Pharmacokinetics under the COVID-19 storm!

Reddy, Venkatesh Pilla; El‐Khateeb, Eman; Jo, Heeseung; Natalie, Natalie; Lythgoe, Emily; Tang, Weifeng; Jamei, Masoud; Sharma, Shringi; Rostami‐Hodjegan, Amin

doi:10.22541/au.159335607.76402149

Cited by 4 publications

(2 citation statements)

References 23 publications

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“…Um estudo farmacocinético conduzido por Reddy et al (2020) demonstrou que não há necessidade de uma mudança na dosagem da farmacoterapia baseada na idade ou raça, porém o paciente infectado pelo SARS-CoV-2 ao apresentar disfunções hepáticas sofre de um aumento à exposição de determinadas drogas, como a azitromicina, devendo ser utilizada com cautela e frequentemente monitorada.…”

Section: Resumos Expandidosunclassified

Interações Medicamentosas Associadas À Farmacologia Da Covid-19 Em Um Hospital Público Do Sertão De Pernambuco

Sá¹,

Santana²

2021

Anais Do Ii Congresso Norte-Nordeste De Saúde Pública (On Line) Resumos Expandidos

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Introdução. Após um ano de pandemia, apenas o antiviral remdesivir foi aprovado no enfretamento hospitalar ao COVID-19, porém, a farmacoterapia desta infecção, demanda de diversos fármacos para manter a estabilidade respiratória do paciente e os seus sinais vitais. Metodologia: O trabalho foi desenvolvido a partir de uma análise das prescrições de enfrentamento ao COVID-19 no Hospital Regional Inácio de Sá, sendo selecionadas 33 prescrições de diferentes setores de internamento. A verificação das interações ocorreu a partir do site Medscape, sendo classificadas de acordo com o risco ao paciente. Resultado: Um total de 97% das prescrições apresentou interações entre as drogas, sendo os fármacos azitromicina, enoxaparina, dexametasona e ceftriaxona mais frequentes. Apenas as prescrições pediátricas não apresentaram interações, por não utilizarem de múltiplas drogas na terapia. Considerações Finais: Foram identificadas diversas interações entre as drogas, sendo necessários estudos clínicos para verificar as reações adversas provenientes destas interações.

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Section: Resumos Expandidosunclassified

Interações Medicamentosas Associadas À Farmacologia Da Covid-19 Em Um Hospital Público Do Sertão De Pernambuco

Sá¹,

Santana²

2021

Anais Do Ii Congresso Norte-Nordeste De Saúde Pública (On Line) Resumos Expandidos

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“…The peptidic inhibitor, called N3, (half-maximal inhibitory concentration (IC 50 ) = 16.77 μM) was the first to be cocrystallised with SARS-CoV-2 M pro [ 14 ]. Several other peptidic and nonpeptidic covalent inhibitors have since been described [ 15 ], although none has been approved as a cure for COVID-19 to date. On the other hand, noncovalently interacting small molecules may produce fewer off-target side effects and toxicity [ 16 ]; therefore, our work focuses on these.…”

Section: Introductionmentioning

confidence: 99%

Novel Small-Molecule Scaffolds as Candidates against the SARS Coronavirus 2 Main Protease: A Fragment-Guided in Silico Approach

et al. 2020

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The ongoing pandemic caused by the novel coronavirus has been the greatest global health crisis since the Spanish flu pandemic of 1918. Thus far, severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) has resulted in over 1 million deaths, and there is no cure or vaccine to date. The recently solved crystal structure of the SARS-CoV-2 main protease has been a major focus for drug-discovery efforts. Here, we present a fragment-guided approach using ZINCPharmer, where 17 active fragments known to bind to the catalytic centre of the SARS-CoV-2 main protease (SARS-CoV-2 Mpro) were used as pharmacophore queries to search the ZINC databases of natural compounds and natural derivatives. This search yielded 134 hits that were then subjected to multiple rounds of in silico analyses, including blind and focused docking against the 3D structure of the main protease. We scrutinised the poses, scores, and protein–ligand interactions of 15 hits and selected 7. The scaffolds of the seven hits were structurally distinct from known inhibitor scaffolds, thus indicating scaffold novelty. Our work presents several novel scaffolds as potential candidates for experimental validation against SARS-CoV-2 Mpro.

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The investigation of the complex population-drug-drug interaction between ritonavir-boosted lopinavir and chloroquine or ivermectin using physiologically-based pharmacokinetic modeling

Alsmadi

2022

Drug Metabolism and Personalized Therapy

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Objectives Therapy failure caused by complex population-drug-drug (PDDI) interactions including CYP3A4 can be predicted using mechanistic physiologically-based pharmacokinetic (PBPK) modeling. A synergy between ritonavir-boosted lopinavir (LPVr), ivermectin, and chloroquine was suggested to improve COVID-19 treatment. This work aimed to study the PDDI of the two CYP3A4 substrates (ivermectin and chloroquine) with LPVr in mild-to-moderate COVID-19 adults, geriatrics, and pregnancy populations. Methods The PDDI of LPVr with ivermectin or chloroquine was investigated. Pearson’s correlations between plasma, saliva, and lung interstitial fluid (ISF) levels were evaluated. Target site (lung epithelial lining fluid (ELF)) levels of ivermectin and chloroquine were estimated. Results Upon LPVr coadministration, while the chloroquine plasma levels were reduced by 30, 40, and 20%, the ivermectin plasma levels were increased by a minimum of 425, 234, and 453% in adults, geriatrics, and pregnancy populations, respectively. The established correlation equations can be useful in therapeutic drug monitoring (TDM) and dosing regimen optimization. Conclusions Neither chloroquine nor ivermectin reached therapeutic ELF levels in the presence of LPVr despite reaching toxic ivermectin plasma levels. PBPK modeling, guided with TDM in saliva, can be advantageous to evaluate the probability of reaching therapeutic ELF levels in the presence of PDDI, especially in home-treated patients.

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Pharmacokinetics under the COVID-19 storm!

Cited by 4 publications

References 23 publications

Interações Medicamentosas Associadas À Farmacologia Da Covid-19 Em Um Hospital Público Do Sertão De Pernambuco

Interações Medicamentosas Associadas À Farmacologia Da Covid-19 Em Um Hospital Público Do Sertão De Pernambuco

Novel Small-Molecule Scaffolds as Candidates against the SARS Coronavirus 2 Main Protease: A Fragment-Guided in Silico Approach

The investigation of the complex population-drug-drug interaction between ritonavir-boosted lopinavir and chloroquine or ivermectin using physiologically-based pharmacokinetic modeling

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