A tumor-targeting cRGD-EGFR siRNA conjugate and its anti-tumor effect on glioblastoma <i>in vitro</i> and <i>in vivo</i>

He, Shuai; Cen, Bohong; Liao, Lumin; Wang, Zhen; Qin, Yi; Wu, Zhuomin; Liao, Weitang; Zhang, Zhongyi; Ji, Aimin

doi:10.1080/10717544.2016.1267821

Cited by 42 publications

(35 citation statements)

References 37 publications

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“…Aside from cilengitide, there are a number of αvβ3-targeted strategies in development for GBM, including GLPG0187, a small molecule antagonist of multiple integrins including αvβ3, αvβ5, αvβ6, and α5β1 (Cirkel et al, 2016), as well as approaches that use RGD peptides for αvβ3-targeted delivery of radionuclides (Jin et al, 2017), siRNA (He et al, 2017), and chemotherapy-loaded nanoparticles or nanogels (Chen et al, 2017; Fang et al, 2017). Considering that Glut3 addiction is also a feature of GBM cancer stem cells (Flavahan et al, 2013), targeting this phenotype with an αvβ3 antagonist has the potential to eradicate the most aggressive and drug resistant subpopulation within the tumor.…”

Section: Discussionmentioning

confidence: 99%

Glut3 Addiction Is a Druggable Vulnerability for a Molecularly Defined Subpopulation of Glioblastoma

et al. 2017

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SUMMARY While molecular subtypes of glioblastoma (GBM) are defined using gene expression and mutation profiles, we identify a unique subpopulation based on addiction to the high affinity glucose transporter, Glut3. Although Glut3 is a known driver of a cancer stem cell phenotype, direct targeting is complicated by its expression in neurons. Using established GBM lines and patient-derived stem cells, we identify a subset of tumors within the “Proneural” and “Classical” subtypes that are addicted to aberrant signaling from integrin αvβ3 that activates a PAK4-YAP/TAZ signaling axis to enhance Glut3 expression. This defined subpopulation of GBM is highly sensitive to agents that disrupt this pathway, including the integrin antagonist cilengitide, providing a targeted therapeutic strategy for this unique subset of GBM tumors.

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Section: Discussionmentioning

confidence: 99%

Glut3 Addiction Is a Druggable Vulnerability for a Molecularly Defined Subpopulation of Glioblastoma

et al. 2017

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“…In another recent study, a methoxy-modified EGFR siRNA was conjugated to cyclic arginine-glycine-aspartic acid peptide, which binds to avb3 integrins expressed on U-87 MG glioblastoma cells. Cyclic arginine-glycine-aspartic acid-siEGFR conjugate demonstrated high tumor targeting abilities, which facilitated effective reduction of EGFR mRNA levels in the tumor tissues and significant inhibition of U-87 MG tumor growth (56). Another commonly used strategy for nanocarrier-directed siRNA delivery, in addition to encapsulation and conjugation, is electrostatic complexation.…”

Section: Discussionmentioning

confidence: 99%

Reverting the molecular fingerprint of tumor dormancy as a therapeutic strategy for glioblastoma

et al. 2018

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Glioblastoma is an aggressive and invasive brain malignancy with high mortality rates despite current treatment modalities. In this study, we show that a 7-gene signature, previously found to govern the switch of glioblastomas from dormancy to aggressive tumor growth, correlates with improved overall survival of patients with glioblastoma. Using glioblastoma dormancy models, we validated the role of 2 genes from the signature, thrombospondin-1 ( TSP-1) and epidermal growth factor receptor ( EGFR), as regulators of glioblastoma dormancy and explored their therapeutic potential. EGFR up-regulation was reversed using EGFR small interfering RNA polyplex, antibody, or small-molecule inhibitor. The diminished function of TSP-1 was augmented via a peptidomimetic. The combination of EGFR inhibition and TSP-1 restoration led to enhanced therapeutic efficacy in vitro, in 3-dimensional patient-derived spheroids, and in a subcutaneous human glioblastoma model in vivo. Systemic administration of the combination therapy to mice bearing intracranial murine glioblastoma resulted in marginal therapeutic outcomes, probably due to brain delivery challenges, p53 mutation status, and the aggressive nature of the selected cell line. Nevertheless, this study provides a proof of concept for exploiting regulators of tumor dormancy for glioblastoma therapy. This therapeutic strategy can be exploited for future investigations using a variety of therapeutic entities that manipulate the expression of dormancy-associated genes in glioblastoma as well as in other cancer types.-Tiram, G., Ferber, S., Ofek, P., Eldar-Boock, A., Ben-Shushan, D., Yeini, E., Krivitsky, A., Blatt, R., Almog, N., Henkin, J., Amsalem, O., Yavin, E., Cohen, G., Lazarovici, P., Lee, J. S., Ruppin, E., Milyavsky, M., Grossman, R., Ram, Z., Calderón, M., Haag, R., Satchi-Fainaro, R. Reverting the molecular fingerprint of tumor dormancy as a therapeutic strategy for glioblastoma.

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“…The supernatant liquid left after centrifugation was analyzed spectrophotometrically for myeloperoxidase levels. A comparison of exposed tissue samples readings was done with the control group in order to correlate the results with the release profile of myeloperoxidase levels and their inhibition by the prepared formulations [44].…”

Section: Myeloperoxidase Assaymentioning

confidence: 99%

Efficacy of Concanavalin-A conjugated nanotransfersomal gel of apigenin for enhanced targeted delivery of UV induced skin malignant melanoma

Jangdey

Kaur²,

Saraf

2019

Artificial Cells, Nanomedicine, and Biotechnology

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The aim of present study was to develop the efficient targeting of Concanavalin-A conjugated nanotransfersomal gel to bind directly to melanocytes gel layer against UVB induced skin carcinoma. Carbopol loaded nanotransfersomal gel have prepared by modified rotary evaporation sonication technique & conjugated synthesized by carbodiimide method and they were characterized the morphology, zeta potential, penetration and cell viability. In vitro release studies & skin permeation have determined using Franz diffusion cell and confocal laser scanning microscope (CLSM). The conjugated formulation showed vesicles size, polydispersity index, zeta potential and % conjugation efficiency of 179.0 ± 0.32 nm, 0.197 ± 0.07, 35.1 ± 0.21 mV and 89.73 ± 1.29% respectively. The surface morphology was confirmed by transmission electron microscopy (TEM) and FTIR to make sure the compatibility among its ingredients. Con-A conjugated nanotransfersomal gel showed toxicity on melanoma (A375) in a concentration range of 0.4-2.0 mg/mL, but less toxicity toward HaCaT cells. The MTT assay has analyzed against two different cell lines, to determine their anti-cancer potentials and their targeting ability. Conjugated formulation were found to decrease the cell viability, higher skin targeting efficacy in invitro & in-vivo. Concanavalin conjugated nanotransfersomal gel of apigenin promise an efficient and economic approach for the skin cancer.

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A tumor-targeting cRGD-EGFR siRNA conjugate and its anti-tumor effect on glioblastoma in vitro and in vivo

Cited by 42 publications

References 37 publications

Glut3 Addiction Is a Druggable Vulnerability for a Molecularly Defined Subpopulation of Glioblastoma

Glut3 Addiction Is a Druggable Vulnerability for a Molecularly Defined Subpopulation of Glioblastoma

Reverting the molecular fingerprint of tumor dormancy as a therapeutic strategy for glioblastoma

Efficacy of Concanavalin-A conjugated nanotransfersomal gel of apigenin for enhanced targeted delivery of UV induced skin malignant melanoma

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