Your search keyword '"González Quintanilla, Vicente"' showing total 8 results

1. Differences in circulating alpha‐calcitonin gene–related peptide levels in inflammatory bowel disease and its relation to migraine comorbidity: A cross‐sectional study.

Author

Pascual‐Mato, Marta, Gárate, Gabriel, González‐Quintanilla, Vicente, Madera‐Fernández, Jorge, Castro, Beatriz, García, María José, Crespo, Javier, Rivero, Montserrat, and Pascual, Julio

Subjects

RISK assessment, CROSS-sectional method, CROHN'S disease, RESEARCH funding, BRAIN, INTERVIEWING, ENZYME-linked immunosorbent assay, CALCITONIN, GASTROINTESTINAL system, DESCRIPTIVE statistics, ULCERATIVE colitis, INFLAMMATORY bowel diseases, GENES, NEUROPEPTIDES, COMPARATIVE studies, MIGRAINE, COMORBIDITY, DISEASE risk factors, DISEASE complications

Abstract

Objective: To analyze the specificity of calcitonin gene–related peptide (CGRP) levels, we measured alpha‐CGRP circulating levels in a large series of patients with a recent diagnosis of inflammatory bowel disease (IBD) who were interviewed regarding comorbid headache. Background: Several studies have found an association between migraine and IBD. Methods: In this cross‐sectional study performed in an IBD clinic, morning serum alpha‐CGRP levels were measured by enzyme‐linked immunosorbent assay in 96 patients who were recently diagnosed with IBD and compared to those from 50 similar patients with chronic migraine (CM) and 50 healthy controls (HC). Results: Alpha‐CGRP levels were higher in patients with IBD (median [interquartile range] 56.9 [35.6–73.9] pg/mL) and patients with CM (53.0 [36.7–73.9] pg/mL) compared to HC (37.2 [30.0–51.8] pg/mL; p = 0.003; p = 0.019, respectively). Regarding IBD diagnostic subtypes, alpha‐CGRP levels for ulcerative colitis (67.2 ± 49.3 pg/mL; 57.0 [35.6–73.4] pg/mL) and Crohn's disease (54.9 ± 27.5 pg/mL; 57.7 [29.1–76.1] pg/mL) were significantly higher than those of HC (p = 0.013, p = 0.040, respectively). Alpha‐CGRP levels were further different in patients with IBD with migraine (70.9 [51.8–88.7] pg/mL) compared to HC (p < 0.001), patients with IBD without headache (57.5 [33.3–73.8] pg/mL; p = 0.049), and patients with IBD with tension‐type headache but without migraine (41.7 [28.5–66.9] pg/mL; p = 0.004), though alpha‐CGRP levels in patients with IBD without migraine (53.7 [32.9–73.5] pg/mL) remained different over HC (p = 0.028). Conclusion: Together with CM, circulating alpha‐CGRP levels are different in patients with IBD, perhaps reflecting a chronic inflammatory state. IBD is an example of how alpha‐CGRP levels are not a totally specific migraine biomarker. However, alpha‐CGRP levels were further increased in patients with IBD who have a history of migraine, which reinforces its role as a biomarker in migraine patients, always bearing in mind their comorbidities. Plain Language Summary: Alpha‐calcitonin gene–related peptide (CGRP) levels may be a potential migraine biomarker, but it is unclear if this is the case because changes in CGRP concentrations can also be present in other conditions. We measured morning serum alpha‐CGRP levels in 96 patients with a recent inflammatory bowel disease (IBD) diagnosis, and compared them to 50 matched healthy participants and 50 matched patients with chronic migraine (CM). We found a significant increase in serum alpha‐CGRP levels in both patients with IBD and CM compared to healthy controls, which we think may reflect chronic inflammation found in IBD; these results offer another example that alpha‐CGRP concentrations are not totally specific for migraine. [ABSTRACT FROM AUTHOR]

Published

2024

2. Long-term safety of OnabotulinumtoxinA treatment in chronic migraine patients: a five-year retrospective study.

Author

Navarro-Pérez, María Pilar, González-Quintanilla, Vicente, Muñoz-Vendrell, Albert, Madrigal, Elisabet, Alpuente, Alicia, Latorre, Germán, Molina, Francis, Monzón, María José, Medrano, Vicente, García-Azorín, David, González-Oria, Carmen, Gago-Veiga, Ana, Velasco, Fernando, Beltrán, Isabel, Morollón, Noemí, Viguera, Javier, Casas-Limón, Javier, Rodríguez-Vico, Jaime, Cuadrado, Elisa, and Irimia, Pablo

