Your search keyword '"HIV protease inhibitors"' showing total 10,965 results

1. Safety and Efficacy of a Switch to Doravirine, Tenofovir, Lamivudine (MK-1439A) in Human Immunodeficiency Virus (HIV-1)-Infected Participants Virologically Suppressed on an Anti-retroviral Regimen in Combination With Two Nucleoside Reverse Transcriptase Inhibitors (MK-1439A-024) (DRIVE-SHIFT)

Published

2024

2. Strategies and Treatments for Respiratory Infections & Viral Emergencies (STRIVE): Shionogi Protease Inhibitor (Ensitrelvir)

Author

National Institute of Allergy and Infectious Diseases (NIAID)

Published

2024

3. Evaluation of CYT-108, a Recombinant Protease Inhibitor, for Treatment of Mild to Moderate Primary Osteoarthritis of the Knee

Author

Southern Star Research Pty Ltd.

Published

2024

4. Preventing stress ulcer bleeding.

Author

Young, Paul J., Cook, Deborah J., and Deane, Adam M.

Subjects

*MACHINE learning, *GASTROINTESTINAL hemorrhage, *PROTON pump inhibitors, *HIV protease inhibitors, *BARRETT'S esophagus, *RENAL replacement therapy, *PRESSURE ulcers, *INTERNATIONAL normalized ratio, *ARTIFICIAL respiration

Abstract

The document discusses stress ulcer bleeding as a complication of critical illness and the use of stress ulcer prophylaxis to prevent such ulcers. Proton pump inhibitors are the main agents prescribed for stress ulcer prophylaxis, with histamine-2-receptor blockers being less commonly used. The document also highlights the challenges of predicting the severity of bleeding episodes and the uncertainty surrounding the effect of stress ulcer prophylaxis on mortality. Additionally, it explores the potential impact of enteral nutrition on bleeding risk and the importance of discontinuing stress ulcer prophylaxis when no longer needed. [Extracted from the article]

Published

2024

5. Pharmacokinetics of once-daily darunavir/ritonavir in second-line treatment in African children with HIV.

Author

Tsirizani, Lufina, Naghani, Shaghayegh Mohsenian, Waalewijn, Hylke, Szubert, Alexander, Mulenga, Veronica, Chabala, Chishala, Bwakura-Dangarembizi, Mutsa, Chitsamatanga, Moses, Rutebarika, Diana A, Musiime, Victor, Kasozi, Mariam, Lugemwa, Abbas, Monkiewicz, Lara N, McIlleron, Helen M, Burger, David M, Gibb, Diana M, Denti, Paolo, Wasmann, Roeland E, and Colbers, Angela

Subjects

*HIV protease inhibitors, *HIV-positive children, *DARUNAVIR, *RITONAVIR, *TENOFOVIR, *LAMIVUDINE

Abstract

Background Darunavir is a potent HIV protease inhibitor with a high barrier to resistance. We conducted a nested pharmacokinetic sub-study within CHAPAS-4 to evaluate darunavir exposure in African children with HIV, taking once-daily darunavir/ritonavir for second-line treatment. Methods We used data from the CHAPAS-4 pharmacokinetic sub-study treating children with once-daily darunavir/ritonavir (600/100 mg if 14–24.9 kg and 800/100 mg if ≥25 kg) with either tenofovir alafenamide fumarate (TAF)/emtricitabine (FTC), abacavir/lamivudine or zidovudine/lamivudine. Steady-state pharmacokinetic sampling was done at 0, 1, 2, 4, 6, 8, 12 and 24 hours after observed darunavir/ritonavir intake. Non-compartmental and population pharmacokinetic analyses were used to describe the data and identify significant covariates. Reference adult pharmacokinetic data were used for comparison. We simulated the World Health Organization (WHO) recommended 600/100 mg darunavir/ritonavir dose for the 25–34.9 kg weight band. Results Data from 59 children with median age and weight 10.9 (range 3.8–14.7) years and 26.0 (14.5–47.0) kg, respectively, were available. A two-compartment disposition model with transit absorption compartments and weight-based allometric scaling of clearance and volume best described darunavir data. Our population achieved geometric mean (%CV) darunavir AUC0–24h, 94.3(50) mg·h/L and C max, 9.1(35) mg/L, above adult reference values and C trough, 1.5(111) mg/L, like adult values. The nucleoside reverse-transcriptase inhibitor backbone was not found to affect darunavir concentrations. Simulated WHO-recommended darunavir/ritonavir doses showed exposures equivalent to adults. Higher alpha-1-acid glycoprotein increased binding to darunavir and decreased apparent clearance of darunavir. Conclusions Darunavir exposures achieved in our trial are within safe range. Darunavir/ritonavir can safely be co-administered with TAF/FTC. Both WHO-recommended 600/100 mg and CHAPAS-4 800/100 mg darunavir/ritonavir doses for the 25–34.9 kg weight band offer favourable exposures. The choice between them can depend on tablet availability. [ABSTRACT FROM AUTHOR]

