United Kingdom National Register Study of Anti-Epileptic Medications: Suspected Foetal Congenital And Pregnancy-Associated Side Effects

Phillips, Benjamin; Evans, Ismay; Skerrett, Victoria; Jones, Alan M.

doi:10.1101/2024.03.26.24304895

Cited by 2 publications

(2 citation statements)

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“…The ADR data required standardisation to allow for comparisons between the different drugs. ADRs per 100,000 R x is a standard approach in signal hypothesis generation [18, 28-33] Drugs were compared to each other in terms of ADR SOCs ( Table S2 and Table 4 ) to determine statistically significant signals and where P < .001, high level group terms (HLGT) were additionally explored ( Table S3 and Table 5 ).…”

Section: Methodsmentioning

confidence: 99%

Suspected Adverse Drug Reactions Associated with Leukotriene Receptor Antagonists Versus First Line Asthma Medications: A National Registry-Pharmacology Approach

Khan,

Hirsch,

Jones

2024

Preprint

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AimsTo determine the suspected adverse drug reaction (ADR) profile of leukotriene receptor antagonists (LTRAs: montelukast and zafirlukast) relative to first-line asthma medications short-acting beta agonists (SABA: salbutamol) and inhaled corticosteroid (ICH: beclomethasone) in the United Kingdom. To determine chemical and pharmacological rationale for the suspected ADR signals.MethodsProperties of the asthma medications (pharmacokinetics and pharmacology) were datamined from the chemical database of bioactive molecules with drug-like properties, European molecular Biology laboratory (ChEMBL). Suspected ADR profiles of the asthma medications was curated from the Medicines and Healthcare products Regulatory Authority (MHRA) Yellow Card interactive drug analysis profiles (iDAP) and concatenated to the standardised prescribing levels (Open Prescribing) between 2018-2023.ResultsTotal ADRs per 100,000Rx(P< .001) and psychiatric system organ class (SOC) ADRs (P< .001) reached statistical significance. Montelukast exhibited the greatest ADR rate at 15.64 per 100,000Rx. The low lipophilic ligand efficiency (LLE = 0.15) of montelukast relative to the controls may explain the promiscuity of interactions with off-target G-coupled protein receptors (GPCRs). This included the dopamine signalling axis, which in combination with bioaccumulation in the cerebrospinal fluid (CSF) to achieve Cmaxbeyond a typical dose can be ascribed to the psychiatric side effects observed. Cardiac ADRs did not reach statistical significance but inhibitory interaction of montelukast with the MAP kinase p38 alpha (a cardiac protective pathway) was identified as a potential rationale for montelukast withdrawal cardiac effects.ConclusionRelative to the controls, montelukast displays a range of suspected system organ class level ADRs. For psychiatric ADR, montelukast is statistically significant (P< .001). A mechanistic hypothesis is proposed based on polypharmacological interactions in combination with CSF levels attained. This work further supports the close monitoring of montelukast for neuropsychiatric side effects.

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Section: Methodsmentioning

confidence: 99%

Suspected Adverse Drug Reactions Associated with Leukotriene Receptor Antagonists Versus First Line Asthma Medications: A National Registry-Pharmacology Approach

Khan,

Hirsch,

Jones

2024

Preprint

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“…The ability to determine correlation of NSARAs ADRs to molecular structure and/or off-target pharmacological factors is therefore timely. [11][12][13][14][15][16][17][18]…”

Section: Introductionmentioning

confidence: 99%

The Interplay Between Molecular Architecture, Pharmacology, and Suspected Adverse Drug Reactions Associated with Non-Steroidal Androgen Antagonists in The United Kingdom

