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Dive into the research topics where Almudena Íñigo-Portugués is active.

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Featured researches published by Almudena Íñigo-Portugués.


Drug Delivery and Translational Research | 2016

Polymeric nanocapsules: a potential new therapy for corneal wound healing

Sonia Reimondez-Troitiño; Ignacio Alcalde; Noemi Csaba; Almudena Íñigo-Portugués; Maria de la Fuente; Federico Bech; Ana Cristina Riestra; Jesus Merayo-Lloves; María J. Alonso

Corneal injuries are one of the most frequently observed ocular diseases, leading to permanent damage and impaired vision if they are not treated properly. In this sense, adequate wound healing after injury is critical for keeping the integrity and structure of the cornea. The goal of this work was to assess the potential of polymeric nanocapsules, either unloaded or loaded with cyclosporine A or vitamin A, alone or in combination with mitomycin C, for the treatment of corneal injuries induced by photorefractive keratectomy surgery. The biopolymers selected for the formation of the nanocapsules were polyarginine and protamine, which are known for their penetration enhancement effect. The results showed that, following topical instillation to a mouse model of corneal injury, all the nanocapsule formulations, either unloaded or loaded with cyclosporine A or vitamin A, were able to stimulate corneal wound healing. In addition, the healing rate observed for the combination of unloaded protamine nanocapsules with mitomycin C was comparable to the one observed for the positive control Cacicol®, a biopolymer known as a corneal wound healing enhancer. Regarding the corneal opacity, the initial grade of corneal haze (>3) induced by the photorefractive keratectomy was more rapidly reduced in the case of the positive control, Cacicol®, than in corneas treated with the nanocapsules. In conclusion, this work shows that drug-free arginine-rich (polyarginine, protamine) nanocapsules exhibit a positive behavior with regard to their potential use for corneal wound healing.


The Journal of Comparative Neurology | 2018

Morphological and functional changes in TRPM8-expressing corneal cold thermoreceptor neurons during aging and their impact on tearing in mice

Ignacio Alcalde; Almudena Íñigo-Portugués; Omar González-González; Laura Almaraz; Enol Artime; Cruz Morenilla-Palao; Juana Gallar; Félix Viana; Jesus Merayo-Lloves; Carlos Belmonte

Morphological and functional alterations of peripheral somatosensory neurons during the aging process lead to a decline of somatosensory perception. Here, we analyze the changes occurring with aging in trigeminal ganglion (TG), TRPM8‐expressing cold thermoreceptor neurons innervating the mouse cornea, which participate in the regulation of basal tearing and blinking and have been implicated in the pathogenesis of dry eye disease (DED). TG cell bodies and axonal branches were examined in a mouse line (TRPM8BAC‐EYFP) expressing a fluorescent reporter. In 3 months old animals, about 50% of TG cold thermoreceptor neurons were intensely fluorescent, likely providing strongly fluorescent axons and complex corneal nerve terminals with ongoing activity at 34°C and low‐threshold, robust responses to cooling. The remaining TRPM8+ corneal axons were weakly fluorescent with nonbeaded axons, sparsely ramified nerve terminals, and exhibited a low‐firing rate at 34°C, responding moderately to cooling pulses as do weakly fluorescent TG neurons. In aged (24 months) mice, the number of weakly fluorescent TG neurons was strikingly high while the morphology of TRPM8+ corneal axons changed drastically; 89% were weakly fluorescent, unbranched, and often ending in the basal epithelium. Functionally, 72.5% of aged cold terminals responded as those of young animals, but 27.5% exhibited very low‐background activity and abnormal responsiveness to cooling pulses. These morpho‐functional changes develop in parallel with an enhancement of tears basal flow and osmolarity, suggesting that the aberrant sensory inflow to the brain from impaired peripheral cold thermoreceptors contributes to age‐induced abnormal tearing and to the high incidence of DED in elderly people.