Published

2024

6. Brief communication: The extent and determinants of viral suppression among patients on protease inhibitor-based Anti-retro-viral therapy undergoing intensive adherence counselling in a public HIV care center in Uganda.

Author

Lukyamuzi, Zubair, Ibanda, Hood, Ggita, Joseph, Mawanda, Denis, Gati, Brenda M, Nakalega, Rita, and Kiguba, Ronald

Subjects

*CLINICAL drug trials, *PATIENT compliance, *VIRAL load, *SOCIAL determinants of health, *STATISTICAL significance, *RESEARCH funding, *HIV protease inhibitors, *HIV infections, *TREATMENT effectiveness, *RETROSPECTIVE studies, *DESCRIPTIVE statistics, *THEMATIC analysis, *RESEARCH methodology, *MEDICAL records, *ACQUISITION of data, *METROPOLITAN areas, *ANTI-HIV agents, *COUNSELING, *PUBLIC health, *HEALTH facilities, *DATA analysis software, *PATIENTS' attitudes

Abstract

Background: Protease inhibitor (PI)-based Antiretroviral Therapy (ART) regimens are key drugs in HIV management, especially when used as second line drugs. However, some PI-based ART have high adherence demands or tolerable adverse effects which may affect adherence and subsequently viral suppression. We assessed the extent of viral suppression, its determinants, and the experiences of clients on PI-based ART undergoing intensive adherence counselling (IAC) in a public HIV clinic. Methods: Mixed methods sequential explanatory study involving a quantitative retrospective chart review for clients on PI-based ART who had received IAC from Dec 2016 to May 2023 and qualitative interviews for clients on PI-based ART who had received IAC in the past six months at an urban public HIV clinic in Uganda. Results: In this study, a total of 189 client charts were included. The median number of IAC sessions received was three (interquartile range, IQR, of 3 to 4) with median time of receiving IAC of three (IQR, of 2 to 4). One half (51%, 95/186) of the clients had achieved viral suppression and the odds of suppression increased by 30% for every additional month on IAC. Respondents perceived the effectiveness of PI-based ART and IAC in achieving and supporting viral suppression, respectively. Conclusion: Despite the perceived effectiveness of PI-based ART and IAC, suboptimal levels of viral suppression were observed among clients on PI-based ART who had received IAC. Therefore, it is important to provide IAC for optimal duration as it increases the chances of viral suppression. Further investigation of the barriers of viral suppression for clients on PI-based ART undergoing IAC is needed. [ABSTRACT FROM AUTHOR]

Published

2024

7. Ritonavir's Evolving Role: A Journey from Antiretroviral Therapy to Broader Medical Applications.

Author

Pereira, Mariana and Vale, Nuno

Subjects

*CYTOCHROME P-450 CYP3A, *HEAT shock proteins, *CANCER cell proliferation, *DRUG repositioning, *ANTINEOPLASTIC agents, *HIV protease inhibitors, *CYCLIN-dependent kinases