Subjects

MIGRAINE, BOTULINUM A toxins, TERMINATION of treatment, TRAPEZIUS muscle, MUSCULAR atrophy

Abstract

Background: Real-world studies have shown the sustained therapeutic effect and favourable safety profile of OnabotulinumtoxinA (BoNTA) in the long term and up to 4 years of treatment in chronic migraine (CM). This study aims to assess the safety profile and efficacy of BoNTA in CM after 5 years of treatment in a real-life setting. Methods: We performed a retrospective chart review of patients with CM in relation to BoNTA treatment for more than 5 years in 19 Spanish headache clinics. We excluded patients who discontinued treatment due to lack of efficacy or poor tolerability. Results: 489 patients were included [mean age 49, 82.8% women]. The mean age of onset of migraine was 21.8 years; patients had CM with a mean of 6.4 years (20.8% fulfilled the aura criteria). At baseline, patients reported a mean of 24.7 monthly headache days (MHDs) and 15.7 monthly migraine days (MMDs). In relation to effectiveness, the responder rate was 59.1% and the mean reduction in MMDs was 9.4 days (15.7 to 6.3 days; p < 0.001). The MHDs were also reduced by 14.9 days (24.7 to 9.8 days; p < 0.001). Regarding the side effects 17.5% experienced neck pain, 17.3% headache, 8.5% eyelid ptosis, 7.5% temporal muscle atrophy and 3.2% trapezius muscle atrophy. Furthermore, after longerterm exposure exceeding 5 years, there were no serious adverse events (AE) or treatment discontinuation because of safety or tolerability issues. Conclusion: Treatment with BoNTA led to sustained reductions in migraine frequency, even after long-term exposure exceeding 5 years, with no evidence of new safety concerns. [ABSTRACT FROM AUTHOR]

Published

2024

3. Restless legs-like syndrome as an emergent adverse event of CGRP monoclonal antibodies: A report of two cases.

Author

González-Quintanilla, Vicente, Pérez-Pereda, Sara, González-Suárez, Andrea, Madera, Jorge, Toriello, María, and Pascual, Julio

Subjects

*MONOCLONAL antibodies, *RESTLESS legs syndrome, *ERENUMAB, *SYMPTOMS, *SYNDROMES

Abstract

Background: One of the advantages of CGRP monoclonal antibodies is their excellent safety and tolerability. However, postmarketing surveillance, is essential to detect potential rare emergent adverse events. Objectives: To report two patients who developed restless legs syndrome symptoms after treatment with CGRP antibodies. Methods and results: Two women with chronic refractory migraine, with no significant medical antecedents, developed typical restless legs syndrome symptoms 1.5 and 4 months after starting erenumab 140 mg, respectively. In case 1 symptoms resolved when erenumab was stopped for two months but reappeared on galcanezumab. In both patients migraine attacks had dramatically decreased and no iron deficiency was found. Conclusions: Even though caution is needed before establishing a causal relationship, these cases suggest that restless legs-like symptoms might be an emergent adverse event of CGRP antibodies, regardless of the mechanism of action. We propose that plastic changes in CGRP sensory fibers, which are very abundant in legs, induced by CGRP monoclonal antibodies could be the reason for restless legs syndrome development. [ABSTRACT FROM AUTHOR]

Published

2021

4. Methylation analysis of NPTX2 and SH2D5 genes in chronic migraine: A case-control study.

Author

Pérez Pereda, Sara, Toriello Suárez, María, González Quintanilla, Vicente, and Oterino, Agustín

Published

2020

5. Chronic Migraine With Apparent Loss of Response to Onabotulinum Toxin Type A Due to Local Nitroglycerin Treatment for an Anal Fissure: A Case Report.

