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1. Monoklonální protilátky v neurologii -- léčba roztroušené sklerózy a migrén.

Author

Bartošová, Olga

Subjects
CELL receptors, CALCITONIN gene-related peptide, MEMBRANE proteins, MONOCLONAL antibodies, CELL populations, ALEMTUZUMAB
Abstract

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Published
2023
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2. Twelve-month safety, tolerability and susceptibility to adverse events of prophylactic migraine therapy with erenumab: a retrospective real-world study

Author

Hannah Schenk, Dagny Holle, Michael Nsaka, Christoph Kleinschnitz, Martin Glas, and Armin Scheffler

Subjects
CGRP antibody, Erenumab, Migraine, Safety and tolerability, Adverse event, Real-world, Medicine
Abstract

Abstract Background Erenumab is a monoclonal antibody (mAb) against the calcitonin gene related peptide (CGRP) receptor and is commonly used in migraine prophylaxis. Pivotal and open-label studies show a good safety and tolerability. However, little is known about possible predictors, dose dependence and time course of development of adverse events (AEs) during the treatment under real-world conditions. Methods Clinical routine data of 128 patients with migraine treated in the West German Headache Center Essen were analyzed regarding AEs during a treatment interval of up to 12 months (3mo n = 128, 6mo n = 105, 9mo n = 74, 12mo n = 54). Patients obtained subcutaneous erenumab injections with either 70 mg or 140 mg per month. The occurrence and alterations of AEs were evaluated. All reported AEs, regardless of their severity, were included. AEs were graded using the common terminology criteria for adverse events (CTCAE). Possible parameters that could influence the occurrence of AEs (sex, episodic or chronic migraine, medication overuse headache, aura and the dosage of erenumab) were analyzed using the Chi-squared test, alpha adjustment was done using the Bonferroni’s correction (6 tests, adjusted alpha = 0.0083). Results The proportion of patients who reported at least one AE were stable over the course of 12 months (after 3mo = 37%, 6mo = 36%, 9mo = 32%, 12mo = 35%). All reported AEs were grade 1 according to CTCAE with one exception (grade 2). Throughout the interval, five AEs were mostly reported: constipation, skin reactions, fatigue, sleep disturbances and nausea/emesis. Discontinuation of erenumab therapy was rarely caused by AEs (5/49). Increasing the dosage from 70 mg to 140 mg per month caused no higher frequency of AEs (Chi-squared test, p = 0.57). Significant more AEs were reported by females and by patients with aura (Chi-squared test, p

Published
2022
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3. Visual snow syndrome is probably not mediated by CGRP: A case series.

Author

Evers, Stefan, Holle-Lee, Dagny, Schankin, Christoph J, Kull, Pia, and Raffaelli, Bianca

Abstract

Background: Visual snow syndrome is a phenomenon for which no effective treatment is known. It is highly comorbid with migraine, therefore we performed a retrospective chart review of patients with visual snow syndrome treated with a monoclonal antibody against calcitonin gene related peptide or its receptor. Findings: We enrolled 15 patients with visual snow syndrome who received at least once a monoclonal antibody against calcitonin gene related peptide or its receptor. None of the patients reported relief of visual snow syndrome whereas those patients with comorbid migraine reported a very good efficacy of the antibody against the migraine headache but not against the migraine aura. Conclusion: The data suggest that visual snow syndrome is not mediated by calcitonin gene related peptide in a relevant way and that the calcitonin gene related peptide receptor is not involved in the network underlying the visual snow syndrome. [ABSTRACT FROM AUTHOR]

Published
2022
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4. CGRP antibody therapy in patients with drug resistant migraine and chronic daily headache: a real-world experience

Author

Armin Scheffler, Hannah Schenk, Sebastian Wurthmann, Michael Nsaka, Christoph Kleinschnitz, Martin Glas, and Dagny Holle

Subjects
Migraine, CGRP antibody, Therapy, Real-world, Chronic daily headache, Medicine
Abstract

Abstract Background Calcitonin gene-related peptide (CGRP) (receptor) antibodies (erenumab, fremanezumab and galcanezumab) are increasingly used in prophylactic treatment of migraine. In the approval studies, severely affected patients with migraine and chronic daily headache without any headache free days were excluded. Thus, less is known about the effectiveness of CGRP antibody treatment in this cohort. Methods Clinical routine data of 32 patients with migraine and daily headache were analysed after three months of treatment with a CGRP antibody (16 erenumab, 7 galcanezumab, 9 fremanezumab), including changes of monthly headache days (MHD) monthly migraine days (MMD) and monthly acute medication intake (AMD) as well as migraine characteristics. Statistical analysis was performed with the Wilcoxon-Test. Migraine characteristics were analysed descriptively. Results The number of MHD was significantly reduced (mean reduction (standard error), p-value): (-4.2 (1.3), p = 0.009) as well as MMD (-4.3 (1.6), p = 0.033). Four patients (13 %) reached a 50 % reduction regarding MHD and 8 patients (25 %) regarding MMD, migraine duration and intensity improved under therapy. Conclusions Despite the low responder rate, CGRP antibodies can be effective at least in a few cases of severely affected patients with drug resistant migraine and chronic daily headache. Trial registration Retrospective registered.