Abstract

Ritonavir is a protease inhibitor initially developed for HIV treatment that is now used as a pharmacokinetic booster for other antiretrovirals due to it being a cytochrome P450 3A4 enzyme and P-glycoprotein inhibitor. Consequently, ritonavir is of special interest for repurposing in other diseases. It had an important role in battling the COVID-19 pandemic as a part of the developed drug Paxlovid® in association with nirmatrelvir and has shown effects in hepatitis and other pathogenic diseases. Ritonavir has also shown promising results in overcoming drug resistance and enhancing the efficacy of existing chemotherapeutic agents in oncology. Evidence of cancer repurposing potential was demonstrated in cancers such as ovarian, prostate, lung, myeloma, breast, and bladder cancer, with several mechanisms of action presented. In vitro studies indicate that ritonavir alone can inhibit key pathways involved in cancer cell survival and proliferation, causing apoptosis, cell cycle arrest, endoplasmic reticulum stress, and metabolic stress due to the inhibition of molecules like heat shock protein 90 and cyclin-dependent kinases. Ritonavir also causes resistant cells to become sensitized to anticancer drugs like gemcitabine or docetaxel. These findings indicate that repurposing ritonavir, either on its own or in combination with other medications, could be a promising approach for treating various diseases. This is particularly relevant in cancer therapy, where ritonavir repurposing is the central focus of this review. [ABSTRACT FROM AUTHOR]

Published

2024

8. Susceptibility of HPV-18 Cancer Cells to HIV Protease Inhibitors.

Author

Makgoo, Lilian, Mosebi, Salerwe, and Mbita, Zukile

Subjects

*HIV protease inhibitors, *HUMAN papillomavirus, *CERVICAL cancer, *HIV, *CELL cycle, *PAPILLOMAVIRUSES

Abstract

Cervical cancer cases continue to rise despite all the advanced screening and preventative measures put in place, which include human papillomavirus (HPV) vaccination. These soaring numbers can be attributed to the lack of effective anticancer drugs against cervical cancer; thus, repurposing the human immunodeficiency virus protease inhibitors is an attractive innovation. Therefore, this work was aimed at evaluating the potential anticancer activities of HIV-PIs against cervical cancer cells. The MTT viability assay was used to evaluate the effect of HIV protease inhibitors on the viability of cervical cancer cells (HeLa) and non-cancerous cells (HEK-293). Further confirmation of the MTT assay was performed by confirming the IC50s of these HIV protease inhibitors on cervical cancer cells and non-cancerous cells using the Muse™ Count and Viability assay. To confirm the mode of death induced by HIV protease inhibitors in the HPV-associated cervical cancer cell line, apoptosis was performed using Annexin V assay. In addition, the Muse™ Cell Cycle assay was used to check whether the HIV protease inhibitors promote or halt cell cycle progression in cervical cancer cells. HIV protease inhibitors did not affect the viability of non-cancerous cells (HEK-293), but they decreased the viability of HeLa cervical cancer cells in a dose-dependent manner. HIV protease inhibitors induced apoptosis in HPV-related cervical cancer cells. Furthermore, they also induced cell cycle arrest, thus halting cell cycle progression. Therefore, the use of HIV drugs, particularly HIV-1 protease inhibitors, as potential cancer therapeutics represents a promising strategy. This is supported by our study demonstrating their anticancer properties, notably in HPV-associated cervical cancer cell line. [ABSTRACT FROM AUTHOR]

Published

2024

9. In Silico Investigation of Molecular Properties and Molecular Docking of Darunavir: An Anti‐HIV Drug.

Author

Kumar, Shiv, Tiwari, Gargi, and Sharma, Dipendra

Subjects

*HIV protease inhibitors, *MOLECULAR docking, *MOLECULAR shapes, *PROTEIN receptors, *DENSITY functional theory