Author

Pérez‐Pereda, Sara, González‐Quintanilla, Vicente, Madera, Jorge, and Pascual, Julio

Subjects

*BOTULINUM toxin, *MIGRAINE, *NITRIC oxide, *NITROGLYCERIN, *FISSURE in ano

Abstract

Many patients with chronic migraine are difficult to treat. We present a patient with chronic migraine with good response to onabotulinum toxin type A whose headaches worsened in clear temporal relationship to local treatment with glyceryl trinitrate for an anal fissure. Our case shows that the use, even at distance, of nitric oxide donors can be a precipitating factor for migraineurs and should be always inquired in chronic migraine patients. In addition, the presence of frequent headaches should always be ruled out before prescribing such medications. [ABSTRACT FROM AUTHOR]

Published

2020

6. Systemic and cerebral endothelial dysfunction in chronic migraine. A case-control study with an active comparator.

Author

González-Quintanilla, Vicente, Toriello, María, Palacio, Enrique, González-Gay, Miguel A., Castillo, Jesús, Montes, Silvia, Martínez-Nieto, Rosa, Fernandez, Jenifer, Rojo, Alvaro, Gutiérrez, Silvia, Pons, Enar, and Oterino, Agustín

Subjects

*MIGRAINE, *ENDOTHELIUM diseases, *CARDIOVASCULAR diseases risk factors, *CAROTID intima-media thickness, *CEREBRAL cortex diseases, *BIOMARKERS, *VASODILATION, *VASCULAR diseases, *CARDIOVASCULAR system physiology, *ENDOTHELIUM, *CASE-control method, *DISEASE complications, MIGRAINE complications

Abstract

Background and Objective: Unlike migraine and migraine with aura, little information exists regarding chronic migraine (CM) as a risk factor for cardiovascular disease. In this study we aim to determine whether an association between CM and endothelial dysfunction exists.Methods: Individuals 18 years and older diagnosed with episodic migraine (EM) and CM according to ICHD criteria were studied. After an overnight fast and abstinence from vasoactive drugs, ultrasound studies were performed and blood samples taken from patients and matched controls according to internationally agreed on protocols.Results: A total of 113 individuals were enrolled (35 CM, 37 EM, 41 controls). CM patients had a lower percentage of flow-mediated vasodilation (FMD; difference of means = 5.03%; p = 1.0E-6) and breath-holding index (BHI; difference of means 0.754; p = 2.0E-6), as well as increased carotid intima media thickness (cIMT; difference of means = 0.128 mm; p = 7.0E-5) than controls. The EM patients and controls comparison found similar, but less pronounced, differences: decreased BHI (p = 0.031), and increased cIMT (p = 0.028). Fibrinogen (r = 0.277; p = 0.006), C-reactive protein (r = 0.288; p = 0.003), and erythrocyte rate sedimentation (r = 0.298; p = 0.002) also correlated with cIMT, and inversely with BHImV and FMD.Conclusions: Migraine is associated with systemic and cerebral endothelial dysfunction demonstrated by ultrasound studies and biological markers. The degree of these changes was strongly associated with the severity of migraine. Our data indicate that migraine may be a cerebral disorder with systemic endothelial damage. [ABSTRACT FROM AUTHOR]

Published

2016

7. Antibodies anti-CGRP in migraine: medium-long term experience

Author

Gilot Sancho, Marina, Pascual Gómez, Julio, González Quintanilla, Vicente, and Universidad de Cantabria

Subjects

Migraña crónica, Monoclonal antibodies anti-CGRP (MAB), MC, Anticuerpos anti-CGRP, Migraña, Migraine, Chronic migraine

