7 results on '"J. F. Muñoz-Valle"'
Search Results
2. Expression of BAFF and BAFF receptors in primary Sjögren’s syndrome patients with ectopic germinal center-like structures
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F. J. Carrillo-Ballesteros, C. A. Palafox-Sánchez, R. A. Franco-Topete, J. F. Muñoz-Valle, G. Orozco-Barocio, G. E. Martínez-Bonilla, C. E. Gómez-López, M. Marín-Rosales, E. F. López-Villalobos, S. Luquin, A. Castañeda-Chávez, and Edith Oregon-Romero
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Adult ,Male ,musculoskeletal diseases ,0301 basic medicine ,medicine.medical_specialty ,Transmembrane Activator and CAML Interactor Protein ,medicine.medical_treatment ,Salivary Glands, Minor ,Severity of Illness Index ,General Biochemistry, Genetics and Molecular Biology ,Immunophenotyping ,Pathogenesis ,03 medical and health sciences ,0302 clinical medicine ,stomatognathic system ,Internal medicine ,B-Cell Activating Factor ,medicine ,Humans ,B-Cell Maturation Antigen ,skin and connective tissue diseases ,B-cell activating factor ,Receptor ,Aged ,Hematology ,business.industry ,Germinal center ,General Medicine ,Middle Aged ,Germinal Center ,medicine.disease ,Sialadenitis ,eye diseases ,Pathophysiology ,stomatognathic diseases ,Sjogren's Syndrome ,030104 developmental biology ,Cytokine ,Case-Control Studies ,030220 oncology & carcinogenesis ,Immunology ,Female ,business ,B-Cell Activation Factor Receptor - Abstract
B cell-activating factor (BAFF) is an essential cytokine in primary Sjogren’s syndrome (pSS) physiopathology. It has been reported that pSS patients develop germinal center-like (GC-like) structures in their minor salivary glands (MSGs). BAFF, BAFF-R, TACI, and BCMA expression was analyzed in MSGs from 29 subjects (nonspecific chronic sialadenitis and focal lymphocytic sialadenitis with the presence [pSS-GC(+)] or absence [pSS-GC(−)] of GC-like structures). Twenty-four percent of patients showed ectopic GC-like structures and a high focus score [p
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- 2020
3. A differential sex-specific pattern of IgG2 and IgG4 subclasses of anti-drug antibodies (ADAs) induced by glatiramer acetate in relapsing-remitting multiple sclerosis patients
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Sonia Mayra Pérez-Tapia, J. F. Muñoz-Valle, Mario A. Mireles-Ramírez, Daniel Ortuño-Sahagún, Gilberto Pérez-Sánchez, José de Jesús Guerrero-García, Emilio Medina-Rivero, Enrique Becerril-Villanueva, Lenin Pavón, Sandra Avila, Argelia E. Rojas-Mayorquín, and Luis Vallejo-Castillo
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Drug ,Adult ,Male ,media_common.quotation_subject ,Subclass ,03 medical and health sciences ,Interferon-gamma ,0302 clinical medicine ,Multiple Sclerosis, Relapsing-Remitting ,medicine ,Humans ,In patient ,030212 general & internal medicine ,Glatiramer acetate ,media_common ,Sex Characteristics ,biology ,business.industry ,Multiple sclerosis ,General Medicine ,Glatiramer Acetate ,medicine.disease ,Sex specific ,Neurology ,Relapsing remitting ,Immunoglobulin G ,Immunology ,biology.protein ,Female ,Neurology (clinical) ,Antibody ,business ,030217 neurology & neurosurgery ,Immunosuppressive Agents ,medicine.drug - Abstract
Background Glatiramer acetate (GA) is a drug for Multiple Sclerosis (MS) treatment. However, its administration induces anti-drug antibodies (ADA). This research evaluated the sex differences in humoral response against GA in RR-MS patients Methods We analyzed 69 RR-MS patients, 43 treated with GA and 26 treated with IFN-β. In all cases, the serum concentration of IgG antibodies was determined by UPLC, whereas the levels of IgG subclasses (1–4) of anti-GA antibodies and the concentration of IL-6 were detected by Multiplex and IL-10, and IFN-γ were detected by ELISA. Results The total concentration of IgG antibodies in patients did not differ between treatments, whereas the IgG levels of ADA were higher in male and female patients treated with GA (P ≤ 0.0001). The subclasses of IgG anti-GA antibodies were as follows: IgG4>>IgG3>IgG1>IgG2. Statistical analysis showed differences in the IgG2 (P ≤ 0.01) and IgG4 (P ≤ 0.0001) subclasses by sex in RR-MS patients. Levels of IgG1 subclass in male patients correlated positively with the circulatory levels of IL-6 (rs = 0.587, P ≤ 0.04) and IFN-γ (rs = 0.721, P ≤ 0.001), while IgG2 subclass levels in female patients correlated with serum levels of IFN-γ (rs = 0.628, P ≤ 0.0006). Statistical analysis did not detect correlations between the levels of IgG (1–4) subclasses of anti-GA antibodies and the evaluated clinical parameters. Conclusion This study showed differences in the levels of IgG2 and IgG4 subclasses of ADA between male and female RR-MS patients. Further studies are necessary to take advantage of the clinical potential of this finding.