Abstract

A second‐generation HIV protease enzyme inhibitor, darunavir is used in combination therapy for patients with history of prior antiretroviral treatments. It inhibits the cleavage of HIV encoded gag‐pol polyprotein in cells contaminated by a virus and thereby hinders the development of mature and infectious new virions. In this paper, optimization of molecular geometry of darunavir has been obtained by Density Functional Theory based B3LYP and ωB97XD methods with 6–311+G(d,p) basis set. The electro‐optical, global reactivity descriptors, and UV–visible spectrum of the drug have been examined using both the functionals. Further, binding affinity of darunavir at different sites of protein receptor (PDB ID: 5b18) has been analyzed using molecular docking technique. Results have been used to discuss electro‐optical and electronic properties of the drug along with its binding affinities with protein receptors. [ABSTRACT FROM AUTHOR]

Published

2024

10. Clinical characteristics of women with HIV in the RESPOND cohort: A descriptive analysis and comparison to men.

Author

Hutchinson, J., Neesgard, B., Kowalska, J., Grabmeier‐Pfistershammer, K., Johnson, M., Kusejko, K., De Wit, S., Wit, F., Mussini, C., Castagna, A., Stecher, M., Pradier, C., Domingo, P., Carlander, C., Wasmuth, J., Chkhartishvili, N., Uzdaviniene, V., Haberl, A., d'Arminio Monforte, A., and Garges, H.

Subjects

*HIV integrase inhibitors, *WOMEN, *VIRAL load, *ANTIRETROVIRAL agents, *SECONDARY analysis, *RESEARCH funding, *HIV-positive persons, *CD4 lymphocyte count, *SEX distribution, *HIV protease inhibitors, *HIV infections, *SEVERITY of illness index, *DESCRIPTIVE statistics, *AGE distribution, *MEN who have sex with men, *RACE, *INFECTIOUS disease transmission, *COMORBIDITY, *NUCLEOSIDE reverse transcriptase inhibitors, *SYMPTOMS

Abstract

Background: Women with HIV are globally underrepresented in clinical research. Existing studies often focus on reproductive outcomes, seldom focus on older women, and are often underpowered to assess sex/gender differences. We describe CD4, HIV viral load (VL), clinical characteristics, comorbidity burden, and use of antiretroviral therapy (ART) among women with HIV in the RESPOND study and compare them with those of the men in RESPOND. Methods: RESPOND is a prospective, multi‐cohort collaboration including over 34 000 people with HIV from across Europe and Australia. Demographic and clinical characteristics, including CD4/VL, comorbidity burden, and ART are presented at baseline, defined as the latter of 1 January 2012 or enrolment into the local cohort, stratified by age and sex/gender. We further stratify men by reported mode of HIV acquisition, men who have sex with men (MSM) and non‐MSM. Results: Women account for 26.0% (n = 9019) of the cohort, with a median age of 42.2 years (interquartile range [IQR] 34.7–49.1). The majority (59.3%) of women were white, followed by 30.3% Black. Most women (75.8%) had acquired HIV heterosexually and 15.9% via injecting drug use. Nearly half (44.8%) were receiving a boosted protease inhibitor, 31.4% a non‐nucleoside reverse transcriptase inhibitor, and 7.8% an integrase strand transfer inhibitor. The baseline year was 2012 for 73.2% of women and >2019 for 4.2%. Median CD4 was 523 (IQR 350–722) cells/μl, and 73.6% of women had a VL <200 copies/mL. Among the ART‐naïve population, women were more likely than MSM but less likely than non‐MSM (p < 0.001) to have CD4 <200 cells/μL and less likely than both MSM and non‐MSM (p < 0.001) to have VL ≥100 000 copies/mL. Women were also more likely to be free of comorbidity than were both MSM and non‐MSM (p < 0.0001). Conclusion: RESPOND women are diverse in age, ethnicity/race, CD4/VL, and comorbidity burden, with important differences relative to men. This work highlights the importance of stratification by sex/gender for future research that may help improve screening and management guidelines specifically for women with HIV. [ABSTRACT FROM AUTHOR]

Published

2024

11. Increased incidence of diabetes in people living with HIV treated with first‐line integrase strand transfer inhibitors: A French multicentre retrospective study.