Published
2021
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5. Twelve-month safety, tolerability and susceptibility to adverse events of prophylactic migraine therapy with erenumab: a retrospective real-world study.

Author

Schenk, Hannah, Holle, Dagny, Nsaka, Michael, Kleinschnitz, Christoph, Glas, Martin, and Scheffler, Armin

Subjects
*THERAPEUTIC use of monoclonal antibodies, *STATISTICS, *MIGRAINE, *DESCRIPTIVE statistics, *CHI-squared test, *DRUG side effects, *DATA analysis, *PATIENT safety
Abstract

Background: Erenumab is a monoclonal antibody (mAb) against the calcitonin gene related peptide (CGRP) receptor and is commonly used in migraine prophylaxis. Pivotal and open-label studies show a good safety and tolerability. However, little is known about possible predictors, dose dependence and time course of development of adverse events (AEs) during the treatment under real-world conditions. Methods: Clinical routine data of 128 patients with migraine treated in the West German Headache Center Essen were analyzed regarding AEs during a treatment interval of up to 12 months (3mo n = 128, 6mo n = 105, 9mo n = 74, 12mo n = 54). Patients obtained subcutaneous erenumab injections with either 70 mg or 140 mg per month. The occurrence and alterations of AEs were evaluated. All reported AEs, regardless of their severity, were included. AEs were graded using the common terminology criteria for adverse events (CTCAE). Possible parameters that could influence the occurrence of AEs (sex, episodic or chronic migraine, medication overuse headache, aura and the dosage of erenumab) were analyzed using the Chi-squared test, alpha adjustment was done using the Bonferroni's correction (6 tests, adjusted alpha = 0.0083). Results: The proportion of patients who reported at least one AE were stable over the course of 12 months (after 3mo = 37%, 6mo = 36%, 9mo = 32%, 12mo = 35%). All reported AEs were grade 1 according to CTCAE with one exception (grade 2). Throughout the interval, five AEs were mostly reported: constipation, skin reactions, fatigue, sleep disturbances and nausea/emesis. Discontinuation of erenumab therapy was rarely caused by AEs (5/49). Increasing the dosage from 70 mg to 140 mg per month caused no higher frequency of AEs (Chi-squared test, p = 0.57). Significant more AEs were reported by females and by patients with aura (Chi-squared test, p < 0.001, respectively). Conclusion: In general, erenumab is well tolerated up to a treatment interval of 12 months and reported AEs rarely lead to discontinuation of therapy. A higher dosage does not increase the patient reported AEs. Furthermore, no habituation of AEs is observed. Nevertheless, females and patients with aura seem to be more prone to have AEs. Trial registration: No registration, retrospective analysis. [ABSTRACT FROM AUTHOR]

Published
2022
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6. CGRP antibody therapy in patients with drug resistant migraine and chronic daily headache: a real-world experience.

Author

Scheffler, Armin, Schenk, Hannah, Wurthmann, Sebastian, Nsaka, Michael, Kleinschnitz, Christoph, Glas, Martin, and Holle, Dagny

Subjects
*THERAPEUTIC use of immunoglobulins, *THERAPEUTIC use of monoclonal antibodies, *MIGRAINE, *CHRONIC diseases, *CALCITONIN, *DRUG resistance, *MANN Whitney U Test, *TREATMENT effectiveness, *SYMPTOMS, *DESCRIPTIVE statistics, *CHEMICAL inhibitors
Abstract

Background: Calcitonin gene-related peptide (CGRP) (receptor) antibodies (erenumab, fremanezumab and galcanezumab) are increasingly used in prophylactic treatment of migraine. In the approval studies, severely affected patients with migraine and chronic daily headache without any headache free days were excluded. Thus, less is known about the effectiveness of CGRP antibody treatment in this cohort. Methods: Clinical routine data of 32 patients with migraine and daily headache were analysed after three months of treatment with a CGRP antibody (16 erenumab, 7 galcanezumab, 9 fremanezumab), including changes of monthly headache days (MHD) monthly migraine days (MMD) and monthly acute medication intake (AMD) as well as migraine characteristics. Statistical analysis was performed with the Wilcoxon-Test. Migraine characteristics were analysed descriptively. Results: The number of MHD was significantly reduced (mean reduction (standard error), p-value): (-4.2 (1.3), p = 0.009) as well as MMD (-4.3 (1.6), p = 0.033). Four patients (13 %) reached a 50 % reduction regarding MHD and 8 patients (25 %) regarding MMD, migraine duration and intensity improved under therapy. Conclusions: Despite the low responder rate, CGRP antibodies can be effective at least in a few cases of severely affected patients with drug resistant migraine and chronic daily headache. Trial registration: Retrospective registered. [ABSTRACT FROM AUTHOR]