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- 2019
4. AB0016 ASSOCIATION OF PTPN22 GENETIC VARIANTS WITH DISEASE SUSCEPTIBILITY AND CLINICAL VARIABLES IN PRIMARY SJÖGREN SYNDROME
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J. F. Muñoz Valle, D. C. Salazar Camarena, P. A. Menchaca Tapia, E. Oregón Romero, M. Marin Rosales, and C. A. Palafox Sánchez
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medicine.medical_specialty ,education.field_of_study ,business.industry ,Immunology ,Population ,Heterozygote advantage ,Disease ,medicine.disease_cause ,medicine.disease ,Ulcerative colitis ,General Biochemistry, Genetics and Molecular Biology ,Rheumatology ,Autoimmunity ,PTPN22 ,Internal medicine ,Genotype ,medicine ,Immunology and Allergy ,business ,education - Abstract
Background:Primary Sjögren’s syndrome (pSS) is a systemic autoimmune disease characterized by dysfunction of exocrine glands secondary to lymphocytic infiltration. Lymphoid tyrosine phosphatase (LYP) regulates T and B lymphocyte activation.PTPN22gene encodes LYP; multiple polymorphic variants have been described as genetic risk factor of autoimmune diseases.Objectives:The aim was to analyze thePTPN22rs2488457G>C, rs33996649G>A, and rs2476601C>T genetic variants relationship with the development risk of pSS in the western Mexico population.Methods:One hundred and eighty healthy subjects (HS) and 150 pSS patients, classified according to EULAR 2016 criteria, were included. The genetic variants and mRNA expression were determined through PCR-RFLP and qPCR assays.Results:The frequency of heterozygote rs33996649GA genotype was higher in pSS patients than HS [OR=3.143 (1–10.234), p=0.046], and also, rs33996649GA genotype was associated with high SSDAI score (p=0.01). The pSS patients showed 44-fold more mRNA expression in comparison with HS (p=0.002), and mRNA expression correlates with SSDAI (r2=0.512, p=0.006).Conclusion:The rs33996649G>A genetic variant of thePTPN22gene is associated with increased development risk of pSS in the western Mexican population. The expression mRNA correlates with disease activity in pSS.References:[1]Brito-Zerón, P., Baldini, C., Bootsma, H., Bowman, S. J., Jonsson, R., Mariette, X., Ramos-Casals, M. (2016). Sjögren syndrome.Nature Reviews Disease Primers, 2(July), 1–20.https://doi.org/10.1038/nrdp.2016.47[2]Stanford, S. M., & Bottini, N. (2014). PTPN22: The archetypal non-HLA autoimmunity gene.Nature Reviews Rheumatology,10(10), 602–611.https://doi.org/10.1038/nrrheum.2014.109[3]Chen, Z., Zhang, H., Xia, B., Wang, P., Jiang, T., Song, M., & Wu, J. (2013). Association of PTPN22 gene (rs2488457) polymorphism with ulcerative colitis and high levels of PTPN22 mRNA in ulcerative colitis.International Journal of Colorectal Disease,28(10), 1351–1358.https://doi.org/10.1007/s00384-013-1671-3[4]Machado-Contreras, J. R., Muñoz-Valle, J. F., Cruz, A., Salazar-Camarena, D. C., Marín- Rosales, M., & Palafox-Sánchez, C. A. (2016b). Distribution of PTPN22 polymorphismsin SLE from western Mexico: correlation with mRNA expression and disease activity.Clinical and Experimental Medicine,16(3), 399–406.https://doi.org/10.1007/s10238-015-0359-0Disclosure of Interests:None declared
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- 2020
5. Rheumatoid arthritis and other inflammatory joint diseases (human studies) (PP-036)
