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Neuropilin-1 is over-expressed in claudin-low breast cancer and promotes tumor progression through acquisition of stem cell characteristics and RAS/MAPK pathway activation
by
Volpert, Marianna
, Hollier, Brett G.
, Rockstroh, Anja
, Thompson, Erik W.
, Lehman, Melanie
, Tang, Yu Hin
, Sokolowski, Kamil A.
, Gregory, Philip A.
, Nelson, Colleen C.
, Lynam, Layla-Rose
in
Animal models
/ Animals
/ Biomedical and Life Sciences
/ Biomedicine
/ Breast cancer
/ Breast Neoplasms - metabolism
/ Cancer Research
/ Cancer stem cells
/ Cancer therapies
/ Cell Line, Tumor
/ Cell proliferation
/ Cell Proliferation - genetics
/ Cell surface
/ Chemotherapy
/ Claudin-low
/ Claudins - metabolism
/ Development and progression
/ Female
/ Gene expression
/ Genomes
/ Humans
/ Kinases
/ MAP kinase
/ MAP Kinase Signaling System
/ Medical prognosis
/ Mesenchyme
/ Metastases
/ Metastasis
/ Mice
/ Monoclonal antibodies
/ Neoplasm Recurrence, Local
/ Neuropilin
/ Neuropilin-1 - genetics
/ Neuropilin-1 - therapeutic use
/ Oncology
/ Phenotypes
/ Prognosis
/ Protein arrays
/ Proteins
/ Ras protein
/ ras Proteins
/ Research Article
/ Signal transduction
/ siRNA
/ Software
/ Stem cells
/ Stem Cells - metabolism
/ Surgical Oncology
/ Survival analysis
/ Transcriptomics
/ Triple Negative Breast Neoplasms - pathology
/ Triple-negative breast cancer
/ Tumors
/ Western blotting
/ Xenografts
2022
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Neuropilin-1 is over-expressed in claudin-low breast cancer and promotes tumor progression through acquisition of stem cell characteristics and RAS/MAPK pathway activation
by
Volpert, Marianna
, Hollier, Brett G.
, Rockstroh, Anja
, Thompson, Erik W.
, Lehman, Melanie
, Tang, Yu Hin
, Sokolowski, Kamil A.
, Gregory, Philip A.
, Nelson, Colleen C.
, Lynam, Layla-Rose
in
Animal models
/ Animals
/ Biomedical and Life Sciences
/ Biomedicine
/ Breast cancer
/ Breast Neoplasms - metabolism
/ Cancer Research
/ Cancer stem cells
/ Cancer therapies
/ Cell Line, Tumor
/ Cell proliferation
/ Cell Proliferation - genetics
/ Cell surface
/ Chemotherapy
/ Claudin-low
/ Claudins - metabolism
/ Development and progression
/ Female
/ Gene expression
/ Genomes
/ Humans
/ Kinases
/ MAP kinase
/ MAP Kinase Signaling System
/ Medical prognosis
/ Mesenchyme
/ Metastases
/ Metastasis
/ Mice
/ Monoclonal antibodies
/ Neoplasm Recurrence, Local
/ Neuropilin
/ Neuropilin-1 - genetics
/ Neuropilin-1 - therapeutic use
/ Oncology
/ Phenotypes
/ Prognosis
/ Protein arrays
/ Proteins
/ Ras protein
/ ras Proteins
/ Research Article
/ Signal transduction
/ siRNA
/ Software
/ Stem cells
/ Stem Cells - metabolism
/ Surgical Oncology
/ Survival analysis
/ Transcriptomics
/ Triple Negative Breast Neoplasms - pathology
/ Triple-negative breast cancer
/ Tumors
/ Western blotting
/ Xenografts
2022
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Neuropilin-1 is over-expressed in claudin-low breast cancer and promotes tumor progression through acquisition of stem cell characteristics and RAS/MAPK pathway activation
by
Volpert, Marianna
, Hollier, Brett G.
, Rockstroh, Anja
, Thompson, Erik W.
, Lehman, Melanie
, Tang, Yu Hin
, Sokolowski, Kamil A.
, Gregory, Philip A.
, Nelson, Colleen C.