Published
2021
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7. Physician and patient preferences for dosing options in migraine prevention

Author

Robert Cowan, Joshua M. Cohen, Erik Rosenman, and Ravi Iyer

Subjects
CGRP antibody, Dosing preference, Dosing flexibility, Therapy adherence, Migraine prevention, Monthly dosing, Medicine
Abstract

Abstract Background Adherence to a therapy, though a key factor for successful treatment, is low among patients with chronic conditions such as migraine. Dose frequency plays a major role in adherence. This study evaluated the impact of having flexible dosing options on acceptance of and adherence to a new migraine preventive therapy class among adults with migraine. Methods In this observational study, two 20-min online surveys were completed: one by physicians currently treating adult patients with migraine and the other by adults with migraine. Both surveys presented the participants with three scenarios: 1) only monthly, 2) only quarterly, and 3) both dosing options of the new medication are available. Physicians estimated the proportion of their migraine patients who would receive the new medication in each scenario. Patients were asked about their dosing preference when either or both options are available. Respondents were asked to rate the likelihood of their acceptance of and adherence to the therapy. Results 400 physicians and 417 US adults with migraine completed the surveys. The availability of both dosing options yielded a significant increase in the proportion of patients expected to receive the new medication. The overall proportion of patients favoring monthly dosing (35%) was similar to the proportion favoring quarterly dosing (40%). Among those who preferred monthly dosing (n = 147), a greater proportion indicated they are more likely to fill the prescription (77% vs 56%, P

Published
2019
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8. CGRP and migraine from a cardiovascular point of view: what do we expect from blocking CGRP?

Author

Valentina Favoni, Luca Giani, Linda Al-Hassany, Gian Maria Asioli, Calogera Butera, Irene de Boer, Martina Guglielmetti, Chrysoula Koniari, Theodoros Mavridis, Marge Vaikjärv, Iris Verhagen, Angela Verzina, Bart Zick, Paolo Martelletti, Simona Sacco, and European Headache Federation School of Advanced Studies (EHF-SAS)

Subjects
CGRP, CGRP antibody, Migraine treatment, Cardiovascular, Medicine
Abstract

Abstract Calcitonin gene-related peptide (CGRP) is a neuropeptide with a pivotal role in the pathophysiology of migraine. Blockade of CGRP is a new therapeutic target for patients with migraine. CGRP and its receptors are distributed not only in the central and peripheral nervous system but also in the cardiovascular system, both in blood vessels and in the heart. We reviewed the current evidence on the role of CGRP in the cardiovascular system in order to understand the possible short- and long-term effect of CGRP blockade with monoclonal antibodies in migraineurs. In physiological conditions, CGRP has important vasodilating effects and is thought to protect organs from ischemia. Despite the aforementioned cardiovascular implication, preventive treatment with CGRP antibodies has shown no relevant cardiovascular side effects. Results from long-term trials and from real life are now needed.

Published
2019
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9. PACAP Induces Light Aversion in Mice by an Inheritable Mechanism Independent of CGRP.

Author

Kuburas, Adisa, Mason, Bianca N., Hing, Benjamin, Wattiez, Anne-Sophie, Reis, Alyssa S., Sowers, Levi P., Loomis, Cristina Moldovan, Garcia-Martinez, Leon F., and Russo, Andrew F.

Subjects
*AVERSION, *CALCITONIN gene-related peptide, *HORMONE receptors, *MICE, *ION channels
Abstract

The neuropeptides CGRP (calcitonin gene-related peptide) and PACAP (pituitary adenylate cyclase-activating polypeptide) have emerged as mediators of migraine, yet the potential overlap of their mechanisms remains unknown. Infusion of PACAP, like CGRP, can cause migraine in people, and both peptides share similar vasodilatory and nociceptive functions. In this study, we have used light aversion in mice as a surrogate for migraine-like photophobia to compare CGRP and PACAP and ask whether CGRP or PACAP actions were dependent on each other. Similar to CGRP, PACAP induced light aversion in outbred CD-1 mice. The light aversion was accompanied by increased resting in the dark, but not anxiety in a light-independent open field assay. Unexpectedly, about one-third of the CD-1 mice did not respond to PACAP, which was not seen with CGRP. The responder and nonresponder phenotypes were stable, inheritable, and not sex linked, although there was a trend for greater responses among male mice. RNA-sequencing analysis of trigeminal ganglia yielded hierarchical clustering of responder and nonresponder mice and revealed a number of candidate genes, including greater expression of the Trpc5 and Kcnk12 ion channels and glycoprotein hormones and receptors in a subset of male responder mice. Importantly, an anti-PACAP monoclonal antibody could block PACAP-induced light aversion but not CGRP-induced light aversion. Conversely, an anti-CGRP antibody could not block PACAP-induced light aversion. Thus, we propose that CGRP and PACAP act by independent convergent pathways that cause a migraine-like symptom in mice. [ABSTRACT FROM AUTHOR]

Published
2021
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11. Peripheral and central nervous system distribution of the CGRP neutralizing antibody [125I] galcanezumab in male rats.