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G. P. Nolan, T. Kinoshita, C. Lam, A. Grützkau, N. Lee, M. Horiuchi, M. Mackay, T. Tomita, T. Sumida, J. Tebib, S. Ohnishi, S. Tsujimura, N. Umeda, R. Burgos-Vargas, Y. Asanuma, C. Ionita, L. Limón-Camacho, K. Yasui, J. M. Witkowski, H. Ionita, H. Kajiyama, T. Naka, S. Tominaga, F. Miyoshi, C. Schütz, S. Hirohata, H. Amuro, M. Iwamoto, I. P. Guzmán-Guzmán, N. Miyasaka, Y. Araki, D. Naysmith, E. Meugnier, J. Kong, Y. Valle, T. N. Shibata, T. J. A. Lehman, M. García-García, Y. Yoshikai, W. Lee, I. Hideya, B. Thumthanaruk, Z. Smolenska, L. Kremer, M. Lu, T. Atsumi, Y. Hwang, J. Saegusa, A. Manki, M. Soroczynska-Cybula, T. Klaiwong, L. Jiang, V. Paunescu, P. Charles, T. Wada, E. Humphreys, B. Prakken, M. Kato, J. Sibilia, H. Ozaki, K. Watanabe, F. Terabe, R. E. Navarro-Hernández, D. Hull, K. Shimamoto, H. Kataoka, H. Okazaki, K. Yokota, B. Wang, G. Mijnheer, J. L. Huang, H. Aizawa, S. Blazickova, L. Llorente, T. Kishimoto, J. Pawlowska, H. Vidal, A. Morinobu, M. Fujita, S. Abraham, T. Avčin, N. H. Fabien, A. Palfreeman, S. Castañeda, P. Taylor, X. Chang, T. Morishima, Y. Tanaka, H. Khalili, A. S. Williams, J. R. Grün, I. Gonzalez-Alvaro, Y. Nasuhara, R. Minami, T. Takii, D. Pramod, G. Manda, A. Ortiz, K. Saito, I. Matsumoto, H. Ishibashi, S. Fukuhara, P. Wu, H. Itoh, M. Mizushima, M. Nakamura, C. C. Liao, Y. Onodera, T. Koike, P. Bowness, S. Ito, J. Chen, Y. Fujieda, S. Takei, R. Amakawa, A. Radbruch, S. A. Alzabin, A. Inoue, J. Jiang, A. Ma, K. Sawai, I. Y. Ledezma-Lozano, H. Chen, M. Vargas-Rojas, J. M. Salvador, I. V. Neagoe, R. Straub, M. Lopez-Santalla, K. Matsuo, H. Imaoka, J. Sieper, S. Ozaki, J. Bienvenu, H. Yu, H. Maeng, M. Fujimoto, A. Bucur, T. Nanki, Y. Matsuyama, R. Miyamoto, W. Maśliński, W. F. N. Chan, R. M. Goodfellow, C. Ferraro-Peyret, H. Bang, F. Batliwalla, M. Hoshino, K. Kaneko, S. Nomoto, R. S. Sadler, H. Yamada, S. Bae, M. Kosmač, K. Misaki, K. Sato, B. Diamond, B. L. Ferry, K. Otomo, F. Coury, A. R. Balanescu, T. Nishikawa, J. L. Nelson, N. Toplak, J. Kang, D. Zhang, F. Jones, C. Aranow, Y. Son, J. Ptacek, A. Komori, V. Cortez, N. van der Westhuizen, K. Onozaki, S. Tanaka, M. Steinbrich-Zöllner, P. K. Gregersen, H. Rangel-Villalobos, D. Chen, M. Inoue, M. Vázquez-Del Mercado, T. Hayashi, T. Kimata, U. Skalska, N. Eiró, S. Buranapraditkun, T. Hoshino, Y. Yu, Z. Newton, M. A. Llamas-Covarrubias, E. Bryl, H. Igarashi, M. Sawada, C. M. Chang, H. Tamemoto, A. Oyamada, Z. Rahman, F. Roncal, C. J. Calder, J. Rovensky, M. Herold, C. Martínez-A, J. F. Muñoz-Valle, E. C. Wang, K. Nakajima, J. Woo, S. Serada, T. Horita, D. Halbritter, Y. Akiyama, S. Minota, M. Tsuge, S. Yasuda, H. Huang, C. Probst, S. Itoh, S. Kumagai, T. Ito, C. A. Roberts, S. Capellino, J. Mulero, M. Yamasaki, T. Mori, N. Lai, H. Kim, M. Fleck, H. Oda, V. Čurin Šerbec, Y. Ozaki, S. Okamoto, R. Cimaz, S. Rome, J. Schölmerich, N. Jeerapadungkiat, T. Mimura, A. Tuchynova, L. Albulescu, R. Williams, P. Ammaranond, S. Sato, D. Goto, H. Yoshikawa, C. J. Atkins, G. Cioaca, C. Wong, M. Salvador-Bernaldez, K. Ishihara, V. Preoteasa, A. Daca, I. Ionita, E. Kontny, F. van Wijk, M. B. Hale, K. Yuge, Y. Sakazaki, E. J. Wehrens, and K. Migita
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Human studies ,business.industry ,Rheumatoid arthritis ,Immunology ,medicine ,Immunology and Allergy ,General Medicine ,medicine.disease ,business ,Joint (geology) - Published
- 2010
