Dysfunction of Autophagy: A Possible Mechanism Involved in the Pathogenesis of Vitiligo by Breaking the Redox Balance of Melanocytes

Hamade

et al. 2019

CTOY

Introduction: bacterial keratitis caused by Pseudomonas aeruginosa is one of the causes of blindness in the world, due to pathogenicity of the bacteria that can lead to corneal perforation. Studies on the protein annexin A1 (AnxA1) point it as one of the essential mediators in homeostasis of inflammation and ocular infections. However, there are no known reports of AnxA1 in keratitis. Objetive: to investigate the expression profile of AnxA1 in the P. aeruginosainduced keratitis model in two strains of mice (susceptible and pathogen resistant).Method: for the development of experimetal keratitis, the mice had their right eyes ulcerated and immediately inoculated with 5 μl of P. aeruginosa in PBS. The animals were euthanized after 24 hours of the bacteria inoculation. The eyes were clinically evaluated and histopathologically processed for quantitative analyses of the inflammatory infiltrate and immunohistochemical studies of the expressions of the AnxA1 and the receptor for formylated peptides (fpr2).Results: our results demonstrated a higher influx of inflammatory cells, mainly neutrophils in the susceptible animals (C57BL / 6) compared to those considered resistant (BALB / c) and controls. Immunohistochemical studies indicated weak expression of AnxA1 and fpr2 in the anterior epithelium and stroma of the cornea. However, after keratitis induction, overexpression of AnxA1 and fpr2 occurred in the corneas of both mice strains. Furthermore, greater expression of AnxA1 in the anterior corneal epithelium was observed in the C57BL / 6 animals.Conclusions: AnxA1 and fpr2 may be related to infectious keratitis induced by P.aeruginosa, which stimulates further investigations on the use of AnxA1 as a possible coadjuvant therapeutic strategy in bacterial keratitis.

Section: Introductionmentioning

confidence: 99%

Evaluation of Annexin A1 Protein in an Infectious Keratitis Model: Therapeutic Perspectives

Hamade

et al. 2019

CTOY

“…Vitiligo is a hypopigmentary skin autoimmune pathology characterized by the development of lesions lacking melanin, which is the natural pigment of the skin produced by melanocytes. Vitiligo affects 0.5–2% of the global population, with the highest incidence rates occurring in India, Japan, and Mexico [ 1 , 2 , 3 ]. This pathology can be classified as either nonsegmental, due to the symmetrical arrangement of the lesions, or segmental, due to the nonsymmetrical disposition of the lesions [ 4 ].…”

Section: Introductionmentioning

confidence: 99%

“…The etiology of vitiligo is not completely understood; nevertheless, different theories could explain the development and progression of this pathology. Amongst these, oxidative stress and the involvement of the immune system are positioned as the most accepted theories, in addition to genetic factors that predispose individuals to vitiligo [ 3 , 12 , 13 ]. An increase in reactive oxygen species that cause DNA damage, the release of exosomes with intracellular peptides and misfolded proteins, and apoptosis have been reported.…”

Section: Introductionmentioning

confidence: 99%

“…An increase in reactive oxygen species that cause DNA damage, the release of exosomes with intracellular peptides and misfolded proteins, and apoptosis have been reported. Thus, released peptides and misfolded proteins can be recognized by the immune system and stimulate the development of autoreactive lymphocytes responsive to melanocyte epitopes [ 3 , 14 , 15 ]. Moreover, CD8 + T lymphocytes were identified as being responsible for the progress and intensity of vitiligo; once melanocyte antigens are recognized, these lymphocytes release granzyme and perforin, promoting apoptosis in melanocyte cells.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Computational Study of C-X-C Chemokine Receptor (CXCR)3 Binding with Its Natural Agonists Chemokine (C-X-C Motif) Ligand (CXCL)9, 10 and 11 and with Synthetic Antagonists: Insights of Receptor Activation towards Drug Design for Vitiligo

Aguilera-Durán

Romo-Mancillas

2020

Molecules

Vitiligo is a hypopigmentary skin pathology resulting from the death of melanocytes due to the activity of CD8+ cytotoxic lymphocytes and overexpression of chemokines. These include CXCL9, CXCL10, and CXCL11 and its receptor CXCR3, both in peripheral cells of the immune system and in the skin of patients diagnosed with vitiligo. The three-dimensional structure of CXCR3 and CXCL9 has not been reported experimentally; thus, homology modeling and molecular dynamics could be useful for the study of this chemotaxis-promoter axis. In this work, a homology model of CXCR3 and CXCL9 and the structure of the CXCR3/Gαi/0βγ complex with post-translational modifications of CXCR3 are reported for the study of the interaction of chemokines with CXCR3 through all-atom (AA-MD) and coarse-grained molecular dynamics (CG-MD) simulations. AA-MD and CG-MD simulations showed the first activation step of the CXCR3 receptor with all chemokines and the second activation step in the CXCR3-CXCL10 complex through a decrease in the distance between the chemokine and the transmembrane region of CXCR3 and the separation of the βγ complex from the α subunit in the G-protein. Additionally, a general protein–ligand interaction model was calculated, based on known antagonists binding to CXCR3. These results contribute to understanding the activation mechanism of CXCR3 and the design of new molecules that inhibit chemokine binding or antagonize the receptor, provoking a decrease of chemotaxis caused by the CXCR3/chemokines axis.

“…The melanocytes of vitiligo are particularly vulnerable to damage or apoptosis under certain circumstances such as excessive ROS production. 8,9 ROS can attack melanocytes and interfere with the normal metabolism, proliferation, and differentiation of melanocytes, causing cell apoptosis and defects. 10 Excessive accumulation of ROS in the epidermis of vitiligo patients leads to the disorders of melanocytes, resulting in damage to the mitochondrial electron transport chain; this further forms a vicious cycle and leads to the destruction of melanocytes.…”

Section: Introductionmentioning

confidence: 99%

Sodium tanshinone IIA silate increases melanin synthesis by activating the MAPK and PKA pathways and protects melanocytes from H₂O₂-induced oxidative stress

Zhong

et al. 2019

RSC Adv.