Generalized Anxiety Disorder Clinical Trial
— AlpraOfficial title:
Efficacy and Safety Study of a IMSS Developed Phytopharmaceutical for the Treatment of Anxiety. Double Blind and Randomized Clinical Trial Controlled With Alprazolam
The investigator's group at the Mexican Institute of Social Security has worked for more than
20 years in the scientific research of the plant species Galphimia glauca Cav., which is used
in Mexican Traditional Medicine for the treatment of mental disorders. With the obtained
results it was possible the development of a phytopharmaceutical elaborated with the extract
of this plant, which was standardized in its content of Galphimine-B (G-B). This new compound
is a nor, seco-triterpene, which possesses selective effects on the central nervous system.
Through electrophysiological neuronal unitary records it was identified that G-B acts on the
ventral tegmental area (VTA), and exerts its effect on (N-methyl-D-aspartate) NMDA receptors
in dopaminergic neurons. The new phytopharmaceutical, elaborated from a standardized extract
(in its G-B content) of G. glauca, was subjected to a double blind and randomized clinical
study that compared its efficacy and therapeutic tolerability with a similar drug formulated
with lorazepam in patients with diagnosis of generalized anxiety disorder (GAD). In a total
of 152 patients, it was evidenced that the phytomedicine administered orally (for 4 weeks)
was able to significantly reduce anxiety, in a similar way as lorazepam did, but with better
tolerability. Several patients who were treated with lorazepam had to leave the study because
they had daytime sleepiness.
In clinical practice, different benzodiazepines have specific indications. In the case of
anxiety disorders, the drug of first choice is Alprazolam, this, because it manifests a more
powerful anxiolytic effect with a lower degree of sedation and daytime sleepiness.
Objective: The present project aims to compare the efficacy and therapeutic safety of an
elaborated phytopharmaceutical with the standardized extract of Galphimia glauca with
Alprazolam .
Status | Recruiting |
Enrollment | 122 |
Est. completion date | October 19, 2020 |
Est. primary completion date | September 19, 2020 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years and older |
Eligibility |
Inclusion Criteria: - Patients of both sexes - Eighteen years of age and older - Clinical diagnosis of Generalized Anxiety Disorder - Eighteen points or more on Hamilton Anxiety Scale - Without previous treatment for this disease (for at least one month before). - In case of being women of reproductive age, who are not pregnant or lactating. - To sign an informed consent letter of participation in the investigation. Exclusion Criteria: - Patients who have treatment for their condition - Patients who have another mental disorder added - Patients with alcoholism, smoking or drug addiction - Patients who live alone - Ingest of drugs for insomnia - Ingest of drugs of the Monoamine Oxidase Inhibitors group - Patients with epilepsy - Patients who operate dangerous machinery - Patients who have to drive at work (car, truck or other motor vehicle) for a long time. |
Country | Name | City | State |
---|---|---|---|
Mexico | Regional General Hospital Number 1 at Cuernavaca, Morelos. Mexican Insitute of Social Security | Cuernavaca | Morelos |
Lead Sponsor | Collaborator |
---|---|
Coordinación de Investigación en Salud, Mexico |
Mexico,
Abarca Vargas R, Zamilpa A, Aguilar FA, Herrera-Ruiz M, Tortoriello J, Jiménez-Ferrer E. Pharmacokinetic study in mice of galphimine-A, an anxiolytic compound from Galphimia glauca. Molecules. 2014 Mar 12;19(3):3120-34. doi: 10.3390/molecules19033120. — View Citation
Aguilar-Santamaría L, Ramírez G, Herrera-Arellano A, Zamilpa A, Jiménez JE, Alonso-Cortés D, Cortés-Gutiérrez EI, Ledesma N, Tortoriello J. Toxicological and cytotoxic evaluation of standardized extracts of Galphimia glauca. J Ethnopharmacol. 2007 Jan 3;1 — View Citation
González-Cortazar M, Herrera-Ruiz M, Zamilpa A, Jiménez-Ferrer E, Marquina S, Alvarez L, Tortoriello J. Anti-inflammatory activity and chemical profile of Galphimia glauca. Planta Med. 2014 Jan;80(1):90-6. doi: 10.1055/s-0033-1360150. Epub 2013 Dec 11. — View Citation
González-Cortazar M, Tortoriello J, Alvarez L. Norsecofriedelanes as spasmolytics, advances of structure-activity relationships. Planta Med. 2005 Aug;71(8):711-6. — View Citation
Herrera-Arellano A, Jiménez-Ferrer E, Zamilpa A, Morales-Valdéz M, García-Valencia CE, Tortoriello J. Efficacy and tolerability of a standardized herbal product from Galphimia glauca on generalized anxiety disorder. A randomized, double-blind clinical tri — View Citation
Herrera-Arellano A, Jiménez-Ferrer JE, Zamilpa A, García-Alonso G, Herrera-Alvarez S, Tortoriello J. Therapeutic effectiveness of Galphimia glauca vs. lorazepam in generalized anxiety disorder. A controlled 15-week clinical trial. Planta Med. 2012 Sep;78( — View Citation
Herrera-Ruiz M, González-Cortazar M, Jiménez-Ferrer E, Zamilpa A, Alvarez L, Ramírez G, Tortoriello J. Anxiolytic effect of natural galphimines from Galphimia glauca and their chemical derivatives. J Nat Prod. 2006 Jan;69(1):59-61. Erratum in: J Nat Prod. — View Citation