Author

Ursenbach, Axel, Sireyjol, Antoine, Delpierre, Cyrille, Duvivier, Claudine, Hocqueloux, Laurent, and Rey, David

Subjects

*PEOPLE with diabetes, *REVERSE transcriptase inhibitors, *HIV-positive persons, *INTEGRASE inhibitors, *ANTIRETROVIRAL agents, *HIV protease inhibitors

Abstract

Introduction Methods Results Conclusions Prevention of cardiovascular disease is a major issue in the current management of people living with HIV. Concern is growing about the metabolic impact of integrase strand transfer inhibitors (INSTIs), which could lead to an increased risk of diabetes, but the data are conflicting. This is an updated version of our previous analysis, with longer follow‐up and new molecules.We retrospectively evaluated the incidence of new‐onset diabetes in people living with HIV starting combined antiretroviral therapy with an INSTI compared with non‐nucleoside reverse transcriptase inhibitors and protease inhibitors. Data were collected from the Dat'AIDS cohort study, a collaboration of 30 HIV treatment centres in France. We used a propensity score‐based inverse probability of treatment weighting approach to adjust for baseline characteristics between the two groups (INSTI and non‐INSTI).Between 2009 and 2021, a total of 12 150 people living with HIV were included. The incidence of diabetes was higher in the INSTI group than in the non‐INSTI group (hazard ratio 1.38; 95% confidence interval 1.07–1.77; p = 0.012). Regardless of the third drug, but to a greater extent for INSTIs, we observed a peak of new‐onset diabetes in the year following initiation of combined antiretroviral therapy.The incidence of diabetes was higher in people treated with integrase inhibitors than in those receiving other third agents. This increased risk occurred both during the first year of treatment and in the longer term. [ABSTRACT FROM AUTHOR]

Published

2024

12. It's good to know what to BACE the specificity of your inhibitors on.

Author

Murray, Aoife, Muñiz-García, Ana, Alić, Ivan, and Nižetić, Dean

Subjects

*AMYLOID beta-protein precursor, *ALZHEIMER'S disease, *PEPTIDES, *HIV protease inhibitors, *AMYLOID

Abstract

Production, aggregation, and clearance of the amyloid β peptide (Aβ) are important processes governing the initial pathogenesis of Alzheimer's disease (AD). Inhibition of β-site amyloid precursor protein (APP) cleaving enzyme (BACE1) (one of two key proteases responsible for Aβ production) as an AD-therapeutic approach so far has failed to yield a successful drug. BACE1 and its homologue BACE2 are frequently inhibited by the same inhibitors. Several genetic and cerebral organoid modeling studies suggest that BACE2 has dose-dependent AD-suppressing activity, which makes its unwanted inhibition potentially counterproductive for AD treatment. The in vivo effects of an unwanted cross inhibition of BACE2 have so far been impossible to monitor because of the lack of an easily accessible pharmacodynamic marker specific for BACE2 cleavage. In this issue of the JCI, work led by Stefan F. Lichtenthaler identifies soluble VEGFR3 (sVEGFR3) as a pharmacodynamic plasma marker for BACE2 activity not shared with BACE1. [ABSTRACT FROM AUTHOR]

Published

2024

13. Advances in the synthesis of (3R,3aS,6aR)-hexahydrofuro-[2,3-b]furan-3-ol, a key ligand of the HIV protease inhibitors.