Author

Johnson, Kirk W, Morin, S Michelle, Wroblewski, Victor J, and Johnson, Michael P

Subjects
*PERIPHERAL nervous system, *CENTRAL nervous system, *DURA mater, *CEREBROSPINAL fluid, *SPINAL cord
Abstract

Objective: The objective of this investigation was to examine the distribution of galcanezumab and a control immunoglobulin 4 antibody containing the same constant regions as galcanezumab, into peripheral and central tissues.Methods: Galcanezumab and a control immunoglobulin 4 antibody were radioiodinated with Iodine-125 to specific activities of 0.11 mCi/mg and 0.16 mCi/mg, respectively. At 24, 72, and 168 hours following subcutaneous injection of either antibody (4 mg/kg), cerebrospinal fluid and plasma were obtained followed by saline perfusion to remove residual blood and collection of selected tissues for determination of Iodine-125 content by gamma counting.Results: The peak plasma levels of Iodine-125 galcanezumab and Iodine-125 control immunoglobulin 4 were observed at 72 hours and remained high at 168 hours post-dose. The rank order of tissue levels was dura mater = spleen > trigeminal ganglia ≫hypothalamus = spinal cord = prefrontal cortex = cerebellum. Iodine-125 galcanezumab levels in peripheral tissue (dura mater, spleen, and trigeminal ganglia) averaged 5% to 11% of plasma, whereas all of the central nervous system (CNS) tissue levels and the cerebrospinal fluid levels were < 0.4% of plasma. Distribution of the antibodies into the dura mater and the trigeminal ganglia was similar to that observed in the spleen and significantly greater than exposure in the brain or spinal cord.Conclusions: The central levels of galcanezumab were relatively low, which would favor the dura mater and trigeminal ganglia as sites of action for its observed clinical efficacy. However, a central site of action cannot be excluded. [ABSTRACT FROM AUTHOR]

Published
2019
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12. Getting to the Heart of the Matter: Migraine, Triptans, DHE, Ditans, CGRP Antibodies, First/Second‐Generation Gepants, and Cardiovascular Risk.

Author

Mathew, Paul G. and Klein, Brad C.

Subjects
*THERAPEUTIC use of monoclonal antibodies, *ANALGESICS, *CARDIOVASCULAR diseases risk factors, *CEREBRAL ischemia, *DRUG side effects, *MIGRAINE, *GENETIC mutation, *MYOCARDIAL infarction, *NEUROPEPTIDES, *TRYPTAMINE, *TREATMENT effectiveness, *DIHYDROERGOTAMINE, *CHEMICAL inhibitors
Abstract

Premise: The science of migraine pathophysiology has advanced significantly since the 1930's. Imaging techniques, neurochemical analysis, clinical trials, and the clinical experience of providers treating migraine patients have not only sharpened our understanding of the disease, but have also led to the development of novel neural‐based targets. Targeted therapies such as calcitonin gene‐related peptide (CGRP) antibodies and "Second Generation" CGRP receptor antagonists (Gepants) have not only demonstrated efficacy, but have not resulted in any significant cardiovascular nor other serious adverse events. "First Generation" Gepants were associated with liver toxicity. Problem: Triptans and dihydroergotamine (DHE) are contraindicated in patients with hemiplegic and basilar migraine based on theories of migraine pathophysiology from the 1930s. While our understanding of migraine has evolved substantially, perceived concerns of safety from almost a century ago continue to preclude their use in certain patient populations. Potential solution: While migraine aura was once thought to be primarily due to vasoconstriction, current evidence debunks this concept. For instance, hemiplegic migraine is the consequence of genetic mutations resulting in channelopathies without evidence of cerebral ischemia or infarction. Evidence of basilar artery constriction as postulated in basilar migraine is also lacking. This recognition has led the International Headache Society to rename basilar‐type migraine to migraine with brainstem aura. The following discussion reviews current literature with respect to migraine as a neuronal disorder, as well as the published data on the safety of triptans, DHE, Ditans (a novel class of 5‐HT1f receptor agonists), CGRP antibodies, and Gepants. [ABSTRACT FROM AUTHOR]

Published
2019
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13. CGRP antibody therapy in patients with drug resistant migraine and chronic daily headache: a real-world experience

Author

Hannah Schenk, Christoph Kleinschnitz, Michael Nsaka, Sebastian Wurthmann, Dagny Holle, Armin Scheffler, and Martin Glas

