Modulation of biomarkers related to tumor initiation and promotion in mouse skin by a natural β-glucuronidase inhibitor and its precursors

Kowalczyk, Magdalena C.; Spears, Erick; Naróg, Maciej; Zoltaszek, Robert; Kowalczyk, Piotr; Hanausek, Margaret; Yoshimi, Naoki; Slaga, Thomas J.; Wałaszek, Zbigniew

doi:10.3892/or.2011.1351

Cited by 4 publications

(7 citation statements)

References 17 publications

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“…In another study, D-SAL was more therapeutically efficient compared to its natural precursor (D-GL), for reducing epidermal hyperplasia (lethargic tumour promoter) and inflammation in 7,12dimethylbenz(a)anthracene (DMBA)-induced complete skin carcinogenesis of SENCAR mice [125]. Pre and cotreatment of murine models with D-SAL for 4-weeks (twice weekly) by topical administration (0.5e4 mg) or dietary treatment (0.5 and 1%), both significantly reduced epidermal hyperplasia and inflammation by up to 57% of DMBA-controls in a dose-dependent manner.…”

Section: Natural Acids and Lactonesmentioning

confidence: 99%

Therapeutic significance of β-glucuronidase activity and its inhibitors: A review

Awolade

Cele

Kerru

et al. 2020

European Journal of Medicinal Chemistry

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BiomarkerEnzyme inhibition Molecular target Structure activity relationship a b s t r a c tThe emergence of disease and dearth of effective pharmacological agents on most therapeutic fronts, constitutes a major threat to global public health and man's existence. Consequently, this has created an exigency in the search for new drugs with improved clinical utility or means of potentiating available ones. To this end, accumulating empirical evidence supports molecular target therapy as a plausible egress and, b-glucuronidase (bGLU) e a lysosomal acid hydrolase responsible for the catalytic deconjugation of b-D-glucuronides has emerged as a viable molecular target for several therapeutic applications. The enzyme's activity level in body fluids is also deemed a potential biomarker for the diagnosis of some pathological conditions. Moreover, due to its role in colon carcinogenesis and certain drug-induced dose-limiting toxicities, the development of potent inhibitors of bGLU in human intestinal microbiota has aroused increased attention over the years. Nevertheless, although our literature survey revealed both natural products and synthetic scaffolds as potential inhibitors of the enzyme, only few of these have found clinical utility, albeit with moderate to poor pharmacokinetic profile. Hence, in this review we present a compendium of exploits in the present millennium directed towards the inhibition of bGLU. The aim is to proffer a platform on which new scaffolds can be modelled for improved bGLU inhibitory potency and the development of new therapeutic agents in consequential.

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Section: Natural Acids and Lactonesmentioning

confidence: 99%

Therapeutic significance of β-glucuronidase activity and its inhibitors: A review

Awolade

Cele

Kerru

et al. 2020

European Journal of Medicinal Chemistry

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“…As demonstrated in another study, the topical administration of the βG inhibitor, D-glucaro-1,4-lactone (1,4-GL), or D-glucuronic acid-γ-lactone (GUL) its precursor, to SENCAR mice with skin carcinogenesis, epidermal hyperplasia was significantly reduced along with a decrease in inflammation ( 107 ). Moreover, Ha-ras mutations were reduced upon experimental therapy.…”

Section: Testing Avenues Using Animal Models Of Skin Carcinogenesimentioning

confidence: 83%

“…Moreover, Ha-ras mutations were reduced upon experimental therapy. That study demonstrated that whether administered topically or through diet, therapy with GUL or 1,4-GL was effective in hindering experimental skin tumorigenesis ( 107 ).…”

