Proteomic Analysis of HCC-1954 and MCF-7 Cell Lines Highlights Crosstalk between αv and β1 Integrins, E-Cadherin and HER-2

Overexpression of human epidermal growth factor receptor-2 (HER-2) occurs in 20% of all breast cancer subtypes, especially those that present the worst prognostic outcome through a very invasive and aggressive tumour. HCC-1954 (HER-2+) is a highly invasive, metastatic cell line, whereas MCF-7 is mil...

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Published in:International journal of molecular sciences 2022-09, Vol.23 (17), p.10194
Main Authors: de Abreu Pereira, Denise, Sandim, Vanessa, Fernandes, Thais F. B., Almeida, Vitor Hugo, Rocha, Murilo Ramos, do Amaral, Ronaldo J. F. C., Rossi, Maria Isabel D., Kalume, Dário Eluan, Zingali, Russolina B.
Format: Article
Language:English
Subjects:
Apoptosis
Breast cancer
Cancer therapies
Cell division
Crosstalk
Cytoskeleton
Dehydrogenases
E-cadherin
Epidermal growth factor
ErbB-2 protein
Extracellular matrix
Flow cytometry
Gene expression
Genomes
Growth factors
HER protein
Immunofluorescence
Integrins
Mass spectrometry
Mass spectroscopy
Membrane proteins
Membranes
Metastases
Metastasis
Mortality
Patients
Phenotypes
Protein expression
Proteins
Proteomics
Statistical analysis
Trastuzumab
Tumors
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Summary:Overexpression of human epidermal growth factor receptor-2 (HER-2) occurs in 20% of all breast cancer subtypes, especially those that present the worst prognostic outcome through a very invasive and aggressive tumour. HCC-1954 (HER-2+) is a highly invasive, metastatic cell line, whereas MCF-7 is mildly aggressive and non-invasive. We investigated membrane proteins from both cell lines that could have a pivotal biological significance in metastasis. Membrane protein enrichment for HCC-1954 and MCF-7 proteomic analysis was performed. The samples were analysed and quantified by mass spectrometry. High abundance membrane proteins were confirmed by Western blot, immunofluorescence, and flow cytometry. Protein interaction prediction and correlations with the Cancer Genome Atlas (TCGA) patient data were conducted by bioinformatic analysis. In addition, β1 integrin expression was analysed by Western blot in cells upon trastuzumab treatment. The comparison between HCC-1954 and MCF-7 membrane-enriched proteins revealed that proteins involved in cytoskeleton organisation, such as HER-2, αv and β1 integrins, E-cadherin, and CD166 were more abundant in HCC-1954. β1 integrin membrane expression was higher in the HCC-1954 cell line resistant after trastuzumab treatment. TCGA data analysis showed a trend toward a positive correlation between HER-2 and β1 integrin in HER-2+ breast cancer patients. Differences in protein profile and abundance reflected distinctive capabilities for aggressiveness and invasiveness between HCC-1954 and MCF-7 cell line phenotypes. The higher membrane β1 integrin expression after trastuzumab treatment in the HCC-1954 cell line emphasised the need for investigating the contribution of β1 integrin modulation and its effect on the mechanism of trastuzumab resistance.
ISSN:1422-0067
1661-6596
1422-0067
DOI:10.3390/ijms231710194