Subjects
Calcitonin, medicine.medical_specialty, Neurology, Medizinische Fakultät » Universitätsklinikum Essen » Klinik für Neurologie, Calcitonin Gene-Related Peptide, Migraine Disorders, Medizin, Drug resistance, Calcitonin gene-related peptide, Chronic daily headache, Daily headache, Double-Blind Method, Calcitonin Gene-Related Peptide Receptor Antagonists, Internal medicine, medicine, Humans, ddc:610, Migraine, Medizinische Fakultät » Universitätsklinikum Essen » Center for Translational and Behavioral Neuroscience, Retrospective Studies, CGRP antibody, business.industry, General Medicine, medicine.disease, Anesthesiology and Pain Medicine, Treatment Outcome, Pharmaceutical Preparations, Real-world, Cohort, Medicine, Neurology (clinical), Therapy, Antibody therapy, business, Research Article
Abstract

Background Calcitonin gene-related peptide (CGRP) (receptor) antibodies (erenumab, fremanezumab and galcanezumab) are increasingly used in prophylactic treatment of migraine. In the approval studies, severely affected patients with migraine and chronic daily headache without any headache free days were excluded. Thus, less is known about the effectiveness of CGRP antibody treatment in this cohort. Methods Clinical routine data of 32 patients with migraine and daily headache were analysed after three months of treatment with a CGRP antibody (16 erenumab, 7 galcanezumab, 9 fremanezumab), including changes of monthly headache days (MHD) monthly migraine days (MMD) and monthly acute medication intake (AMD) as well as migraine characteristics. Statistical analysis was performed with the Wilcoxon-Test. Migraine characteristics were analysed descriptively. Results The number of MHD was significantly reduced (mean reduction (standard error), p-value): (-4.2 (1.3), p = 0.009) as well as MMD (-4.3 (1.6), p = 0.033). Four patients (13 %) reached a 50 % reduction regarding MHD and 8 patients (25 %) regarding MMD, migraine duration and intensity improved under therapy. Conclusions Despite the low responder rate, CGRP antibodies can be effective at least in a few cases of severely affected patients with drug resistant migraine and chronic daily headache. Trial registration Retrospective registered.

Published
2021

14. Prevention of stress- or nitric oxide donor-induced medication overuse headache by a calcitonin gene-related peptide antibody in rodents.

Author

Kopruszinski, Caroline Machado, Xie, Jennifer Yanhua, Eyde, Nathan Mackenzie, Remeniuk, Bethany, Walter, Sarah, Stratton, Jennifer, Bigal, Marcelo, Chichorro, Juliana Geremias, Dodick, David, and Porreca, Frank

Subjects
*CALCITONIN gene-related peptide, *MIGRAINE, *NITRIC oxide, *ALLODYNIA, *IMMUNOGLOBULINS, *THERAPEUTIC use of monoclonal antibodies, *ANIMAL experimentation, *ANIMALS, *CARDIOVASCULAR agents, *HEADACHE, *HYPERALGESIA, *MONOCLONAL antibodies, *NEUROPEPTIDES, *RATS, *PSYCHOLOGICAL stress, *SUMATRIPTAN, *CHEMICAL inhibitors, *PREVENTION
Abstract

Objective The objective of this study was the determination of the role of calcitonin gene-related peptide (CGRP) in the induction of medication overuse headache (MOH)-related migraine in an injury-free preclinical model. Methods Rats were primed by a 7-day period of exposure to acute migraine therapies including sumatriptan and morphine. After an additional 14-day drug-free period, rats were exposed to putative migraine triggers including bright light stress (BLS) or nitric oxide (NO) donor in the presence or absence of TEV48125, a fully humanized CGRP antibody. Cutaneous allodynia (CA) was used as an outcome measure and CGRP blood and cerebrospinal fluid (CSF) levels were measured. Results BLS and NO donor challenge evoked delayed, long-lasting CA selectively in rats that were previously treated with sumatriptan or morphine. BLS produced a significant increase in CGRP in the plasma, but not CSF, in animals that were previously exposed to sumatriptan compared to saline controls. TEV48125 did not modify baseline tactile thresholds or produce behavioral side effects, but significantly inhibited both BLS- and NO donor-induced CA in animals that were previously primed with sumatriptan or morphine; an isotype control protein that does not bind CGRP had no effect. Interpretation These data suggest that acute migraine medications may promote MOH in susceptible individuals through CGRP-dependent mechanisms and that anti-CGRP antibodies may be a useful clinical strategy for the treatment of MOH. [ABSTRACT FROM AUTHOR]

Published
2017
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15. Changes in Cerebral Blood Flow after Erenumab Treatment in Good and Non-Responders—A Pilot Study of Migraine Patients

