Evaluation of chemotherapeutic and cancer-protective properties of sphingosine and C2-ceramide in a human breast stem cell derived carcinogenesis model.
Int J Oncol
; 54(2): 655-664, 2019 02.
Article
em En
| MEDLINE
| ID: mdl-30483770
The overall goal of the present study was to evaluate the chemotherapeutic and cancerprotective properties of Derythrosphingosine (sphingosine) and C2ceramide using a human breast epithelial cell (HBEC) culture system, which represents multiplestages of breast carcinogenesis. The HBEC model includes Type I HBECs (normal stem), Type II HBECs (normal differentiated) and transformed cells (immortal/nontumorigenic cells and tumorigenic cells, which are transformed from the same parental normal stem cells). The results of the present study indicate that sphingosine preferentially inhibits proliferation and causes death of normal stem cells (Type I), tumorigenic cells, and MCF7 breast cancer cells, but not normal differentiated cells (Type II). In contrast to the selective antiproliferative effects of sphingosine, C2ceramide inhibits proliferation of normal differentiated cells as well as normal stem cells, tumorigenic cells, and MCF7 cancer cells with similar potency. Both sphingosine and C2ceramide induce apoptosis in tumorigenic cells. Among the sphingosine stereoisomers (Derythro, Dthreo, Lerythro, and Lthreo) and sphinganine that were tested, Lerythrosphingosine most potently inhibits proliferation of tumorigenic cells. The inhibition of breast tumorigenic/cancer cell proliferation by sphingosine was accompanied by inhibition of telomerase activity. Sphingosine at noncytotoxic concentrations, but not C2ceramide, induces differentiation of normal stem cells (Type I), thereby reducing the number of stem cells that are more susceptible to neoplastic transformation. To the best of our knowledge, the present study demonstrates one of the first results that sphingosine can be a potential chemotherapeutic and cancerprotective agent, whereas C2ceramide is not an ideal chemotherapeutic and cancerprotective agent due to its antiproliferative effects on Type II HBECs and its inability to induce the differentiation of Type I to Type II HBECs.
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Base de dados:
MEDLINE
Assunto principal:
Esfingosina
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Mama
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Neoplasias da Mama
Limite:
Female
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Humans
Idioma:
En
Ano de publicação:
2019
Tipo de documento:
Article