A New Strategy to Control and Eradicate "Undruggable" Oncogenic K-RAS-Driven Pancreatic Cancer: Molecular Insights and Core Principles Learned from Developmental and Evolutionary Biology.

Van Sciver, Robert E; Lee, Michael P; Lee, Caroline Dasom; Lafever, Alex C; Svyatova, Elizaveta; Kanda, Kevin; Colliver, Amber L; Siewertsz van Reesema, Lauren L; Tang-Tan, Angela M; Zheleva, Vasilena; Bwayi, Monicah N; Bian, Minglei; Schmidt, Rebecca L; Matrisian, Lynn M; Petersen, Gloria M; Tang, Amy H

Van Sciver, Robert E; Lee, Michael P; Lee, Caroline Dasom; Lafever, Alex C; Svyatova, Elizaveta; Kanda, Kevin; Colliver, Amber L; Siewertsz van Reesema, Lauren L; Tang-Tan, Angela M; Zheleva, Vasilena; Bwayi, Monicah N; Bian, Minglei; Schmidt, Rebecca L; Matrisian, Lynn M; Petersen, Gloria M; Tang, Amy H.

Afiliación

Van Sciver RE; Department of Microbiology and Molecular Cell Biology, Leroy T. Canoles Jr. Cancer Research Center, Eastern Virginia Medical School, Norfolk, VA 23507, USA. VanSciRE@EVMS.EDU.
Lee MP; School of Medicine, Eastern Virginia Medical School, Norfolk, VA 23507, USA. LeeMP@EVMS.EDU.
Lee CD; School of Medicine, Eastern Virginia Medical School, Norfolk, VA 23507, USA. LeeDC@EVMS.EDU.
Lafever AC; School of Medicine, Eastern Virginia Medical School, Norfolk, VA 23507, USA. LafeveAC@EVMS.EDU.
Svyatova E; Department of Microbiology and Molecular Cell Biology, Leroy T. Canoles Jr. Cancer Research Center, Eastern Virginia Medical School, Norfolk, VA 23507, USA. SvyatoE@EVMS.EDU.
Kanda K; Department of Microbiology and Molecular Cell Biology, Leroy T. Canoles Jr. Cancer Research Center, Eastern Virginia Medical School, Norfolk, VA 23507, USA. KandaK@EVMS.EDU.
Colliver AL; School of Medicine, Eastern Virginia Medical School, Norfolk, VA 23507, USA. CollieAL@EVMS.EDU.
Siewertsz van Reesema LL; School of Medicine, Eastern Virginia Medical School, Norfolk, VA 23507, USA. SiewerLL@EVMS.EDU.
Tang-Tan AM; Department of Molecular and Cell Biology, University of California at Berkeley, Berkeley, CA 94720, USA. angelatangtan@berkeley.edu.
Zheleva V; Department of Surgery, Eastern Virginia Medical School, Norfolk, VA 23507, USA. vasilena.zheleva@gmail.com.
Bwayi MN; Department of Microbiology and Molecular Cell Biology, Leroy T. Canoles Jr. Cancer Research Center, Eastern Virginia Medical School, Norfolk, VA 23507, USA. Monicah.Bwayi@STJUDE.ORG.
Bian M; Department of Microbiology and Molecular Cell Biology, Leroy T. Canoles Jr. Cancer Research Center, Eastern Virginia Medical School, Norfolk, VA 23507, USA. bianm@yahoo.com.
Schmidt RL; Department of Biology, Upper Iowa University, Fayette, IA 52142, USA. Schmidtr@uiu.edu.
Matrisian LM; Pancreatic Cancer Action Network, 1050 Connecticut Ave NW, Suite 500, Washington, DC 20036, USA. lmatrisian@pancan.org.
Petersen GM; Pancreatic Cancer Action Network, 1500 Rosecrans Ave, Suite 200, Manhattan Beach, CA 90266, USA. lmatrisian@pancan.org.
Tang AH; Department of Health Sciences Research, Mayo Clinic Cancer Center, Mayo Clinic Pancreatic Cancer SPORE, BioBusiness 5-85, 200 First Street SW, Rochester, MN 55905, USA. Petersen.gloria@mayo.edu.

Cancers (Basel) ; 10(5)2018 May 14.

Article en En | MEDLINE | ID: mdl-29757973

ABSTRACT

ABSTRACT

Oncogenic K-RAS mutations are found in virtually all pancreatic cancers, making K-RAS one of the most targeted oncoproteins for drug development in cancer therapies. Despite intense research efforts over the past three decades, oncogenic K-RAS has remained largely "undruggable". Rather than targeting an upstream component of the RAS signaling pathway (i.e., EGFR/HER2) and/or the midstream effector kinases (i.e., RAF/MEK/ERK/PI3K/mTOR), we propose an alternative strategy to control oncogenic K-RAS signal by targeting its most downstream signaling module, Seven-In-Absentia Homolog (SIAH). SIAH E3 ligase controls the signal output of oncogenic K-RAS hyperactivation that drives unchecked cell proliferation, uncontrolled tumor growth, and rapid cancer cell dissemination in human pancreatic cancer. Therefore, SIAH is an ideal therapeutic target as it is an extraordinarily conserved downstream signaling gatekeeper indispensable for proper RAS signaling. Guided by molecular insights and core principles obtained from developmental and evolutionary biology, we propose an anti-SIAH-centered anti-K-RAS strategy as a logical and alternative anticancer strategy to dampen uncontrolled K-RAS hyperactivation and halt tumor growth and metastasis in pancreatic cancer. The clinical utility of developing SIAH as both a tumor-specific and therapy-responsive biomarker, as well as a viable anti-K-RAS drug target, is logically simple and conceptually innovative. SIAH clearly constitutes a major tumor vulnerability and K-RAS signaling bottleneck in pancreatic ductal adenocarcinoma (PDAC). Given the high degree of evolutionary conservation in the K-RAS/SIAH signaling pathway, an anti-SIAH-based anti-PDAC therapy will synergize with covalent K-RAS inhibitors and direct K-RAS targeted initiatives to control and eradicate pancreatic cancer in the future.

Palabras clave

SINA and SIAH family of RING domain E3 ligases; evolutionary conservation; oncogenic K-RAS mutations; oncogenic K-RAS pathway activation; oncogenic K-RAS-driven tumor relapse and metastasis; pancreatic tumor vulnerability; signaling gatekeeper; ubiquitin-mediated proteolysis

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Texto completo: 1 Bases de datos: MEDLINE Idioma: En Revista: Cancers (Basel) Año: 2018 Tipo del documento: Article País de afiliación: Estados Unidos