Author

Magdalena Nowaczewska, Grzegorz Meder, Wojciech Kaźmierczak, and Marcin Straburzyński

Subjects
medicine.medical_specialty, efficacy, Cerebral arteries, cerebral blood flow, medication overuse, Article, transcranial Doppler, 03 medical and health sciences, 0302 clinical medicine, Chronic Migraine, medicine.artery, Internal medicine, Basilar artery, Medicine, MOH, migraine, 030212 general & internal medicine, Mean Blood Flow Velocity, CGRP antibody, business.industry, General Medicine, medicine.disease, Transcranial Doppler, Migraine, Cerebral blood flow, erenumab, Cohort, outcome, Cardiology, business, headache, 030217 neurology & neurosurgery
Abstract

Erenumab showed efficacy in migraine prevention, however we cannot identify which patients to treat by predicting efficacy response. The aim of this study was to compare changes in cerebral blood flow (CBF) reflected by transcranial Doppler (TCD) in erenumab good responders (GR) and non-responders, in order to identify a parameter that could predict the treatment response. In this study, migraineurs treated with erenumab underwent clinical and TCD evaluations before and 6 weeks after the treatment, including data on migraine type, monthly migraine days (MMD), medication overuse headache (MOH) presence, mean blood flow velocity (Vm) and pulsatility index (PI) in cerebral arteries (CA). GR were defined as reporting ≥50% reduction in MMD. Thirty women were enrolled, of mean age 40.53 years, 20 with chronic migraine, 14 with MOH, and 19 were GR. Baseline Vm values in right CA and basilar artery (BA) were significantly lower in GR as compared with non-responders. Vm values in all arteries significantly increased after the treatment as compared with corresponding baseline values, but only in GR. A significant negative correlation was observed between baseline Vm in right CA and treatment effectiveness. Baseline Vm in right CA and basilar artery is reduced in erenumab GR as compared with non-responders. This asymmetry normalizes after the treatment with significant Vm increase in CA which may reflect CBF increase in GR only. Lower baseline Vm in right CA may predict erenumab efficacy, however, these results should be replicated in a larger cohort.

Published
2021

18. CGRP and migraine from a cardiovascular point of view: what do we expect from blocking CGRP?

Author

Favoni, V., Giani, L., Al-Hassany, L., Asioli, G.M., Butera, C., den Boer, I., Guglielmetti, M., Koniari, C., Mavridis, T., Vaikjarv, M., Verhagen, I., Verzina, A., Zick, B., Martelletti, P., Sacco, S., Favoni, V., Giani, L., Al-Hassany, L., Asioli, G.M., Butera, C., den Boer, I., Guglielmetti, M., Koniari, C., Mavridis, T., Vaikjarv, M., Verhagen, I., Verzina, A., Zick, B., Martelletti, P., and Sacco, S.

Abstract

Calcitonin gene-related peptide (CGRP) is a neuropeptide with a pivotal role in the pathophysiology of migraine. Blockade of CGRP is a new therapeutic target for patients with migraine. CGRP and its receptors are distributed not only in the central and peripheral nervous system but also in the cardiovascular system, both in blood vessels and in the heart. We reviewed the current evidence on the role of CGRP in the cardiovascular system in order to understand the possible short- and long-term effect of CGRP blockade with monoclonal antibodies in migraineurs. In physiological conditions, CGRP has important vasodilating effects and is thought to protect organs from ischemia. Despite the aforementioned cardiovascular implication, preventive treatment with CGRP antibodies has shown no relevant cardiovascular side effects. Results from long-term trials and from real life are now needed.

Published
2019
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19. Effect of two novel CGRP-binding compounds in a closed cranial window rat model

Author

Juhl, Louise, Edvinsson, Lars, Olesen, Jes, and Jansen-Olesen, Inger

Subjects
*ELECTRIC stimulation, *NUCLEIC acids, *SCAVENGERS (Zoology), *BLOOD pressure
Abstract

Abstract: We investigated the in vivo effects of two novel calcitonin gene-related peptide (CGRP) binding molecules in the genuine closed cranial window model in the rat. The RNA-Spiegelmer (NOX-C89) and the monoclonal CGRP antibody are CGRP scavengers and might be used as an alternative to CGRP-receptor antagonists in the treatment of migraine. Rats were anaesthetized and a closed cranial window established. Changes in dural and pial artery diameter and mean arterial blood pressure were measured simultaneously. Infusion of the RNA-Spiegelmer or the CGRP antibody alone had no effect on the arteries or the mean arterial blood pressure. We then used a bolus of 0.3 μg/kg CGRP (n=6) or electrical stimulation (25 V, 5 Hz, 1 ms pulse width and of 10 s of duration) (n=6) to induce dilatation of dural and pial arteries (mediated via CGRP-receptors). Pre-treatment with the RNA-Spiegelmer inhibited CGRP-induced vasodilatation of the dural artery (from 38±17% to 7±3%) and the pial artery (from 14±1% to 3±2%) (P<0.05). The RNA-Spiegelmer, however, did not significantly inhibit dilatation induced by electrical stimulation (P>0.05). The CGRP antibody caused a significant reduction of the dural artery diameter caused by intravenous CGRP-infusion (from 23±5% to 12±3%) (P<0.05), but did not inhibit dilatation caused by electrical stimulation (P>0.05). In conclusion, the CGRP scavengers effectively inhibited the effect of circulating CGRP but do not modify the effect of electrical stimulation and the consequent liberation of CGRP from perivascular sensory nerve fibres. [Copyright &y& Elsevier]