Abstract

RESUMEN : Introducción: Las cefaleas son el motivo de consulta más habitual en neurología, y, concretamente, la migraña es la entidad más relevante en frecuencia y discapacidad. La prevalencia y el impacto en la calidad de vida de los pacientes, junto con el conocimiento de la fisiopatología de esta enfermedad, han favorecido el desarrollo de nuevas líneas terapéuticas específicas como los anticuerpos antiCGRP, indicados solo en pacientes con migraña crónica refractaria. Actualmente se recomienda la retirada del tratamiento a los 12 meses, sin embargo, se desconoce qué ocurre tras su suspensión. Por lo tanto, son necesarios nuevos estudios en vida real que analicen en la práctica clínica real la experiencia tras un año de tratamiento. Objetivos: Analizar la experiencia en la práctica clínica real en pacientes con migraña crónica (MC) tratados con anticuerpos antiCGRP durante un año y tras su retirada. Metodología: Recogida prospectiva de parámetros demográficos y de eficacia de los pacientes de la Unidad de Cefaleas del Servicio de Neurología del Hospital Universitario Marqués de Valdecilla (HUMV) con MC que habían iniciado tratamiento con los nuevos anticuerpos anti-CGRP. Se recogieron los datos al inicio, y trimestralmente, si bien aquí nos centraremos en la experiencia al año de tratamiento. Se administraron dos fármacos: erenumab (en dosis de 70 y 140 mg) y galcanezumab (240 mg subcutáneas en primer mes y posteriormente 120 mg al mes), según su ficha técnica. Resultados: De los 61 pacientes que completaron el tratamiento anual, todos cumplían criterios de MC de larga evolución (9,5 años de media). La media de edad fue de 48,4 años (18-66 años) y la mayoría eran mujeres (57; 90,5 %). Tras 12 meses con los anticuerpos, los días de dolor al mes disminuyeron un 69,6 % y, de los 60 pacientes que cumplían criterios de abuso de medicación inicialmente, solo 17 lo hacían al final del estudio. Se retiraron los anticuerpos a 34 pacientes y, de estos, 3 de cada 4 vieron empeoradas sus cefaleas, la mayoría dentro de los dos primeros meses. Conclusiones: En este trabajo confirmamos la eficacia de los anticuerpos antiCGRP en vida real tras un año de tratamiento en pacientes con migraña crónica refractaria. Más de la mitad de los pacientes a los que retiramos el fármaco tras 12 meses de tratamiento recurren antes de los 3 primeros meses. Esto significa que hay que tener en cuenta la recaída tras la supresión de los antiCGRP, sin implicar obligatoriamente que estos fármacos deban mantenerse al año. ABSTRACT : Introduction: Headaches are the main cause to seek neurological attention, and specifically, migraine is the most relevant entity in frequency and disability. The prevalence and impact on the quality of life of patients, along with the knowledge of the physiopathology of this disease, have favored the development of new and more specific therapeutic lines such as the monoclonal antibodies anti CGRP (MAB). Nowadays the cease of the treatment is currently recommended after 12 months, however, the afterward effects are still unknown. Therefore, new controlled studies and clinical experience in real life are needed to asses the efficiency of this drugs on the long run. Objectives: To analize the current experience in clinical practice in patients with chronic migraine treated with antiCGRP antibodies for one year and after their withdrawal. Methods: Prospective recollection of demographic and efficiency parameters of the patients of the Headache Unit of the Neurology Service of HUMV with chronic migraine who had started treatment with the new MABs. The data were collected at the beginning, and quarterly, although we will focus on the experience of the year of treatment and at 12 moths from the start of the treatment. Two drugs were administrated: erunumab (70 or 140 mg) and galcanezumab (240mg subcutaneous on the first month and 120mg the following months), according to their techincal sheet. Results: Of the 61 patients that finalized the yearly treatment, all of them met long term chronic migraine criteria (9.5 years on average). The mean age was 48,4 years (18-66 years) and the majority where women (57; 90,5%). After 12 months in treatment with MABs, pain days per month decreased by 69.9% and, of the 60 patients who initially met criteria for drug overuse, only 17 did so at the end of the study. Half of the 34 patients which treatment was withdrawn recurred, most of them in the first two months. Conclusions: In this study we confirmed the effectiveness of antiCGRP antibodies in real life after one year of treatment in patients with chronic refractory migraine. More than half of the patients we remove the drug after 12 months of treatment recur before the first 3 months. This means that relapse after suppression of antiCGRP must be taken into account, without necessarily implying that these drugs must be maintained at one year. Grado en Medicina

Published

2022

8. Results of anti-CGRP antibodies in patients with refractory migraine

Author

Blanco López, Marta, Pascual Gómez, Julio, González Quintanilla, Vicente, and Universidad de Cantabria

Subjects

Migraña crónica, CGRP, Galcanezumab, Migraña, Migraine, Erenumab, Chronic migraine

