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Niosomal Curcumin Suppresses IL17/IL23 Immunopathogenic Axis in Skin Lesions of Psoriatic Patients: A Pilot Randomized Controlled Trial

Psoriasis (PS) is characterized by hyperplasia of epidermis and infiltration of immune cells in the dermis. A negligible susceptibility of hypodermic permeation for local anti-inflammatory remedies is one of the major causes of medication failures. Although curcumin (CUR) has indicated effectiveness...

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Published in:	Life (Basel, Switzerland) Switzerland), 2023-04, Vol.13 (5), p.1076
Main Authors:	Kolahdooz, Hanieh, Khori, Vahid, Erfani-Moghadam, Vahid, Livani, Fatemeh, Mohammadi, Saeed, Memarian, Ali
Format:	Article
Language:	English
Subjects:	Care and treatment Collagen Curcumin Dermis Disease Drug delivery systems Drugs Epidermis Gene expression Health aspects Hyaluronic acid Hydration Hyperplasia IL17 IL22 IL23 Immune system Inflammation Interleukin 17 Interleukin 22 Interleukin 23 Interleukins Ki67 Lesions Nanoparticles Neutrophils niosome Pathogenesis Patients Peptides Permeation Placebos Psoriasis Skin Skin diseases Skin lesions Steroids Stratum corneum Testing Thin films Turmeric Vehicles
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creator	Kolahdooz, Hanieh Khori, Vahid Erfani-Moghadam, Vahid Livani, Fatemeh Mohammadi, Saeed Memarian, Ali
description	Psoriasis (PS) is characterized by hyperplasia of epidermis and infiltration of immune cells in the dermis. A negligible susceptibility of hypodermic permeation for local anti-inflammatory remedies is one of the major causes of medication failures. Although curcumin (CUR) has indicated effectiveness in treatment of inflammation, its successful permeation through the stratum corneum is yet a challenging issue. Therefore, niosome (NIO) nanoparticles were used as curcumin carriers to enhance its delivery and anti-inflammatory effects. Curcumin-niosome (CUR-NIO) formulations were constructed by the thin-film-hydration (TFH) technique and were added to hyaluronic acid and Marine-collagen gel-based formulation. Five mild-to-moderate PS patients (18-60 years) with PASI scores < 30 with symmetrical and similar lesions were included in the study. The prepared formulation (CUR 15 µM) was topically administered for 4 weeks on the skin lesions, in comparison to the placebo. Clinical skin manifestations were monitored and skin punches were obtained for further gene expression analyses. There was a significant reduction in redness, scaling, and an apparent improvement in CUR-NIO-treated group in comparison to the placebo-treated counterpart. The gene expression analyses resulted in significantly downregulation of IL17, IL23, IL22, and TNFα, S100A7, S100A12, and Ki67 in CUR-NIO-treated lesions. Consequently, CUR-NIO could provide therapeutic approaches for the patients with mild-to-moderate PS by suppressing the IL17/IL23 immunopathogenic axis.
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A negligible susceptibility of hypodermic permeation for local anti-inflammatory remedies is one of the major causes of medication failures. Although curcumin (CUR) has indicated effectiveness in treatment of inflammation, its successful permeation through the stratum corneum is yet a challenging issue. Therefore, niosome (NIO) nanoparticles were used as curcumin carriers to enhance its delivery and anti-inflammatory effects. Curcumin-niosome (CUR-NIO) formulations were constructed by the thin-film-hydration (TFH) technique and were added to hyaluronic acid and Marine-collagen gel-based formulation. Five mild-to-moderate PS patients (18-60 years) with PASI scores < 30 with symmetrical and similar lesions were included in the study. The prepared formulation (CUR 15 µM) was topically administered for 4 weeks on the skin lesions, in comparison to the placebo. Clinical skin manifestations were monitored and skin punches were obtained for further gene expression analyses. There was a significant reduction in redness, scaling, and an apparent improvement in CUR-NIO-treated group in comparison to the placebo-treated counterpart. The gene expression analyses resulted in significantly downregulation of IL17, IL23, IL22, and TNFα, S100A7, S100A12, and Ki67 in CUR-NIO-treated lesions. Consequently, CUR-NIO could provide therapeutic approaches for the patients with mild-to-moderate PS by suppressing the IL17/IL23 immunopathogenic axis.</description><identifier>ISSN: 2075-1729</identifier><identifier>EISSN: 2075-1729</identifier><identifier>DOI: 10.3390/life13051076</identifier><identifier>PMID: 37240721</identifier><language>eng</language><publisher>Switzerland: MDPI AG</publisher><subject>Care and treatment ; Collagen ; Curcumin ; Dermis ; Disease ; Drug delivery systems ; Drugs ; Epidermis ; Gene expression ; Health aspects ; Hyaluronic acid ; Hydration ; Hyperplasia ; IL17 ; IL22 ; IL23 ; Immune system ; Inflammation ; Interleukin 17 ; Interleukin 22 ; Interleukin 23 ; Interleukins ; Ki67 ; Lesions ; Nanoparticles ; Neutrophils ; niosome ; Pathogenesis ; Patients ; Peptides ; Permeation ; Placebos ; Psoriasis ; Skin ; Skin diseases ; Skin lesions ; Steroids ; Stratum corneum ; Testing ; Thin films ; Turmeric ; Vehicles</subject><ispartof>Life (Basel, Switzerland), 2023-04, Vol.13 (5), p.1076</ispartof><rights>COPYRIGHT 2023 MDPI AG</rights><rights>2023 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 (https://creativecommons.org/licenses/by/4.0/). 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A negligible susceptibility of hypodermic permeation for local anti-inflammatory remedies is one of the major causes of medication failures. Although curcumin (CUR) has indicated effectiveness in treatment of inflammation, its successful permeation through the stratum corneum is yet a challenging issue. Therefore, niosome (NIO) nanoparticles were used as curcumin carriers to enhance its delivery and anti-inflammatory effects. Curcumin-niosome (CUR-NIO) formulations were constructed by the thin-film-hydration (TFH) technique and were added to hyaluronic acid and Marine-collagen gel-based formulation. Five mild-to-moderate PS patients (18-60 years) with PASI scores < 30 with symmetrical and similar lesions were included in the study. The prepared formulation (CUR 15 µM) was topically administered for 4 weeks on the skin lesions, in comparison to the placebo. Clinical skin manifestations were monitored and skin punches were obtained for further gene expression analyses. 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subjects	Care and treatment Collagen Curcumin Dermis Disease Drug delivery systems Drugs Epidermis Gene expression Health aspects Hyaluronic acid Hydration Hyperplasia IL17 IL22 IL23 Immune system Inflammation Interleukin 17 Interleukin 22 Interleukin 23 Interleukins Ki67 Lesions Nanoparticles Neutrophils niosome Pathogenesis Patients Peptides Permeation Placebos Psoriasis Skin Skin diseases Skin lesions Steroids Stratum corneum Testing Thin films Turmeric Vehicles
title	Niosomal Curcumin Suppresses IL17/IL23 Immunopathogenic Axis in Skin Lesions of Psoriatic Patients: A Pilot Randomized Controlled Trial
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