Published
2007
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20. Physician and patient preferences for dosing options in migraine prevention

Author

Erik Rosenman, Robert Cowan, Joshua M. Cohen, and Ravi Iyer

Subjects
Male, Flexible dosing, lcsh:Medicine, 0302 clinical medicine, Surveys and Questionnaires, Dosing flexibility, Monthly dosing, 030212 general & internal medicine, Aged, 80 and over, CGRP antibody, Analgesics, Migraine prevention, Dosing regimen, Patient Preference, General Medicine, Middle Aged, Patient preference, Female, Research Article, Therapy adherence, Adult, medicine.medical_specialty, Adolescent, Migraine Disorders, Drug Administration Schedule, Medication Adherence, Young Adult, 03 medical and health sciences, Physicians, Internal medicine, medicine, Humans, Dosing, Medical prescription, Aged, Biological Products, Physician-Patient Relations, Adult patients, business.industry, lcsh:R, Quarterly dosing, medicine.disease, Anesthesiology and Pain Medicine, Migraine, Chronic Disease, Dosing preference, Observational study, Neurology (clinical), business, 030217 neurology & neurosurgery
Abstract

Background Adherence to a therapy, though a key factor for successful treatment, is low among patients with chronic conditions such as migraine. Dose frequency plays a major role in adherence. This study evaluated the impact of having flexible dosing options on acceptance of and adherence to a new migraine preventive therapy class among adults with migraine. Methods In this observational study, two 20-min online surveys were completed: one by physicians currently treating adult patients with migraine and the other by adults with migraine. Both surveys presented the participants with three scenarios: 1) only monthly, 2) only quarterly, and 3) both dosing options of the new medication are available. Physicians estimated the proportion of their migraine patients who would receive the new medication in each scenario. Patients were asked about their dosing preference when either or both options are available. Respondents were asked to rate the likelihood of their acceptance of and adherence to the therapy. Results 400 physicians and 417 US adults with migraine completed the surveys. The availability of both dosing options yielded a significant increase in the proportion of patients expected to receive the new medication. The overall proportion of patients favoring monthly dosing (35%) was similar to the proportion favoring quarterly dosing (40%). Among those who preferred monthly dosing (n = 147), a greater proportion indicated they are more likely to fill the prescription (77% vs 56%, P

Published
2019

21. CGRP and migraine from a cardiovascular point of view: what do we expect from blocking CGRP?

Author

Martina Guglielmetti, Iris Verhagen, Simona Sacco, Theodoros Mavridis, Valentina Favoni, Linda Al-Hassany, Angela Verzina, Paolo Martelletti, Chrysoula Koniari, Marge Vaikjärv, Gian Maria Asioli, Irene de Boer, Calogera Butera, Luca Giani, Bart Zick, Internal Medicine, and Valentina Favoni, Luca Giani, Linda Al-Hassany, Gian Maria Asioli, Calogera Butera, Irene de Boer, Martina Guglielmetti, Chrysoula Koniari, Theodoros Mavridis, Marge Vaikjärv, Iris Verhagen, Angela Verzina, Bart Zick, Paolo Martelletti, Simona Sacco, European Headache Federation School of Advanced Studies (EHF-SAS)

Subjects
Calcitonin Gene-Related Peptide Receptor Antagonist, Cardiovascular, CGRP, CGRP antibody, Migraine treatment, Antibodies, Monoclonal, Calcitonin Gene-Related Peptide, Calcitonin Gene-Related Peptide Receptor Antagonists, Cardiovascular System, Humans, Migraine Disorders, Receptors, Calcitonin Gene-Related Peptide, Sex Factors, Vasodilation, Ischemia, lcsh:Medicine, Sex Factor, Review Article, Calcitonin gene-related peptide, Pharmacology, Antibodies, 03 medical and health sciences, 0302 clinical medicine, Migraine Disorder, Monoclonal, Receptors, medicine, 030212 general & internal medicine, integumentary system, business.industry, lcsh:R, General Medicine, medicine.disease, 3. Good health, Blockade, Anesthesiology and Pain Medicine, medicine.anatomical_structure, nervous system, Migraine, Calcitonin, Peripheral nervous system, Neurology (clinical), business, 030217 neurology & neurosurgery, Human
Abstract