Herrera-Ruiz M, Jiménez-Ferrer JE, De Lima TC, Avilés-Montes D, Pérez-García D, González-Cortazar M, Tortoriello J. Anxiolytic and antidepressant-like activity of a standardized extract from Galphimia glauca. Phytomedicine. 2006 Jan;13(1-2):23-8. Epub 200 — View Citation
Jiménez-Ferrer E, Herrera-Ruiz M, Ramírez-García R, Herrera-Arellano A, Tortoriello J. Interaction of the natural anxiolytic Galphimine-B with serotonergic drugs on dorsal hippocampus in rats. J Ethnopharmacol. 2011 Sep 1;137(1):724-9. doi: 10.1016/j.jep. — View Citation
Jiménez-Ferrer E, Santillán-Urquiza MA, Alegría-Herrera E, Zamilpa A, Noguerón-Merino C, Tortoriello J, Navarro-García V, Avilés-Flores M, Fuentes-Mata M, Herrera-Ruiz M. Anxiolytic effect of fatty acids and terpenes fraction from Aloysia triphylla: Serot — View Citation
Mangas S, Bonfill M, Osuna L, Moyano E, Tortoriello J, Cusido RM, Piñol MT, Palazón J. The effect of methyl jasmonate on triterpene and sterol metabolisms of Centella asiatica, Ruscus aculeatus and Galphimia glauca cultured plants. Phytochemistry. 2006 Se — View Citation
Osuna L, Moyano E, Mangas S, Bonfill M, Cusidó RM, Piñol MT, Zamilpa A, Tortoriello J, Palazón J. Immobilization of Galphimia glauca plant cell suspensions for the production of enhanced amounts of Galphimine-B. Planta Med. 2008 Jan;74(1):94-9. doi: 10.10 — View Citation
Osuna L, Pereda-Miranda R, Tortoriello J, Villarreal ML. Production of the sedative triterpene galphimine B in Galphimia glauca tissue culture. Planta Med. 1999 Mar;65(2):149-52. — View Citation
Prieto-Gómez B, Tortoriello J, Vázquez-Alvarez A, Reyes-Vázquez C. Galphimine B modulates synaptic transmission on dopaminergic ventral tegmental area neurons. Planta Med. 2003 Jan;69(1):38-43. — View Citation
Rojas G, Aranda E, Navarro V, Zamilpa A, Tortoriello J. In vitro propagation of Galphimia glauca and content of the sedative compound galphimine-B in wild and micropropagated plants. Planta Med. 2005 Nov;71(11):1076-8. — View Citation
Santillán-Urquiza MA, Herrera-Ruiz M, Zamilpa A, Jiménez-Ferrer E, Román-Ramos R, Tortoriello J. Pharmacological interaction of Galphimia glauca extract and natural galphimines with Ketamine and Haloperidol on different behavioral tests. Biomed Pharmacoth — View Citation
Tortoriello J, Lozoya X. Effect of Galphimia glauca methanolic extract on neuropharmacological tests. Planta Med. 1992 Jun;58(3):234-6. — View Citation
Tortoriello J, Ortega A, Herrera-Ruíz M, Trujillo J, Reyes-Vázquez C. Galphimine-B modifies electrical activity of ventral tegmental area neurons in rats. Planta Med. 1998 May;64(4):309-13. — View Citation
Tortoriello J, Ortega A. Sedative effect of galphimine B, a nor-seco-triterpenoid from Galphimia glauca. Planta Med. 1993 Oct;59(5):398-400. — View Citation
* Note: There are 19 references in all — Click here to view all references
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Therapeutic efficacy: improvement of the clinical condition higher than 90%. It will be measured by means of the Hamilton Rating Scale for Anxiety. | It will be considered when the patient presents an improvement of the clinical condition higher than 90% on the scales of measurement (HAM-A). Hamilton Rating Scale for Anxiety (HAM-A) consisted of 14 items that assessed the severity of anxiety. Each item was scored using a 5-point scale (0=not present to 4=very severe). The HAM-A Total Score could have ranged from 0 to 56 and higher scores indicated a greater degree of symptom severity. Scores 14-21 indicate mild anxiety; scores 21-29 indicate moderate anxiety; scores over 29 indicate severe anxiety | Up to 10 weeks | |
Secondary | Therapeutic Tolerability: Number of participants with treatment-related adverse events as assessed by CTCAE v4.0 | Incidence and duration of adverse events monitored throughout the study by physical examination and the application of a questionnaire. It will by considered as Treatment Tolerability when the participant does not present adverse effect of Grade 3 according to the Common Terminology Criteria for Adverse Events v4.0 | Up to 10 weeks | |
Secondary | Clinical Global Impression of Improvement Scale (CGI-I). A 7 points scale that is used to evaluate how much the patient's illness has improved or worsened relative to a baseline state at the beginning of the intervention. | Clinical Global Impression of Improvement Scale is useful to evaluate the clinician's perception of the participant improvement at the time of assessment compared with the baseline condition, before initiating the intervention. The scale could have ranged from 1 to 7, where 1 means very much improved since the initiation of treatment; 2 means much improved; 3 means minimal improved; 4 means no change from baseline; 5 means minimally worse; 6 means much worse; 7 means very much worse. Values near to 1 or equal to 1 are considered better outcome, while higher values near to 7 or equal to 7 are considered worse outcome. |
Up to 10 weeks |
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