Author

Dong, Mengqi, Teng, Dawei, and Cao, Guorui

Subjects

*HIV protease inhibitors, *CHIRAL centers, *LIGANDS (Chemistry), *DRUG resistance, *DRUG toxicity

Abstract

(3R,3aS,6aR)-Hexahydrofuro[2,3-b]furan-3-ol (bis-THF alcohol) is a key intermediate for the synthesis of HIV protease inhibitors with lower toxicity and better drug resistance. Due to its unique structure with three chiral centers and the high cost of this double-ring compound, chemists have paid much attention to the development of new synthetic routes. Based on the sources of the chiral carbon in bis-THF alcohol, this work systematically summarizes the existing synthetic processes using enzyme-catalyzed resolution, asymmetric metal catalysis, and chiral-substrate-induced reactions. [ABSTRACT FROM AUTHOR]

Published

2024

14. In silico Rational Design to Discover new Fullerene Derivatives bearing a Catechol Group to Serve as HIV-PR Inhibitors.

Author

Petrakos, Charalabos, Awad, Dimosthenis, and Mavromoustakos, Thomas

Subjects

HIV protease inhibitors, FULLERENE derivatives, BINDING sites, MOLECULAR docking, STERIC hindrance

Abstract

The HIV protease has, for a long time, sparked interest within the scientific community as a great target for potential drugs to fight against AIDS. A group of chemical compounds that show great potential in this regard are fullerene derivatives. In this study we examined and presented a new series of fullerene derivatives that carry a catechol group. Using in silico approaches and molecular docking we carried out experiments to investigate the potential of these derivatives to act as inhibitors for the HIV protease and therefore as drugs for AIDS. The results were very encouraging and so we also examined a plethora of bioisosteres to discover new molecules that showed even greater inhibition of the target enzyme. The exact interactions of these bioisosteres were examined and visualized using PyMOL and through this we were able to discover that these compounds inhibit the active site of the protease by both steric hindrance and direct interaction with the enzyme's active site amino acids. The overall results showed a discovery of many new potential drugs against HIV. [ABSTRACT FROM AUTHOR]

Published

2024

15. Brief Report: Suboptimal Lopinavir Exposure in Infants on Rifampicin Treatment Receiving Double-dosed or Semisuperboosted Lopinavir/Ritonavir: Time for a Change

Author

Jacobs, Tom G, Mumbiro, Vivian, Chitsamatanga, Moses, Namuziya, Natasha, Passanduca, Alfeu, Domínguez-Rodríguez, Sara, Tagarro, Alfredo, Nathoo, Kusum J, Nduna, Bwendo, Ballesteros, Alvaro, Madrid, Lola, Mujuru, Hilda A, Chabala, Chishala, Buck, W Chris, Rojo, Pablo, Burger, David M, Moraleda, Cinta, and Colbers, Angela

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Pediatric, HIV/AIDS, Infectious Diseases, Clinical Research, Clinical Trials and Supportive Activities, Pediatric AIDS, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Infection, Good Health and Well Being, Male, Infant, Humans, Child, Female, Lopinavir, Ritonavir, Rifampin, HIV Infections, Anti-HIV Agents, HIV Protease Inhibitors, lopinavir, infants, rifampin, HIV, tuberculosis, drug-drug interaction, EMPIRICAL Clinical Trial Group, Public Health and Health Services, Virology, Clinical sciences, Epidemiology, Public health

Abstract

BackgroundAlthough super-boosted lopinavir/ritonavir (LPV/r; ratio 4:4 instead of 4:1) is recommended for infants living with HIV and receiving concomitant rifampicin, in clinical practice, many different LPV/r dosing strategies are applied due to poor availability of pediatric separate ritonavir formulations needed to superboost. We evaluated LPV pharmacokinetics in infants with HIV receiving LPV/r dosed according to local guidelines in various sub-Saharan African countries with or without rifampicin-based tuberculosis (TB) treatment.MethodsThis was a 2-arm pharmacokinetic substudy nested within the EMPIRICAL trial (#NCT03915366). Infants aged 1-12 months recruited into the main study were administered LPV/r according to local guidelines and drug availability either with or without rifampicin-based TB treatment; during rifampicin cotreatment, they received double-dosed (ratio 8:2) or semisuperboosted LPV/r (adding a ritonavir 100 mg crushed tablet to the evening LPV/r dose). Six blood samples were taken over 12 hours after intake of LPV/r.ResultsIn total, 14/16 included infants had evaluable pharmacokinetic curves; 9/14 had rifampicin cotreatment (5 received double-dosed and 4 semisuperboosted LPV/r). The median (IQR) age was 6.4 months (5.4-9.8), weight 6.0 kg (5.2-6.8), and 10/14 were male. Of those receiving rifampicin, 6/9 infants (67%) had LPV Ctrough

