Delving into the Latest Updates on Metildigoxin with Synapse

Overview

Basic Info

Drug Type

Small molecule drug

Synonyms

Medigoxin, Medigoxin (BAN), Metildigoxin (INN)

+ [5]

Target-

Mechanism-

Therapeutic Areas

Cardiovascular Diseases

Active Indication

Atrial FibrillationHeart FailureTachycardia

Inactive Indication-

Originator Organization

Sanofi (China) Investment Co. Ltd.

Active Organization

Chugai Pharmaceutical Co., Ltd.

Sanofi (China) Investment Co. Ltd.

Inactive Organization-

Drug Highest PhaseApproved

First Approval Date

JP (13 Mar 1979),

Atrial FibrillationHeart FailureTachycardia

Regulation-

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Structure

Molecular FormulaC42H66O14

InChIKeyIYJMSDVSVHDVGT-PEQKVOOWSA-N

CAS Registry30685-43-9

Drug-induced long QT syndrome (diLQTS) is a rare but serious adverse drug reaction. Drug-drug interaction (DDI) is one of the risk factors for the development of diLQTS. However, the combinations of drugs that increase the risk of diLQTS have not been extensively investigated. This study was performed to analyse the potential DDIs that elevate the incidence of diLQTS using a spontaneous reporting system.

METHODS:

The Japanese Adverse Drug Event Report database from April 2004 to January 2020 was used to assess adverse event reports. We calculated the reporting odds ratio and 95% confidence interval for signal detection.

RESULTS AND DISCUSSION:

Signals for concomitant use risk were detected in 31 drug combinations. Combinations of antipsychotics and antidepressants were the most common (olanzapine & fluvoxamine, olanzapine & trazodone, quetiapine & paroxetine, sulpiride & fluvoxamine, sulpiride & trazodone). Sixteen, 17 and 21 combinations were designated as requiring precaution for concomitant use in at least one of the package inserts in Japan, the United States and the United Kingdom, respectively, although no such precautions were described for the remaining combinations. On the contrary, a combination of bepridil & clarithromycin was categorized as "X (avoid combination)" and two combinations (chlorpromazine & haloperidol, amiodarone & metildigoxin) were classified as "D (modify regimen)" in the Lexicomp^® risk rating.

WHAT IS NEW AND CONCLUSION:

This study identified 31 combinations of drugs that may elevate the risk of diLQTS. The use of these drug combinations should be monitored more carefully in future.

01 Mar 2016·Journal of veterinary internal medicineQ2 · AGRICULTURAL & FORESTRY SCIENCE

Long‐term Outcome of Irish Wolfhound Dogs with Preclinical Cardiomyopathy, Atrial Fibrillation, or Both Treated with Pimobendan, Benazepril Hydrochloride, or Methyldigoxin Monotherapy

Q2 · AGRICULTURAL & FORESTRY SCIENCE

ArticleOA

Author: Fox, P.R. ; Vollmar, A.C.

Background:

Dilated cardiomyopathy (DCM) is a common cause of morbidity and mortality in the Irish Wolfhound (IW). However, the benefit of medical treatment in IW dogs with preclinical DCM, atrial fibrillation (AF), or both has not been demonstrated.

Objectives:

Compare the time to develop congestive heart failure (CHF) or sudden death in IW dogs with preclinical DCM, AF, or both receiving monotherapy with pimobendan, methyldigoxin, or benazepril hydrochloride.

Animals:

Seventy‐five client‐owned IW dogs.

Methods:

Irish Wolfhound dogs were prospectively randomized to receive pimobendan (Vetmedin®), benazepril HCl (Fortekor®), or methyldigoxin (Lanitop®) monotherapy in a 1:1:1 ratio in a blinded clinical trial. The prospectively defined composite primary endpoint was onset of CHF or sudden death. To assure stringent evaluation of treatment effect, data from dogs complying with the study protocol were analyzed.

Results:

Sixty‐six IW fulfilling the study protocol included 39 males, 27 females; median (interquartile range) age, 4.0 years (3.0–5.0 years) and weight, 70.0 kg (63.0–75.0 kg). Primary endpoint was reached in 5 of 23 (21.7%) IW receiving pimobendan, 11 of 22 (50.0%) receiving benazepril HCl, and 9 of 21 (42.9%) receiving methyldigoxin. Median time to primary endpoint was significantly longer for pimobendan (1,991 days; 65.4 months) compared to methyldigoxin (1,263 days; 41.5 months; P = .031) or benazepril HCl‐(997 days; 32.8 months; P = .008) treated dogs.

Conclusions and Clinical Importance:

In IW dogs with preclinical DCM, AF or both, pimobendan monotherapy significantly prolonged time to onset of CHF or sudden death than did monotherapy with benazepril HCl or methyldigoxin.

01 Aug 2014·Forensic science internationalQ3 · MEDICINE

Unintentional lethal overdose with metildigoxin in a 36-week-old infant – post mortem tissue distribution of metildigoxin and its metabolites by liquid chromatography tandem mass spectrometry

Q3 · MEDICINE

ArticleOA

Author: Hess, Cornelius ; Musshoff, Frank ; Doberentz, Elke ; Brockmann, Christopher ; Madea, Burkhard

A massive lethal overdose with beta-metildigoxin in a 36-week-old infant is presented. Determination of beta-metildigoxin and its metabolites digoxin, digoxigenin and digoxigenin-monodigitoxosid is achieved by a liquid chromatographic mass spectrometric (LC-MS/MS) method. Measured concentrations for beta-metildigoxin and digoxin in peripheral blood were 40.2 ng/ml and 25.6 ng/ml, respectively. Tissue distribution showed highest concentrations in kidney tissue and gastric content. The metabolite digoxigenin-monodigitoxosid could be detected in heart blood, duodenal content, gastric content and fat tissue while the metabolite digoxigenin could only be detected in gastric content since the drug was given by a stomach tube.

100 Deals associated with Metildigoxin

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External Link

KEGG	Wiki	ATC	Drug Bank
D09847	Metildigoxin	C01AA08	DB13401

R&D Status

10 top approved records.

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Indication	Country/Location	Organization	Date
Atrial Fibrillation	JP	Chugai Pharmaceutical Co., Ltd.	13 Mar 1979
Heart Failure	JP	Chugai Pharmaceutical Co., Ltd.	13 Mar 1979
Tachycardia	JP	Chugai Pharmaceutical Co., Ltd.	13 Mar 1979