Transdermal administration of melatonin coupled to cryopass laser treatment as noninvasive therapy for prostate cancer
Melatonin, a pineal gland hormone, exerts oncostatic activity in several types of human cancer, including prostate, the most common neoplasia and the third most frequent cause of male cancer death in the developed world. The growth of androgen-sensitive LNCaP prostate cancer cells in mice is inhibit...
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doaj-07907334f9d64e4192accb489f044fee2020-11-25T03:28:53ZengTaylor & Francis GroupDrug Delivery1071-75441521-04642017-01-0124197998510.1080/10717544.2017.13387931338793Transdermal administration of melatonin coupled to cryopass laser treatment as noninvasive therapy for prostate cancerLaura Terraneo0Paola Bianciardi1Eleonora Virgili2Elena Finati3Michele Samaja4Rita Paroni5University of MilanUniversity of MilanUniversity of MilanUniversity of MilanUniversity of MilanUniversity of MilanMelatonin, a pineal gland hormone, exerts oncostatic activity in several types of human cancer, including prostate, the most common neoplasia and the third most frequent cause of male cancer death in the developed world. The growth of androgen-sensitive LNCaP prostate cancer cells in mice is inhibited by 3 mg/kg/week melatonin (0.09 mg/mouse/week) delivered by i.p. injections, which is equivalent to a dose of 210 mg/week in humans. The aim of this study is to test an alternative noninvasive delivery route based on transdermal administration of melatonin onto the tumor area followed by cryopass-laser treatment. Two groups of immunodepressed mice were studied, one (n = 10) subjected to 18 cryopass-laser therapy sessions and one (n = 10) subjected to the same treatment without melatonin. These groups were compared with mice treated with i.p.-administered melatonin or vehicle with the same time schedule. We found that cryopass-laser treatment is as efficient as i.p. injections in reducing the growth of LNCaP tumor cells, affecting plasma melatonin and redox balance. Furthermore, both delivery routes share the same effects on the involved biochemical pathway driven by hypoxia-inducible factor 1α. However, cryopass-laser, as used in the present experimental setup, is less efficient than i.p delivery route in increasing the melatonin content and Nrf2 expression in the tumor mass. We conclude that cryopass-laser treatment may have impact for melatonin-based therapy of prostate cancer, by delivering drugs transdermally without causing pain and targeting directly on the site of interest, thereby potentially making long-term treatments more sustainable.http://dx.doi.org/10.1080/10717544.2017.1338793melatonindrug deliveryexperimental prostate cancercryopass-laser therapyanticancer activitytransdermal administration |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Laura Terraneo Paola Bianciardi Eleonora Virgili Elena Finati Michele Samaja Rita Paroni |
spellingShingle |
Laura Terraneo Paola Bianciardi Eleonora Virgili Elena Finati Michele Samaja Rita Paroni Transdermal administration of melatonin coupled to cryopass laser treatment as noninvasive therapy for prostate cancer Drug Delivery melatonin drug delivery experimental prostate cancer cryopass-laser therapy anticancer activity transdermal administration |
author_facet |
Laura Terraneo Paola Bianciardi Eleonora Virgili Elena Finati Michele Samaja Rita Paroni |
author_sort |
Laura Terraneo |
title |
Transdermal administration of melatonin coupled to cryopass laser treatment as noninvasive therapy for prostate cancer |
title_short |
Transdermal administration of melatonin coupled to cryopass laser treatment as noninvasive therapy for prostate cancer |
title_full |
Transdermal administration of melatonin coupled to cryopass laser treatment as noninvasive therapy for prostate cancer |
title_fullStr |
Transdermal administration of melatonin coupled to cryopass laser treatment as noninvasive therapy for prostate cancer |
title_full_unstemmed |
Transdermal administration of melatonin coupled to cryopass laser treatment as noninvasive therapy for prostate cancer |
title_sort |
transdermal administration of melatonin coupled to cryopass laser treatment as noninvasive therapy for prostate cancer |
publisher |
Taylor & Francis Group |
series |
Drug Delivery |
issn |
1071-7544 1521-0464 |
publishDate |
2017-01-01 |
description |
Melatonin, a pineal gland hormone, exerts oncostatic activity in several types of human cancer, including prostate, the most common neoplasia and the third most frequent cause of male cancer death in the developed world. The growth of androgen-sensitive LNCaP prostate cancer cells in mice is inhibited by 3 mg/kg/week melatonin (0.09 mg/mouse/week) delivered by i.p. injections, which is equivalent to a dose of 210 mg/week in humans. The aim of this study is to test an alternative noninvasive delivery route based on transdermal administration of melatonin onto the tumor area followed by cryopass-laser treatment. Two groups of immunodepressed mice were studied, one (n = 10) subjected to 18 cryopass-laser therapy sessions and one (n = 10) subjected to the same treatment without melatonin. These groups were compared with mice treated with i.p.-administered melatonin or vehicle with the same time schedule. We found that cryopass-laser treatment is as efficient as i.p. injections in reducing the growth of LNCaP tumor cells, affecting plasma melatonin and redox balance. Furthermore, both delivery routes share the same effects on the involved biochemical pathway driven by hypoxia-inducible factor 1α. However, cryopass-laser, as used in the present experimental setup, is less efficient than i.p delivery route in increasing the melatonin content and Nrf2 expression in the tumor mass. We conclude that cryopass-laser treatment may have impact for melatonin-based therapy of prostate cancer, by delivering drugs transdermally without causing pain and targeting directly on the site of interest, thereby potentially making long-term treatments more sustainable. |
topic |
melatonin drug delivery experimental prostate cancer cryopass-laser therapy anticancer activity transdermal administration |
url |
http://dx.doi.org/10.1080/10717544.2017.1338793 |
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