Published

2023

16. Pharmacokinetics and Safety of Twice-daily Ritonavir-boosted Atazanavir With Rifampicin.

Author

Gausi, Kamunkhwala, Mugerwa, Henry, Siccardi, Marco, Montanha, Maiara Camotti, Lamorde, Mohammed, Wiesner, Lubbe, D'Avolio, Antonio, McIlleron, Helen, Wilkins, Edmund, Nicolò, Amedeo De, Maartens, Gary, Khoo, Saye, Kityo, Cissy, Denti, Paolo, and Waitt, Catriona

Subjects

*PREVENTION of drug side effects, *COMBINATION drug therapy, *PATIENT safety, *RESEARCH funding, *HUMAN beings, *HIV protease inhibitors, *HIV infections, *TREATMENT effectiveness, *DESCRIPTIVE statistics, *DOSE-effect relationship in pharmacology, *ATAZANAVIR, *DRUG interactions, *RITONAVIR, *RIFAMPIN

Abstract

Background Critical drug-drug interactions (DDI) and hepatotoxicity complicate concurrent use of rifampicin and protease inhibitors. We investigated whether dose escalation of atazanavir/ritonavir could safely overcome the DDI with rifampicin. Methods DERIVE (NCT04121195, EDCTP) was a dose-escalation trial in people with human immunodeficiency virus (HIV) on atazanavir/ritonavir-based antiretroviral therapy (ART) in Uganda. Four intensive pharmacokinetic (PK) visits were performed: PK1 300/100 mg OD (baseline); PK2 300/100 mg OD with rifampicin 600 mg; PK3 300/100 mg twice a day (BID) with rifampicin 600 mg OD; PK4 300/100 mg BID with rifampicin 1200 mg OD. Dolutegravir 50 mg BID throughout the study period ensured participants remained protected from subtherapeutic atazanavir concentrations. The data were interpreted with noncompartmental analysis. The target minimum concentration was atazanavir's protein-adjusted IC90 (PA-IC90), 0.014 mg/L. Results We enrolled 26 participants (23 female) with median (range) age 44 (28–61) years and weight 67 (50–75) kg. Compared with PK1, atazanavir Ctau, and AUC were significantly reduced at PK2 by 96% and 85%, respectively. The escalation to BID dosing (PK3) reduced this difference in Ctau, and AUC24 to 18% lower and 8% higher, respectively. Comparable exposures were maintained with double doses of rifampicin. Lowest Ctau during PK1, PK3, and PK4 were 12.7-, 4.8-, and 8.6-fold higher than PA-IC90, respectively, whereas 65% of PK2 Ctau were below the limit of quantification (0.03 mg/L), hence likely below PA-IC90. No participant developed significant elevation of liver enzymes, reported a serious adverse event (SAE) or experienced rebound viraemia. Conclusions Twice daily atazanavir/ritonavir during rifampicin co-administration was well tolerated and achieved plasma concentrations above the target. Clinical Trials Registration NCT04121195. Registered on 09 October 2019, https://clinicaltrials.gov/ct2/show/NCT04121195. [ABSTRACT FROM AUTHOR]

Published

2024

17. Role of apoptotic protease activating factor-1 in CD4+ depletion during HIV progression.

Author

Garuba, Wasiu O., Adedeji, Adebayo L., Adedokun, Kamoru A., Ayelagbe, Olubunmi G., Abdullahi, Idris N., and Munirudeen, Ibrahim

Subjects

*CD4 antigen, *ERYTHROCYTES, *BLOOD proteins, *HIV, *HIV protease inhibitors, *ALBUMINS, *HIV-positive persons