6. Assessment of the TNF-A RS1799964 (-1031T>C) polymorphism and soluble protein concentration in acute coronary syndrome: association with circulating levels
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J. F. Muñoz Valle, A. Valdez Haro, F. Rivas, Yeminia Valle, I.J. García González, J.R. Padilla Gutiérrez, E. Valdes Alvarado, H.E. Flores Salinas, and E. Sandoval Pinto
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medicine.medical_specialty ,Acute coronary syndrome ,Endocrinology ,business.industry ,Internal medicine ,medicine ,Tumor necrosis factor alpha ,Cardiology and Cardiovascular Medicine ,medicine.disease ,business ,Protein concentration - Published
- 2015
7. Genotype Ser413/Ser of PAI-2 polymorphism Ser413/Cys is associated with anti-phospholipid syndrome and systemic lupus erythematosus in a familial case: comparison with healthy controls
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Victor E. Arana-Argaez, J. F. Muñoz Valle, C R Best-Aguilera, B T Martín-Márquez, Lourdes Nuñez-Atahualpa, Vidal Delgado-Rizo, M Vázquez-Del Mercado, E-A Martínez-García, Nora Magdalena Torres-Carrillo, T A García-Cobian, and Marcelo H. Petri
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Proband ,Male ,Systemic disease ,Genotype ,Immunology ,medicine.disease_cause ,Autoimmunity ,symbols.namesake ,Rheumatology ,medicine ,Plasminogen Activator Inhibitor 2 ,Immunology and Allergy ,Humans ,Lupus Erythematosus, Systemic ,Child ,Lupus erythematosus ,Polymorphism, Genetic ,business.industry ,General Medicine ,medicine.disease ,Antiphospholipid Syndrome ,Genotype frequency ,Pedigree ,Mendelian inheritance ,symbols ,Female ,Restriction fragment length polymorphism ,business - Abstract
We describe a family with a 7-year-old proband case diagnosed with systemic lupus erythematosus (SLE) plus secondary anti-phospholipid syndrome (APS) as well as two affected paternal aunts. We compared the frequency of these polymorphisms with healthy controls.To evaluate the mode of inheritance in this familial case of APS and SLE and the possible association of plasminogen activator inhibitor-1 (PAI-1) -675 4G/5G and PAI-2 Ser(413)/Cys polymorphisms. To compare the genotype frequency of these polymorphisms with the results found in a Mexican Mestizo population.PAI-1 -675 4G/5G and PAI-2 Ser(413)/Cys were determined by the polymerase chain reaction restriction fragment length polymorphism (PCR-RFLP) technique using Bsl I and Mwo I on four generations of the family studied. PAI-2 Ser(413)/Cys polymorphism was also determined in 50 healthy individuals of Mexican Mestizo origin.The family pedigree demonstrated that this family did not follow a Mendelian inheritance pattern. When the PAI-2 Ser(413)/Cys polymorphism was examined, we found that 60% (3/5) of the relatives homozygous to Ser(413)/Ser were affected with SLE and/or APS (p = 0.027). The proband case was 4G/5G genotype for the PAI-1 -675 4G/5G polymorphism. No differences between healthy controls of the Mexican Mestizo population and the family studied for the PAI-2 Ser(413)/Cys polymorphism or PAI-1 -675 4G/5G polymorphisms were found.Our data indicate that this family did not follow the Mendelian inheritance pattern. The Ser(413)/Ser genotype demonstrated in 60% of the affected members (3/5) of this family might increase the risk for autoimmune syndromes such as APS or SLE.
- Published
- 2007
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