Physiology & Behavior | 2017

Assessing the brain through the eye: New ways to explore hepatic encephalopathy

Natalia Arias; Marta Méndez; Ignacio Alcalde; Almudena Íñigo-Portugués; Jesus Merayo-Lloves; Jaime Arias; Jorge L. Arias

BACKGROUND & AIMS Minimal hepatic encephalopathy (mHE) has been shown to affect daily functioning, quality of life, driving and overall mortality. However, little is known about treating or diagnosing early impairments in mHE. We studied one of its precipitating factors, portal hypertension which is driving the inflammatory process behind mHE. The purpose was to describe an indirect diagnostic method able to detect the pathology at early stages based on the study of the vascularization and mast cells conjunctival hyperplasia as secondary inflammatory response associated to portal hypertension. Finally, we correlated the presence of histological changes in the eye in mHE with deficits in behavioral task acquisition. METHODS Rats were trained on a stimulus-response task and a spatial working memory task using the Morris water maze. Two groups of animals were used: a SHAM (sham-operated) group (n=10) and a portal hypertension (HT) group (n=10). The triple portal vein ligation method was used to create an animal model of mHE. Latencies to reach the platform, number of glial fibrillary acidic protein-immunoreactive astrocytes (GFAP-IR), mast cell expression and presence/absence of blood and lymphatic vessels were examined. RESULTS There were differences in stimulus-response behavioral performance, with a deficit in the acquisition in the HT group. However, no differences between groups were found on the spatial working memory task. At the same time, differences between groups were found in the GFAP-IR density, which was lower in the HT group, and in the number of mast cells and the presence of vessels, which were higher in the HT group. CONCLUSIONS In this study, we provide the first preliminary insight into the validity of exploring the eye as a possible tool to assess the diagnosis of mHE conditions.


Archivos de la Sociedad Española de Oftalmología | 2015

Effects of new biomimetic regenerating agents on corneal wound healing in an experimental model of post-surgical corneal ulcers☆

Ignacio Alcalde; Almudena Íñigo-Portugués; N. Carreño; A.C. Riestra; Jesus Merayo-Lloves


Investigative Ophthalmology & Visual Science | 2016

AGING EFFECTS ON CORNEAL COLD THERMORECEPTOR NEURONS AND CORNEAL NERVES ARE RELATED WITH CHANGES IN BASAL TEARING AND BLINKING RATES

Almudena Íñigo-Portugués; Omar Gonzalez Gonzalez; Ignacio Alcalde; Federico Bech; Juana Gallar; Jesus Merayo-Lloves; Carlos Belmonte


Investigative Ophthalmology & Visual Science | 2016

Morphological and functional characteristics of regenerating corneal nerves in mice following photorefractive surgery

Omar Gonzalez Gonzalez; Federico Bech; Ignacio Alcalde; Almudena Íñigo-Portugués; Jesus Merayo-Lloves; Carlos Belmonte


Investigative Ophthalmology & Visual Science | 2015

FUNTIONAL ACTIVITY OF CORNEAL COLD SENSORY NERVE TERMINALS AND BASAL TEARING RATE IN YOUNG AND AGED MICE

Omar Gonzalez Gonzalez; Ignacio Alcalde; Almudena Íñigo-Portugués; Juana Gallar; Jesus Merayo-Lloves; Carlos Belmonte


Investigative Ophthalmology & Visual Science | 2015

Induction of experimental keratoconic ectasias by Endo-β-Galactosidase extracellular matrix digestion

Federico Bech; Ignacio Alcalde; Almudena Íñigo-Portugués; Paola Braga; Enol Artime; Beatriz García; José F. Alfonso; Jesus Merayo-Lloves


Investigative Ophthalmology & Visual Science | 2015

EFFECTS OF AGING ON NEUROCHEMICAL PROPERTIES OF MOUSE CORNEAL COLD SENSORY NEURONS, CHANGES IN MORPHOLOGY IN THEIR AFFERENT PROJECTIONS AND IMPLICATIONS IN BASAL TEAR SECRETION

Almudena Íñigo-Portugués; Ignacio Alcalde; Omar Gonzalez Gonzalez; Juana Gallar; Jesus Merayo-Lloves; Carlos Belmonte


Investigative Ophthalmology & Visual Science | 2014

REDUCED NUMBER AND ALTERED FUNCTIONAL ACTIVITY OF MOUSE CORNEAL COLD SENSORY NERVE FIBERS WITH AGE DEVELOP IN PARALLEL WITH DECREASED BASAL TEARING

Omar Gonzalez Gonzalez; Ignacio Alcalde; Almudena Íñigo-Portugués; Juana Gallar; Jesus Merayo-Lloves; Carlos Belmonte

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Carlos Belmonte

Spanish National Research Council

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Juana Gallar

Spanish National Research Council

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