Section: Testing Avenues Using Animal Models Of Skin Carcinogenesimentioning

confidence: 98%

Chemically induced skin carcinogenesis: Updates in experimental models (Review)

et al. 2016

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Skin cancer is one of the most common malignancies affecting humans worldwide, and its incidence is rapidly increasing. The study of skin carcinogenesis is of major interest for both scientific research and clinical practice and the use of in vivo systems may facilitate the investigation of early alterations in the skin and of the mechanisms involved, and may also lead to the development of novel therapeutic strategies for skin cancer. This review outlines several aspects regarding the skin toxicity testing domain in mouse models of chemically induced skin carcinogenesis. There are important strain differences in view of the histological type, development and clinical evolution of the skin tumor, differences reported decades ago and confirmed by our hands-on experience. Using mouse models in preclinical testing is important due to the fact that, at the molecular level, common mechanisms with human cutaneous tumorigenesis are depicted. These animal models resemble human skin cancer development, in that genetic changes caused by carcinogens and pro-inflammatory cytokines, and simultaneous inflammation sustained by pro-inflammatory cytokines and chemokines favor tumor progression. Drugs and environmental conditions can be tested using these animal models. keeping in mind the differences between human and rodent skin physiology.

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“…Lysosomale Enzyme wie ß-Glucuronidase (ßG) sind häufig an hyperplastischen epidermalen Prozessen, an der Karzinogenese und Entzündung beteiligt. Es konnte kürzlich gezeigt werden, dass in dem 7,12-dimethylbenz(a)anthrazen induzierbaren Hautkrebsmodell der natürliche Inhibitor G-Glucuro-1,4-Lacton (1,4GL) sowie sein Vorläufermolekül D-Glucuronsäure-gamma-Lacton (GUL) in einer topischen und diätetischen Applikation erhebliche anti-entzündliche und anti-tumoröse Aktivitäten haben [3]. Viele Pflanzeninhaltsstoffe werden an dem Mehrschrittmodell der Haut zur Karzinogenese geprüft.…”

Section: Die Haut Als Organmodell Zum Studium Von Krankheitsbildernunclassified

“…B. die Behandlung von Melasma kaum wissenschaftlich klar strukturiert und standardisiert ist und klinische Studien dringend benötigt werden, um die Wirksamkeit derzeitig marginal effektiver Therapien entscheidend zu verbessern [26]. Störungen in der Melanogenese als klinische Erscheinungsformen von Hautpigmentstörungen sind eng verknüpft mit den Stoffwechselprozessen zur Eumelanin-(dunkel, fotoprotektiv) und zur Phämelanoninbildung (hell, Fotosynthese von Vitamin D [3]); evolutionsbiologisch spielen Glutathion und Melanokortin eine tragende Rolle hinsichtlich der Stimulierung bzw. Inhibition von dunklem und rötlich-hellem Melanin [27].…”

Section: Glutathion Und Bleachingunclassified

Hautschutzmoleküle - Quo vadis? Von der Chemoprävention bis zur kulturell geprägten Dermatoästhetik

Rietz

Zänker

2011

Akt Dermatol

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Zusammenfassung Basierend auf dem sich akkumulierenden Wissen zu genetischen, molekularen und zellul?ren Funktionen der Haut, hat sich die Suche nach neuen Hautschutzmolek?len intensiviert, die 1.) pr?ventiv sind hinsichtlich extrinsischen Noxen, die f?r eine vorzeitige Hautalterung verantwortlich sind, die 2.) pr?ventiv oder kurativ gegen schwere, chronifizierende Hauterkrankungen wirken und 3.) pr?ventiv hinsichtlich einer Tumorigenese eingesetzt werden k?nnen. Zugleich sollen solche Stoffe auch pflegende Eigenschaften im Sinne einer Dermato?sthetik aufweisen. Das Konzept einer personalisierten Medizin l?sst sich dabei beispielhaft an dem Organ Haut verwirklichen, da genetische und epigenetische Daten hinreichend zuverl?ssig erhoben werden und in Therapieoptionen einflie?en k?nnen. Ein therapeutisches Beispiel f?r Hautschutz und -pflege ist die topische Anwendung von Komponenten des Glutathion-Detoxifikationssystems, das reduzierte Glutathion (GSH).

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Modulation of biomarkers related to tumor initiation and promotion in mouse skin by a natural β-glucuronidase inhibitor and its precursors

Cited by 4 publications

References 17 publications

Therapeutic significance of β-glucuronidase activity and its inhibitors: A review

Therapeutic significance of β-glucuronidase activity and its inhibitors: A review

Chemically induced skin carcinogenesis: Updates in experimental models (Review)

Hautschutzmoleküle - Quo vadis? Von der Chemoprävention bis zur kulturell geprägten Dermatoästhetik

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