Dhillon,

Antolin,

Jones

2024

Preprint

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AimsTo correlate potential links between the suspected adverse drug reaction (ADR) profile of licensed non-steroidal androgen receptor antagonists (NSARA) with their unique chemical properties and known off-target polypharmacology.MethodsPhysiochemical and polypharmacology data was curated from the Electronic Medicines Compendium, FDA New Drug Applications documents, and ChEMBL databases. System organ class (SOC, MedDRA) suspected ADRs and fatalities were curated from the United Kingdom Medicines and Healthcare products Regulatory Authority (MHRA) Yellow card spontaneous reporting scheme for their respective prescribing period; apalutamide (Jan 2019-), bicalutamide (Aug 2018-), enzalutamide (Aug 2018-), flutamide (Aug 2018-) and darolutamide (March 2019-) until Oct 2023. The number of daily doses (dd) was extracted from OpenPrescribing and NHS Digital secondary care medicines data. Data was standardised before comparison to suspected ADRs and fatality reports per 100,000dd.ResultsA total ofn= 2,480 suspected ADRs were associated with 42,903,000ddof NSARAs in the United Kingdom. The highest number of ADRs were associated with enzalutamide (n= 1,091) and bicalutamide (n= 749). Enzalutamide was found to have the most off-target pharmacological interactions of the NSARAs studied (n= 5) including potent inhibition of γ-aminobutyric acid, GABA receptor (IC50= 2.6 µM vs Cmax= 7.7 µM) associated with nervous system disorders (n= 72, accounting for 73% of all NSARA ADRs in this SOC). Apalutamide, the only other GABA inhibitor (IC50= 3 µM vs Cmax= 2.9 µM) had the highest relative rate of suspected nervous system ADRs at 1.08 per 100,000 dd.Apalutamide was also a modest inhibitor of the human Ether-à-go-go-Related Gene (hERG) ion channel (IC50= 6 µM vs Cmax= 2.9 µM) and had the highest rate of suspected cardiac arrhythmia ADRs, 30-fold over, enzalutamide, a significantly weaker hERG inhibitor (15.7 µM vs Cmax= 7.7 µM).Darolutamide was the only NSARA to show effects at 5-HT (serotonin) receptor at < 10 µM but did not translate to psychiatric disorders due to low clinical BBB penetration but a an association with hepatobiliary and cardiac disorders was identified based on this inhibitory axis. Suspected skin and subcutaneous SOC ADRs was associated with all NSARAs (except flutamide) but did not reach statistical significance (P= .25). A rationale for epidermis reactions relating to apalutamide containing a masked arylamine was explored but molecular matched pair (MMP) analysis with enzalutamide suggests it may not be a chemical cause. Statistical significance (P< .05) was identified in reported fatalities associated with NSARAs, flutamide hadn= 24 or 897.5 fatalities per 100,000ddwhich was likely due to both the indication and the small number ofdd(n= 3,000) during the time period of the study.ConclusionsAn investigation of suspected ADRs, standardised to the number ofddfor the novel NSARA drug class identified SOCs of potential interest. The highest number of reports related to enzalutamide and bicalutamide. Suspected skin and subcutaneous ADRs approached statistical significance and was interrogated for chemical and pharmacological connections for the first time with the aid of MMP analysis. A potential correlation to nervous system disorders and cardiac arrhythmia for the GABA and hERG inhibitors, enzalutamide and apalutamide, respectively was identified. Darolutamide’s interaction with 5-HT may influence ADRs associated with cardiac and hepatobiliary SOCs. Statistically significant number of suspected fatalities with flutamide was identified.

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United Kingdom National Register Study of Anti-Epileptic Medications: Suspected Foetal Congenital And Pregnancy-Associated Side Effects

Cited by 2 publications

References 54 publications

Suspected Adverse Drug Reactions Associated with Leukotriene Receptor Antagonists Versus First Line Asthma Medications: A National Registry-Pharmacology Approach

Suspected Adverse Drug Reactions Associated with Leukotriene Receptor Antagonists Versus First Line Asthma Medications: A National Registry-Pharmacology Approach

The Interplay Between Molecular Architecture, Pharmacology, and Suspected Adverse Drug Reactions Associated with Non-Steroidal Androgen Antagonists in The United Kingdom

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