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Dive into the research topics where Juan R. Cortés is active.

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Featured researches published by Juan R. Cortés.


Journal of Autoimmunity | 2013

Sjögren's syndrome and the epithelial target: A comprehensive review

M.-J. Barrera; Bahamondes; D. Sepúlveda; Andrew F.G. Quest; Isabel Castro; Juan R. Cortés; Sergio Aguilera; Ulises Urzúa; C. Molina; Patricia Ewert; Cecilia Alliende; Marcela A. Hermoso; Sergio González; Cecilia Leyton; M.-J. González

The most difficult component in our understanding of human autoimmunity remains a rigorous dissection of etiological events. Indeed, the vast literature on autoimmune diseases focuses on the inflammatory response, with the hope of developing drugs that reduce inflammation. However, there is increasing recognition that understanding the immunobiology of target tissues will also have direct relevance to disease natural history, including breach of tolerance. Sjögrens syndrome is essentially an epitheliitis and there are major changes to normal architectural salivary organization. We propose that loss of homeostasis is the initial event that precipitates inflammation and that such inflammatory response includes not only the adaptive response, but also an intense innate immune/bystander response. To understand these events this review focuses on the architecture, phenotype, function and epithelial cell organization. We further submit that there are several critical issues that must be defined to fully understand epithelial cell immunobiology in Sjögrens syndrome, including defining epithelial cell polarity, cell-cell and cell to extracellular matrix interactions and a variety of chemical and mechanical signals. We also argue that disruption of tight junctions induces disorganization of the apical pole of salivary acinar cells in Sjögrens syndrome. In addition, there will be a critical role of inflammatory cytokines in the apico-basal relocation of tight junction proteins. Further, the altered disorganization and relocation of proteins that participate in secretory granule formation are also dysregulated in Sjögrens syndrome and will contribute to abnormalities of mucins within the extracellular matrix. Our ability to understand Sjögrens syndrome and develop viable therapeutic options will depend on defining these events of epithelial cell biology.


Autoimmunity Reviews | 2013

Oral dryness in Sjögren's syndrome patients. Not just a question of water

Isabel Castro; D. Sepúlveda; Juan R. Cortés; Andrew F.G. Quest; M.-J. Barrera; V. Bahamondes; Sergio Aguilera; Ulises Urzúa; Cecilia Alliende; C. Molina; Sergio González; Marcela A. Hermoso; Cecilia Leyton; M.-J. González

Sjögrens syndrome (SS) is a chronic autoimmune disease of undefined etiology. Patients with this syndrome suffer from severe alterations in both the quality and quantity of saliva and tears, due to impaired function of the relevant exocrine glands. Prevalent symptoms experienced by SS-patients include a persistent dry mouth sensation (xerostomia) and dry eyes (keratoconjunctivitis sicca). Water content of saliva depends of acetylcholine levels, glandular innervation, M3R signaling, calcium tunneling and water release, among other factors. However, unstimulated salivary flow correlates only poorly with symptoms of mouth dryness, raising the question as to which other components of saliva may be involved in mouth dryness experienced by SS-patients? Salivary mucins are glycoproteins characterized by the presence of large oligosaccharide side chains attached to the protein backbone. These molecules are key saliva components that are required to sequester water and thereby moisturize, as well as lubricate the oral mucosa. In the labial salivary glands of SS patients, morphological and functional alterations are detectable that affect the maturation and trafficking of salivary mucins. In this review, we will focus the discussion on these aspects of reduced salivary flow and decreased quality of salivary mucins, since they are likely to be responsible for xerostomia in SS-patients.


Rheumatology | 2015

Salivary mucins induce a Toll-like receptor 4-mediated pro-inflammatory response in human submandibular salivary cells: are mucins involved in Sjögren’s syndrome?

María-José Barrera; Sergio Aguilera; Enno C. I. Veerman; Andrew F.G. Quest; David Díaz-Jiménez; Ulises Urzúa; Juan R. Cortés; Sergio González; Isabel Castro; C. Molina; V. Bahamondes; Cecilia Leyton; Marcela A. Hermoso; María-Julieta González

OBJECTIVES A hallmark characteristic of SS patients is the ectopic presence of the mucins MUC5B and MUC7 in the extracellular matrix of salivary glands that have lost apical-basolateral acinar-cell polarity. This study aims to determine whether exogenous salivary mucins induce gene expression of pro-inflammatory cytokines, as well as to evaluate whether the Toll-like receptor-4 (TLR4) pathway is involved in this response. METHODS Differentiated human submandibular gland (HSG) cells were stimulated with mucins or oligosaccharide residues at different concentrations and for different periods of time. The expression of pro-inflammatory cytokines and their receptors was determined by semi-quantitative real time PCR (sqPCR). TLR4-mediated responses induced by mucin were evaluated with the Toll-IL-1 receptor domain containing adaptor protein (TIRAP) inhibitory peptide or using anti-hTLR4 blocking antibody. TLR4-receptor expression was also determined in SS patients, controls and HSG cells. RESULTS Mucins induced a significant increase in CXCL8, TNF-α, IFN-α, IFN-β, IL-6 and IL-1β, but not B cell activating factor (BAFF). Cytokine induction was mediated by TLR4, as shown using TIRAP or using anti-hTLR4 antibody. Sugar residues present in MUC5B, such as sulpho-Lewis (SO3-3Galβ1-3GlcNAc), also induced cytokines. Unexpectedly, mucins induced MUC5B, but not MUC7 expression. CONCLUSION Salivary mucins were recognized by TLR4 in epithelial cells initiating a pro-inflammatory response that could attract inflammatory cells to amplify and perpetuate inflammation and thereby contribute to the development of a chronic state characteristic of SS. The ectopic localization of MUC5B and MUC7 in the salivary gland extracellular matrix from SS patients and the current results reveal the importance of salivary epithelial cells in innate immunity, as well as in SS pathogenesis.