, Lynam, Layla-Rose
in
Animal models
/ Animals
/ Biomedical and Life Sciences
/ Biomedicine
/ Breast cancer
/ Breast Neoplasms - metabolism
/ Cancer Research
/ Cancer stem cells
/ Cancer therapies
/ Cell Line, Tumor
/ Cell proliferation
/ Cell Proliferation - genetics
/ Cell surface
/ Chemotherapy
/ Claudin-low
/ Claudins - metabolism
/ Development and progression
/ Female
/ Gene expression
/ Genomes
/ Humans
/ Kinases
/ MAP kinase
/ MAP Kinase Signaling System
/ Medical prognosis
/ Mesenchyme
/ Metastases
/ Metastasis
/ Mice
/ Monoclonal antibodies
/ Neoplasm Recurrence, Local
/ Neuropilin
/ Neuropilin-1 - genetics
/ Neuropilin-1 - therapeutic use
/ Oncology
/ Phenotypes
/ Prognosis
/ Protein arrays
/ Proteins
/ Ras protein
/ ras Proteins
/ Research Article
/ Signal transduction
/ siRNA
/ Software
/ Stem cells
/ Stem Cells - metabolism
/ Surgical Oncology
/ Survival analysis
/ Transcriptomics
/ Triple Negative Breast Neoplasms - pathology
/ Triple-negative breast cancer
/ Tumors
/ Western blotting
/ Xenografts
2022
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Neuropilin-1 is over-expressed in claudin-low breast cancer and promotes tumor progression through acquisition of stem cell characteristics and RAS/MAPK pathway activation
Journal Article
Neuropilin-1 is over-expressed in claudin-low breast cancer and promotes tumor progression through acquisition of stem cell characteristics and RAS/MAPK pathway activation
2022
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Overview
Background
Triple-negative breast cancers (TNBC) have a relatively poor prognosis and responses to targeted therapies. Between 25 and 39% of TNBCs are claudin-low, a poorly differentiated subtype enriched for mesenchymal, stem cell and mitogen-activated signaling pathways. We investigated the role of the cell-surface co-receptor NRP1 in the biology of claudin-low TNBC.
Methods
The clinical prognostic value of NRP1 was determined by Kaplan–Meier analysis. GSVA analysis of METABRIC and Oslo2 transcriptomics datasets was used to correlate NRP1 expression with claudin-low gene signature scores.
NRP1
siRNA knockdown was performed in MDA-MB-231, BT-549, SUM159 and Hs578T claudin-low cells and proliferation and viability measured by live cell imaging and DNA quantification. In SUM159 orthotopic xenograft models using NSG mice, NRP1 was suppressed by shRNA knockdown or systemic treatment with the NRP1-targeted monoclonal antibody Vesencumab. NRP1-mediated signaling pathways were interrogated by protein array and Western blotting.
Results
High NRP1 expression was associated with shorter relapse- and metastasis-free survival specifically in ER-negative BrCa cohorts. NRP1 was over-expressed specifically in claudin-low clinical samples and cell lines, and NRP1 knockdown reduced proliferation of claudin-low cells and prolonged survival in a claudin-low orthotopic xenograft model. NRP1 inhibition suppressed expression of the mesenchymal and stem cell markers ZEB1 and ITGA6, respectively, compromised spheroid-initiating capacity and exerted potent anti-tumor effects on claudin-low orthotopic xenografts (12.8-fold reduction in endpoint tumor volume). NRP1 was required to maintain maximal RAS/MAPK signaling via EGFR and PDGFR, a hallmark of claudin-low tumors.
Conclusions
These data implicate NRP1 in the aggressive phenotype of claudin-low breast cancer and offer a novel targeted therapeutic approach to this poor prognosis subtype.
Publisher
BioMed Central,BioMed Central Ltd,Springer Nature B.V,BMC
Subject
/ Animals
/ Biomedical and Life Sciences
/ Breast Neoplasms - metabolism
/ Cell Proliferation - genetics
/ Female
/ Genomes
/ Humans
/ Kinases
/ Mice
/ Neuropilin-1 - therapeutic use
/ Oncology
/ Proteins
/ siRNA
/ Software
/ Triple Negative Breast Neoplasms - pathology
/ Triple-negative breast cancer
/ Tumors
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