surgery is not enough. World J Gastroenterol. 2015;21(11):3157–65.
  • [4] Adamska A, Domenichini A, Falasca M. Pancreatic ductal adenocarcinoma: Current and evolving therapies. Int J Mol Sci. 2017;18(7).
  • [5] Mayo SC, Nathan H, Cameron JL, Olino K, Edil BH, Herman JM, et al. Conditional survival in patients with pancreatic ductal adenocarcinoma resected with curative intent. Cancer. 2012;118(10):2674–81.
  • [6] Kong B, Cheng T, Wu W, Regel I, Raulefs S, Friess H, et al. Hypoxia-induced endoplasmic reticulum stress characterizes a necrotic phenotype of pancreatic cancer. Oncotarget. 2015;6(31):32154–60.
  • [7] Hetz C, Zhang K, Kaufman RJ. Mechanisms, regulation and functions of the unfolded protein response. Nat Rev Mol Cell Biol. 2020;21(8):421-438.
  • [8] X-X Li, H-S Zhang, Y-M Xu, R-J Zhang, Y Chen, L Fan, Y-Q Qin, Y Liu ML& JF. Knockdown of IRE1α inhibits colonic tumorigenesis through decreasing β-catenin and IRE1α targeting suppresses colon cancer cells. Oncogene 2017;36:1-9.
  • [9] Adams BM, Oster ME, Herbert DN. Protein quality control in the endoplasmic reticulum. 2019; 38(3):317-329.
  • [10] Zhang K, Kaufman RJ. Signaling the unfolded protein response from the endoplasmic reticulum. J Biol Chem. 2004;279(25):25935–8.
  • [11] Calfon M, Zeng H, Urano F, Till JH, Hubbard SR, Harding HP, Clark SC. IRE1 couples endoplasmic reticulum load to secretory capacity by processing the XBP-1 mRNA. Nature 2002;15:92-96.
  • [12] Hollien J, Weissman JS. Decay of endoplasmic reticulum-localized mRNAs during the unfolded protein response. Science 2006;313(5783):104–7.
  • [13] Heather P. Harding YZ& DR. Protein translation and folding are coupled by an endoplasmic-reticulum-resident kinase. Nature 1999; 397:271-274.
  • [14] Vattem KM, Wek RC. Reinitiation involving upstream ORFs regulates ATF4 mRNA translation in mammalian cells. Proc Natl Acad Sci U S A. 2004;101(31):11269–74.
  • [15] Logue SE, McGrath EP, Cleary P, Greene S, Mnich K, Almanza A, et al. Inhibition of IRE1 RNase activity modulates the tumor cell secretome and enhances response to chemotherapy. Nat Commun 2018;9(1). [16] Talty A, Deegan S, Ljujic M, Mnich K, Naicker SD, Quandt D, et al. Inhibition of IRE1α RNase activity reduces NLRP3 inflammasome assembly and processing of pro-IL1β. Cell Death Dis. 2019;10(9).
  • [17] Dejeans N, Barroso K, Fernandez-Zapico ME, Samali A, Chevet E. Novel roles of the unfolded protein response in the control of tumor development and aggressiveness. Semin Cancer Cell 2015;33:67-73.
  • [18] Papaioannou A, Chevet E. Driving Cancer Tumorigenesis and Metastasis Through UPR Signaling. Top Microbiol Immunol 2018;414:159-192.
  • [19] Siwecka N, Rozpȩdek W, Pytel D, Wawrzynkiewicz A, Dziki A, Dziki Ł, et al. Dual role of endoplasmic reticulum stress-mediated unfolded protein response signaling pathway in carcinogenesis. Int J Mol Sci. 2019;20(18).
  • [20] Erzurumlu Y, Ballar P. Androgen Mediated Regulation of Endoplasmic Reticulum-Associated Degradation and its Effects on Prostate Cancer. Sci Rep 2017;7:1–12.
  • [21] Volkmann K, Lucas JL, Vuga D, Wang X, Brumm D, Stiles C, et al. Potent and selective inhibitors of the inositol-requiring enzyme 1 endoribonuclease. J Biol Chem 2011;286(14):12743–55. [22] Mimura N, Fulciniti M, Gorgun G, Tai YT, Cirstea D, Santo L, Hu Y, Fabre C, Minami J, Ohguchi H, Kiziltepe T, Ikeda H, Kawano Y, French M, Blumenthal M, Tam V, Kertesz NL, Malyankar UM, Hokenson M, Pham T, Zeng Q, Patterson JB, Richardson PG, Munshi NC, Anderson KC. Blockade of XBP1 splicing by inhibition of IRE1α is a promising therapeutic option in multiple myeloma. Blood 2012;119(24):5772-81.
  • [23] Hinshaw DC, Shevde LA. The tumor microenvironment innately modulates cancer progression. Cancer Res. 2019;79(18):4557–67.
Toplam 21 adet kaynakça vardır.

Ayrıntılar

Birincil Dil Türkçe
Konular Sağlık Kurumları Yönetimi
Bölüm Araştırma Makaleleri
Yazarlar

Yalçın Erzurumlu 0000-0001-6835-4436

Proje Numarası -
Yayımlanma Tarihi 11 Nisan 2022
Gönderilme Tarihi 1 Ekim 2021
Yayımlandığı Sayı Yıl 2022

Kaynak Göster

Vancouver Erzurumlu Y. Katlanmamış Protein Yanıtı Sinyal Yolunun IRE1α Kolunun Baskılanmasının PANC-1 Pankreatik Duktal Adenokarsinoma Hücrelerinin Tümörijenik Özellikleri Üzerindeki Etkilerinin İncelenmesi. Süleyman Demirel Üniversitesi Sağlık Bilimleri Dergisi. 2022;13(1):11-8.

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