Calcitonin gene-related peptide (CGRP) is a neuropeptide with a pivotal role in the pathophysiology of migraine. Blockade of CGRP is a new therapeutic target for patients with migraine. CGRP and its receptors are distributed not only in the central and peripheral nervous system but also in the cardiovascular system, both in blood vessels and in the heart. We reviewed the current evidence on the role of CGRP in the cardiovascular system in order to understand the possible short- and long-term effect of CGRP blockade with monoclonal antibodies in migraineurs. In physiological conditions, CGRP has important vasodilating effects and is thought to protect organs from ischemia. Despite the aforementioned cardiovascular implication, preventive treatment with CGRP antibodies has shown no relevant cardiovascular side effects. Results from long-term trials and from real life are now needed.

Published
2019

22. Changes in Cerebral Blood Flow after Erenumab Treatment in Good and Non-Responders—A Pilot Study of Migraine Patients.

Author

Nowaczewska, Magdalena, Straburzyński, Marcin, Meder, Grzegorz, and Kaźmierczak, Wojciech

Subjects
*CEREBRAL circulation, *BASILAR artery, *MIGRAINE, *BLOOD flow, *FLOW velocity, *ERENUMAB
Abstract

Erenumab showed efficacy in migraine prevention, however we cannot identify which patients to treat by predicting efficacy response. The aim of this study was to compare changes in cerebral blood flow (CBF) reflected by transcranial Doppler (TCD) in erenumab good responders (GR) and non-responders, in order to identify a parameter that could predict the treatment response. In this study, migraineurs treated with erenumab underwent clinical and TCD evaluations before and 6 weeks after the treatment, including data on migraine type, monthly migraine days (MMD), medication overuse headache (MOH) presence, mean blood flow velocity (Vm) and pulsatility index (PI) in cerebral arteries (CA). GR were defined as reporting ≥50% reduction in MMD. Thirty women were enrolled, of mean age 40.53 years, 20 with chronic migraine, 14 with MOH, and 19 were GR. Baseline Vm values in right CA and basilar artery (BA) were significantly lower in GR as compared with non-responders. Vm values in all arteries significantly increased after the treatment as compared with corresponding baseline values, but only in GR. A significant negative correlation was observed between baseline Vm in right CA and treatment effectiveness. Baseline Vm in right CA and basilar artery is reduced in erenumab GR as compared with non-responders. This asymmetry normalizes after the treatment with significant Vm increase in CA which may reflect CBF increase in GR only. Lower baseline Vm in right CA may predict erenumab efficacy; however, these results should be replicated in a larger cohort. [ABSTRACT FROM AUTHOR]

Published
2021
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24. Peripheral and central nervous system distribution of the CGRP neutralizing antibody [ 125 I] galcanezumab in male rats.

Author

Johnson KW, Morin SM, Wroblewski VJ, and Johnson MP

Subjects
Animals, Antibodies, Neutralizing pharmacology, Dura Mater metabolism, Iodine Radioisotopes, Male, Rats, Rats, Sprague-Dawley, Spleen metabolism, Tissue Distribution, Trigeminal Ganglion metabolism, Antibodies, Monoclonal, Humanized pharmacokinetics, Brain metabolism, Spinal Cord metabolism
Abstract

Objective: The objective of this investigation was to examine the distribution of galcanezumab and a control immunoglobulin 4 antibody containing the same constant regions as galcanezumab, into peripheral and central tissues., Methods: Galcanezumab and a control immunoglobulin 4 antibody were radioiodinated with Iodine-125 to specific activities of 0.11 mCi/mg and 0.16 mCi/mg, respectively. At 24, 72, and 168 hours following subcutaneous injection of either antibody (4 mg/kg), cerebrospinal fluid and plasma were obtained followed by saline perfusion to remove residual blood and collection of selected tissues for determination of Iodine-125 content by gamma counting., Results: The peak plasma levels of Iodine-125 galcanezumab and Iodine-125 control immunoglobulin 4 were observed at 72 hours and remained high at 168 hours post-dose. The rank order of tissue levels was dura mater = spleen > trigeminal ganglia ≫hypothalamus = spinal cord = prefrontal cortex = cerebellum. Iodine-125 galcanezumab levels in peripheral tissue (dura mater, spleen, and trigeminal ganglia) averaged 5% to 11% of plasma, whereas all of the central nervous system (CNS) tissue levels and the cerebrospinal fluid levels were < 0.4% of plasma. Distribution of the antibodies into the dura mater and the trigeminal ganglia was similar to that observed in the spleen and significantly greater than exposure in the brain or spinal cord., Conclusions: The central levels of galcanezumab were relatively low, which would favor the dura mater and trigeminal ganglia as sites of action for its observed clinical efficacy. However, a central site of action cannot be excluded.

Published
2019
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