Abstract

RESUMEN : Introducción: Dentro de las cefaleas, la migraña es el motivo de consulta más frecuente. Esto, junto al importante impacto en la calidad de vida de los pacientes que la sufren, favorece la búsqueda de nuevas líneas de tratamiento. El papel del CGRP en la fisiopatología de la migraña ha abierto una línea de investigación en tratamientos consistentes en el bloqueo de la acción de este péptido: los anticuerpos antiCGRP. Al tratarse de un tema de actualidad y con poca experiencia en la práctica clínica real, son necesarios además de los ensayos clínicos controlados, experiencias en vida real que valoren la eficacia y tolerabilidad de estos fármacos. Objetivos: Analizar la experiencia en la práctica clínica real con anticuerpos antiCGRP en pacientes con migraña de alta frecuencia o migraña crónica (MC). Metodología: Recogida prospectiva de parámetros de eficacia y seguridad/tolerabilidad a corto plazo (3 meses) de los pacientes de la Unidad de Cefaleas del Servicio de Neurología del Hospital Universitario Marqués de Valdecilla (HUMV) con migraña de alta frecuencia o MC que habían iniciado tratamiento con los nuevos anticuerpos anti-CGRP en el último año. Se administraron dos fármacos: erenumab (en dosis de 70 y 140 mg) y galcanezumab, según ficha técnica (240 mg subcutáneas en primer mes y posteriormente 120 mg al mes). Resultados: Un total de 70 pacientes iniciaron tratamiento con antiCGRPs el último año: 40 con erenumab (14 de ellos con la dosis de 140 mg) y 30 con galcanezumab. De ellos, 66 cumplían criterios de MC (64). La edad media fue de 51 años (18-77 años); la mayoría eran mujeres (64) y cumplían criterios de MC refractaria (fracaso de una media de 9 tratamientos preventivos previos) de larga evolución (13 años de media). A los 3 meses, los días de dolor al mes se redujeron un 55,4% y el 52,5% de los pacientes tuvieron tasas de respuesta superior al 50%. Los pacientes que cumplían criterios de abuso a analgésicos pasaron del 94% al inicio a 35% tras los tres meses de tratamiento. El 73% de los pacientes obtuvieron una puntuación positiva (superior a 4 puntos) en la clasificación PGIC. El 36,5% refirieron uno o más efectos adversos, no siendo ninguno de ellos un motivo de abandono de tratamiento ni una condición de ingreso hospitalario. No observamos diferencias significativas en el perfil de eficacia o efectos adversos entre los dos anticuerpos disponibles en nuestro centro. Conclusiones: A pesar de que los pacientes tratados con estos fármacos cumplían mayoritariamente criterios de MC refractaria de larga evolución y abuso de analgésicos, nuestros datos de práctica real confirman que, al menos a corto plazo, ambos anticuerpos antiCGRP son bien tolerados y eficaces en aproximadamente la mitad de estos pacientes. ABSTRACT : Introduction: migraine is the second most prevalent neurologic disorder (after tension type headache) and the main cause of cephalalgia for which patients seek for medical advice. Furthermore, migraine is one of the most disabling diseases worldwide. Those reasons enhance the research of new lines of treatment. The role of CGRP in the pathophysiology of migraine has opened a line of research in treatments consisting of blocking the action of this peptide: MABs targeting CGRP or its receptor. Because of this being a current issue with little real-life experience, real-life experiences are necessary to evaluate the efficacy and tolerability of these drugs, besides the controlled clinical trials. Purpose: to analyse the experience in real clinical practice with antiCGRP antibodies in patients with high frequency migraine or chronic migraine (CM). Methods: prospective collection of efficacy and safety/tolerability parameters in the short term (3 months) of patients in the Headache Unit of the Neurology Service of the Hospital Universitario Marqués de Valdecilla (HUMV) with high frequency migraine or CM who had started a treatment with the new anti-CGRP antibodies last year. Two drugs were administered: erenumab (in doses of 70 and 140 mg) and galcanezumab, according to protocol (240 mg subcutaneous in the first month and then 120 mg per month). Results: a total of 70 patients started treatment with antiCGRPs in the last year: 40 with erenumab (14 of them with the 140 mg dose) and 30 with galcanezumab. Of these patients, 66 met CM criteria (64) or 2 for high-frequency migraine. The mean age was 51 years (18-77 years). Most of them were women (64) and met criteria for refractory CM (failure of an average of 9 previous preventive treatments) of long evolution (13 years on average). At 3 months, the days of pain per month were reduced by 55.4%, and 52.5% of the patients had response rates greater than 50%. Patients meeting criteria for analgesic abuse went from 94% at baseline to 35% after three months of treatment. 73% of the patients obtained a positive score (greater than 4 points) in the PGIC classification. 36.5% reported one or more adverse effects, none of them being a reason for abandoning treatment or a hospital admission condition. We did not observe significant differences in the efficacy profile or adverse effects between the two antibodies available in our center. Conclusions: even though patients treated with these drugs mostly met criteria for long term refractory CM and analgesic abuse, our data from real-life experience confirms that, at least in the short term, both anti-CGRP antibodies are well tolerated and effective in about half of these patients. Grado en Medicina

Published

2021