Improving Topical Non-Melanoma Skin Cancer Treatment: In vitro Efficacy of a Novel Guanosine-Analog Phosphonate

Abstract: Actinic keratosis, a frequent carcinoma in situ of non-melanoma skin cancer (NMSC), can transform into life-threatening cutaneous squamous cell carcinoma. Current treatment is limited due to low complete clearance rates and asks for novel therapeutic concepts; the novel purine nucleotide analogue OxBu may be an option. In order to enhance skin penetration, solid lipid nanoparticles (SLN, 136-156 nm) were produced with an OxBu entrapment efficiency of 96.5 ± 0.1%. For improved preclinical evaluation, we combine… Show more

“…Hoeller Obrigkeit and colleagues use low carcinoma cell counts [16], Commandeur et al seed carcinoma cells only [15], and we used previously a ratio of 3:100 carcinoma to normal cells [11,18]. Albeit their limitations, carcinoma cell lines are Fig.…”

“…Since organotypic NMSC models are developed for preclinical drug evaluation [11,15,16], we investigated the response of cSCC-E and cSCC-ED models to ingenol mebutate in a blinded vehicle-controlled study design (Fig. 4A).…”

“…Ingenol mebutate offers a short-term treatment regimen, but causes rapid and unspecific necrosis [10]. Purine-analog phosphonates showed promising efficacy in monolayer cell cultures, but first attempts to use nanoparticles for enhanced drug delivery show marginal effects [11]. High-molecular-weight cationic membrane-active peptides [12] are theoretically excluded from topical treatment due to their physicochemical properties [13].…”

“…Currently NMSC is reproduced for preclinical drug evaluation by mouse models [14], organotypic skin models [11,15,16], or tumor specimens [17]. Each approach faces distinct limitations: inter alia murine skin morphology considerably differs from human actinic keratosis, organotypic skin models are based on cell lines and tumor specimens originate from invasive carcinomas.…”

The barrier function of organotypic non-melanoma skin cancer models

“…Hoeller Obrigkeit and colleagues use low carcinoma cell counts [16], Commandeur et al seed carcinoma cells only [15], and we used previously a ratio of 3:100 carcinoma to normal cells [11,18]. Albeit their limitations, carcinoma cell lines are Fig.…”

“…Since organotypic NMSC models are developed for preclinical drug evaluation [11,15,16], we investigated the response of cSCC-E and cSCC-ED models to ingenol mebutate in a blinded vehicle-controlled study design (Fig. 4A).…”

“…Ingenol mebutate offers a short-term treatment regimen, but causes rapid and unspecific necrosis [10]. Purine-analog phosphonates showed promising efficacy in monolayer cell cultures, but first attempts to use nanoparticles for enhanced drug delivery show marginal effects [11]. High-molecular-weight cationic membrane-active peptides [12] are theoretically excluded from topical treatment due to their physicochemical properties [13].…”

“…Currently NMSC is reproduced for preclinical drug evaluation by mouse models [14], organotypic skin models [11,15,16], or tumor specimens [17]. Each approach faces distinct limitations: inter alia murine skin morphology considerably differs from human actinic keratosis, organotypic skin models are based on cell lines and tumor specimens originate from invasive carcinomas.…”

The barrier function of organotypic non-melanoma skin cancer models

“…Very recently, Gosselin et al [34] reported a 2′-C-methyl branched guanosine pro-nucleotide as a potent liver-targeted HCV polymerase inhibitor. Schaefer–Korting et al [35] found that a guanosine-analog phosphonate can improve topical non-melanoma skin cancer treatment.…”

Synthesis and Structure-Activity Relationships of Imidazole-Coumarin Conjugates against Hepatitis C Virus

Core-Shell Nanotransporters for the Skin