Secretion modification region-derived peptide blocks exosome release and mediates cell cycle arrest in breast cancer cells

Huang, Ming-Bo; González, Ricardo R.; Lillard, James W.; Bond, Vincent C.

doi:10.18632/oncotarget.14513

Cited by 43 publications

(51 citation statements)

References 49 publications

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“…According to previous reports, the tolerance to chemotherapy and radiotherapy is closely related with CLU expression in several cancers, and CLU up-regulation has been confirmed in many cancers including prostate, kidney, bladder, breast, head and neck, colon, cervical, pancreatic, lung, melanoma lymphoma [16,18] . Therefore, CLU has been considered as a biomarker for tumour malignancy, and it is believed that improvement of tumour cell sensitivity to chemotherapy and radiotherapy is promising way to control cancer by reducing CLU expression [14,[19][20][21] .…”

Section: Discussionmentioning

confidence: 99%

Cloning and Tissue Expression of Clusterin in Bufo gargarizans

2020

International Journal of Research Studies in Biosciences

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Section: Discussionmentioning

confidence: 99%

Cloning and Tissue Expression of Clusterin in Bufo gargarizans

2020

International Journal of Research Studies in Biosciences

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“…While the SMR peptide and chemotherapeutic drugs were compound to remedy cancer cells, PEG-SMRwt-Clu synergically enhanced the anti-proliferative efficacies of drugs, considerably promoted the tumor cell growth suppression efficacy of drugs and inhibited exosomes secretion in breast cancer cell lines MCF-7 and MDA-MB-231 cells. Therefore the considerable usage of PEG-SMRwt-Clu peptide is pivotal process for the prevention and therapy of human breast tumor cells ( Huang et al, 2017 ).…”

Section: Functions and Remedial Roles Of Exosomes In Different Kindsmentioning

confidence: 99%

Exosomes in cancer: small vesicular transporters for cancer progression and metastasis, biomarkers in cancer therapeutics

Abak

Abhari

Rahimzadeh

2018

PeerJ

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Cancer progression is a polygenic procedure in which the exosomes can function as substantial roles. Exosomes are tiny, phospholipid bilayer membrane nanovesicles of endocytic derivation with a diameter of 40–100 nm. These nanovesicles can transport bioactive molecules containing mRNAs, proteins, DNA fragments, and non-coding RNAs from a donor cell to recipient cells, and cause the alteration in genetic and epigenetic factors and reprogramming of the target cells. Many diverse cell types such as mesenchymal cells, immune cells, and cancer cells can induce the release of exosomes. Increasing evidence illustrated that the exosomes derived from tumor cells might trigger the tumor initiation, tumor cell growth and progression, metastasis, and drug resistance. The secreted nanovesicles of exosomes can play significant roles in cells communicate via shuttling the nucleic acid molecules and proteins to target cells and tissues. In this review, we discussed multiple mechanisms related to biogenesis, load, and shuttle of the exosomes. Also, we illustrated the diverse roles of exosomes in several types of human cancer development, tumor immunology, angiogenesis, and metastasis. The exosomes may act as the promising biomarkers for the prognosis of various types of cancers which suggested a new pathway for anti-tumor therapeutic of these nanovesicles and promoted exosome-based cancer for clinical diagnostic and remedial procedures.

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“…Inhibition of exosomal communication between cancer cells and the stromal microenvironment may have therapeutic potential. 92 , 93 GW4869 is a neutral sphingomyelinase inhibitor that blocks ceramide-mediated inward budding of MVBs and exosome release; furthermore, it is widely used in breast cancer cell and CAF experiments. 38 , 92 , 94 In combination with chemotherapeutic agents, it significantly reduced the survival of carcinoma cells in co-cultures and mouse experiments.…”

Section: Clinical Perspectives and Future Directionsmentioning

confidence: 99%

Perspective: bidirectional exosomal transport between cancer stem cells and their fibroblast-rich microenvironment during metastasis formation

et al. 2018

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Carcinomas are complex structures composed of hierarchically organized distinct cell populations such as cancer stem cells and non-stem (bulk) cancer cells. Their genetic/epigenetic makeup and the dynamic interplay between the malignant cell populations and their stromal fibroblasts are important determinants of metastatic tumor invasion. Important mediators of these interactions are the small, membrane-enclosed extracellular vesicles, in particular exosomes. Both cancer cell and fibroblast-derived exosomes carry a set of regulatory molecules, including proteins and different species of RNA, which cooperatively support metastatic tumor spread. Here, we briefly overview potential links between cancer stem cells and the exosome-mediated fibroblast-enriched metastatic niche formation to discuss their role in the promotion of tumor growth and metastatic expansion in breast carcinoma models.

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Secretion modification region-derived peptide blocks exosome release and mediates cell cycle arrest in breast cancer cells

Cited by 43 publications

References 49 publications

Cloning and Tissue Expression of Clusterin in Bufo gargarizans

Cloning and Tissue Expression of Clusterin in Bufo gargarizans

Exosomes in cancer: small vesicular transporters for cancer progression and metastasis, biomarkers in cancer therapeutics

Perspective: bidirectional exosomal transport between cancer stem cells and their fibroblast-rich microenvironment during metastasis formation

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