Astrophysical Journal Supplement Series | 2014

Integral-Field Stellar and Ionized Gas Kinematics of Peculiar Virgo Cluster Spiral Galaxies

Juan R. Cortés; Jeffrey D. P. Kenney; Eduardo Hardy

We present the stellar and ionized gas kinematics of 13 bright peculiar Virgo cluster galaxies observed with the DensePak Integral Field Unit at the WIYN 3.5-meter telescope, to seek kinematic evidence that these galaxies have experienced gravitational interactions or gas stripping. 2-Dimensional maps of the stellar velocity


Publications of the Astronomical Society of Japan | 2007

A Search for CO (J = 3–2) Emission from the Host Galaxy of GRB 980425 with the Atacama Submillimeter Telescope Experiment

Bunyo Hatsukade; Kotaro Kohno; A. Endo; Tomoka Tosaki; Kouji Ohta; Seiichi Sakamoto; Nobuyuki Kawai; Juan R. Cortés; Kouichiro Nakanishi; Takeshi Okuda; Kazuyuki Muraoka; Takeshi Sakai; Paul M. Vreeswijk; Hajime Ezawa; Nobuyuki Yamaguchi; Kazuhisa Kamegai; Ryohei Kawabe

V


Publications of the Astronomical Society of Japan | 2008

ASTE CO(3-2) Observations of the Southern Barred Spiral Galaxy NGC 986: a Large Gaseous Bar Filled with a Dense Molecular Medium

Kotaro Kohno; Tomoka Tosaki; Rie Miura; Kazuyuki Muraoka; Tsuyoshi Sawada; Kouichiro Nakanishi; Nario Kuno; Takeshi Sakai; Kazuo Sorai; Kazuhisa Kamegai; Kunihiko Tanaka; Takeshi Okuda; Akira Endo; Bunyo Hatsukade; Masahiro Sameshima; Hajime Ezawa; Seiichi Sakamoto; Takeshi Kamazaki; Nobuyuki Yamaguchi; Juan R. Cortés; Yoichi Tamura; Masayuki Fukuhara; Daisuke Iono; Ryohei Kawabe

, and stellar velocity dispersion


Annals of the Rheumatic Diseases | 2015

SAT0380 Impaired Ire1Alpha/XBP-1 Pathway is Associated with Glandular Dysfunction in SjÖgren's Syndrome

D. Sepúlveda; Sergio Aguilera; M.-J. Barrera; V. Bahamondes; Isabel Castro; C. Molina; Juan R. Cortés; Sergio González; Cecilia Leyton; M.-J. González

\sigma


Annals of the Rheumatic Diseases | 2016

OP0271 Perk Pathway Characterization in Labial Salivary Glands of Sjögren Syndrome's Patients: Could It Be An Adaptive Response?

V. Bahamondes; Sergio Aguilera; Juan R. Cortés; Isabel Castro; M.-J. Barrera; Ulises Urzúa; Sergio González; C. Molina; Cecilia Leyton; M.-J. González

and the ionized gas velocity (H


Proceedings of SPIE | 2014

Status of ALMA offline software in the transition from construction to full operations

Daniel Espada; Masao Saito; L.-Å. Nyman; Juan R. Cortés; A. D. Biggs; Felix Stoehr; Itziar de Gregorio; Stephane Leon; Ruediger Kneissl; Liz Humphreys; Emilio Barrios; G. Mathys; Thomas Wiklind; Crystal Lee Brogan; Carol J. Lonsdale; Anthony J. Remijan; Baltasar Vila-Vilaro; Eric Villard; Andreas A. Lundgren; Paola Andreani; Ken'ichi Tatematsu; John E. Hibbard

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Archive | 2008

A Possible Detection of CO (J = 3–2) Emission from the Host Galaxy of GRB980425 with the Atacama Submillimeter Telescope Experiment

Kouji Ohta; Seiichi Sakamoto; Nobuyuki Kawai; Juan R. Cortés; Kouichiro Nakanishi; Takeshi Okuda; Kazuyuki Muraoka; Takeshi Sakai; Hajime Ezawa; Nobuyuki Yamaguchi; Kazuhisa Kamegai; Ryohei Kawabe; Bunyo Hatsukade; Kotaro Kohno; Akira Endo; Tomoka Tosaki

and/or [\ion{O}{3}]) are presented for galaxies in the sample. The stellar rotation curves and velocity dispersion profiles are determined for 13 galaxies, and the ionized gas rotation curves are determined for 6 galaxies. Misalignments between the optical and kinematical major axis are found in several galaxies. While in some cases this is due to a bar, in other cases it seems associated with a gravitational interaction or ongoing ram pressure stripping. Non-circular gas motions are found in nine galaxies, with various causes including bars, nuclear outflows, or gravitational disturbances. Several galaxies have signatures of kinematically distinct stellar components, which are likely signatures of accretion or mergers. We compute for all galaxies the angular momentum parameter

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