ASA Suppresses PGE(2) in Plasma and Melanocytic Nevi of Human Subjects at Increased Risk for Melanoma

Potential anti-inflammatory and anticarcinogenic effects of aspirin (ASA) may be suitable for melanoma chemoprevention, but defining biomarkers in relevant target tissues is prerequisite to performing randomized controlled chemoprevention trials. We conducted open-label studies with ASA in 53 human...

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Autores principales: Varedi, Amir, Rahman, Hafeez, Kumar, Dileep, Catrow, Jonathan L., Cox, James E., Liu, Tong, Florell, Scott R., Boucher, Kenneth M., Okwundu, Nwanneka, Burnett, William J., VanBrocklin, Matthew W., Grossman, Douglas
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7168893/
https://www.ncbi.nlm.nih.gov/pubmed/31906519
http://dx.doi.org/10.3390/ph13010007
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author Varedi, Amir
Rahman, Hafeez
Kumar, Dileep
Catrow, Jonathan L.
Cox, James E.
Liu, Tong
Florell, Scott R.
Boucher, Kenneth M.
Okwundu, Nwanneka
Burnett, William J.
VanBrocklin, Matthew W.
Grossman, Douglas
author_facet Varedi, Amir
Rahman, Hafeez
Kumar, Dileep
Catrow, Jonathan L.
Cox, James E.
Liu, Tong
Florell, Scott R.
Boucher, Kenneth M.
Okwundu, Nwanneka
Burnett, William J.
VanBrocklin, Matthew W.
Grossman, Douglas
author_sort Varedi, Amir
collection PubMed
description Potential anti-inflammatory and anticarcinogenic effects of aspirin (ASA) may be suitable for melanoma chemoprevention, but defining biomarkers in relevant target tissues is prerequisite to performing randomized controlled chemoprevention trials. We conducted open-label studies with ASA in 53 human subjects with melanocytic nevi at increased risk for melanoma. In a pilot study, 12 subjects received a single dose (325 mg) of ASA; metabolites salicylate, salicylurate, and gentisic acid were detected in plasma after 4–8 h, and prostaglandin E2 (PGE(2)) was suppressed in both plasma and nevi for up to 24 h. Subsequently, 41 subjects received either 325 or 81 mg ASA (nonrandomized) daily for one week. ASA metabolites were consistently detected in plasma and nevi, and PGE(2) levels were significantly reduced in both plasma and nevi. Subchronic ASA dosing did not affect 5” adenosine monophosphate-activated protein kinase (AMPK) activation in nevi or leukocyte subsets in peripheral blood, although metabolomic and cytokine profiling of plasma revealed significant decreases in various (non-ASA-derived) metabolites and inflammatory cytokines. In summary, short courses of daily ASA reduce plasma and nevus PGE(2) and some metabolites and cytokines in plasma of human subjects at increased risk for melanoma. PGE(2) may be a useful biomarker in blood and nevi for prospective melanoma chemoprevention studies with ASA.
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spelling pubmed-71688932020-04-20 ASA Suppresses PGE(2) in Plasma and Melanocytic Nevi of Human Subjects at Increased Risk for Melanoma Varedi, Amir Rahman, Hafeez Kumar, Dileep Catrow, Jonathan L. Cox, James E. Liu, Tong Florell, Scott R. Boucher, Kenneth M. Okwundu, Nwanneka Burnett, William J. VanBrocklin, Matthew W. Grossman, Douglas Pharmaceuticals (Basel) Article Potential anti-inflammatory and anticarcinogenic effects of aspirin (ASA) may be suitable for melanoma chemoprevention, but defining biomarkers in relevant target tissues is prerequisite to performing randomized controlled chemoprevention trials. We conducted open-label studies with ASA in 53 human subjects with melanocytic nevi at increased risk for melanoma. In a pilot study, 12 subjects received a single dose (325 mg) of ASA; metabolites salicylate, salicylurate, and gentisic acid were detected in plasma after 4–8 h, and prostaglandin E2 (PGE(2)) was suppressed in both plasma and nevi for up to 24 h. Subsequently, 41 subjects received either 325 or 81 mg ASA (nonrandomized) daily for one week. ASA metabolites were consistently detected in plasma and nevi, and PGE(2) levels were significantly reduced in both plasma and nevi. Subchronic ASA dosing did not affect 5” adenosine monophosphate-activated protein kinase (AMPK) activation in nevi or leukocyte subsets in peripheral blood, although metabolomic and cytokine profiling of plasma revealed significant decreases in various (non-ASA-derived) metabolites and inflammatory cytokines. In summary, short courses of daily ASA reduce plasma and nevus PGE(2) and some metabolites and cytokines in plasma of human subjects at increased risk for melanoma. PGE(2) may be a useful biomarker in blood and nevi for prospective melanoma chemoprevention studies with ASA. MDPI 2020-01-02 /pmc/articles/PMC7168893/ /pubmed/31906519 http://dx.doi.org/10.3390/ph13010007 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Varedi, Amir
Rahman, Hafeez
Kumar, Dileep
Catrow, Jonathan L.
Cox, James E.
Liu, Tong
Florell, Scott R.
Boucher, Kenneth M.
Okwundu, Nwanneka
Burnett, William J.
VanBrocklin, Matthew W.
Grossman, Douglas
ASA Suppresses PGE(2) in Plasma and Melanocytic Nevi of Human Subjects at Increased Risk for Melanoma
title ASA Suppresses PGE(2) in Plasma and Melanocytic Nevi of Human Subjects at Increased Risk for Melanoma
title_full ASA Suppresses PGE(2) in Plasma and Melanocytic Nevi of Human Subjects at Increased Risk for Melanoma
title_fullStr ASA Suppresses PGE(2) in Plasma and Melanocytic Nevi of Human Subjects at Increased Risk for Melanoma
title_full_unstemmed ASA Suppresses PGE(2) in Plasma and Melanocytic Nevi of Human Subjects at Increased Risk for Melanoma
title_short ASA Suppresses PGE(2) in Plasma and Melanocytic Nevi of Human Subjects at Increased Risk for Melanoma
title_sort asa suppresses pge(2) in plasma and melanocytic nevi of human subjects at increased risk for melanoma
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7168893/
https://www.ncbi.nlm.nih.gov/pubmed/31906519
http://dx.doi.org/10.3390/ph13010007
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