Abstract

Objective: This study investigates the role of Apoptotic Protease Activating Factor-1 (APAF-1) in CD4+ cell depletion among human immunodeficiency virus (HIV) patients. Materials and Methods: This is a cross-sectional study in which 105 participants were enrolled, including 60 confirmed HIV-positive patients and 45 HIV-negative controls. HIV-positive patients were further divided based on CD4+ cell counts: Group 1 (<200), Group 2 (200–499), and Group 3 (≥500). An enzyme-linked immunoassay was used to measure APAF-1 levels, and CD4+ T-cell counts were enumerated using a Cyflow counter. Independent student’s t-test, Kruskal-Wallis, and Spearman’s correlation were utilized as needed. Results: Results showed significant reductions in lymphocytes, platelets, red blood cells, hemoglobin, albumin, and CD4+ cell values among HIV-infected individuals compared to controls. Conversely, APAF-1 and total protein levels were elevated in HIV-positive patients. Among HIV-positive groups, those with CD4+ cell counts <200 exhibited the highest median serum APAF-1 concentration. However, these differences were not statistically significant when compared with the other seropositive groups with CD4+ cell counts between 200 and 499 (P = 0.6726) and CD4+ cell counts of 500 or greater (P = 0.4325). The control group had the lowest median SAPAF-1 concentration, significantly different from HIV-positive groups. Positive correlations were observed between CD4+ counts and lymphocytes, hemoglobin, and hypoalbuminemia, while negative correlations were found between these parameters and APAF-1 levels. Conclusion: APAF-1 is a host factor that potentially contributes to CD4+ cell depletion. Similarly, APAF-1, serum total protein, and albumin levels were found to be predictive of disease progression and could serve as valuable diagnostic biomarkers in the monitoring of HIV/AIDS. [ABSTRACT FROM AUTHOR]

Published

2024

18. Phytochemical profiling of the essential oils from three Curcuma species and their in vitro and in silico dengue protease inhibition activity.

Author

Jani, Nor Akmalazura, Maarof, Noor Inani, Zahari, Miew Mohamad Fitri Miew, Jamil, Mailina, Zakaria, Iffah Izzati, Mohamad Zobir, Siti Zuraidah, Kasim, Noraini, Salin, Nurul Hanim, Mohamad Ali, Nor Azah, Khalid, Wan Elina Faradilla Wan, and Pungot, Noor Hidayah

Subjects

ESSENTIAL oils, CURCUMA, TURMERIC, DENGUE, ROSEMARY, HYDROGEN bonding, HIV protease inhibitors, MORINGA oleifera, RHAMNOLIPIDS

Abstract

The chemical compositions, in vitro and in silico anti-dengue activity of the essential oils of the rhizomes of Curcuma longa Linn., C. aeruginosa Roxb., and C. xanthorrhiza Roxb. had been investigated. The C. longa oil was mainly composed of ar-turmerone (54.0%) and curlone (17.7%), while the C. aeruginosa oil was rich in curzerenone (23.4%), 1,8-cineole (21.2%), and camphor (7.1%). Xanthorrhizol (21.6%), β-curcumene (19.5%), ar-curcumene (14.2%), and camphor (9.2%) were the major compounds in the C. xanthorrhiza oil. Among the oils, the C. longa oil was found to be the most active NSB-NS3 protease inhibitor (IC50 1.98 μg/mL). PLS biplot disclosed that the essential oils were classified into three separated clusters based on their characteristic chemical compositions, with C. longa positioned closest to the in vitro anti-dengue activity. Four compounds from the C. longa oil have both hydrogen and hydrophobic bonds that could be responsible for the DENV-2 NS2B-NS3 inhibitory effect. [ABSTRACT FROM AUTHOR]

Published

2024

19. The regulatory role and mechanism of USP14 in endothelial cell pyroptosis induced by coronary heart disease.

Author

Gao, Jie and Gao, Zhao

Subjects

*DEUBIQUITINATING enzymes, *CORONARY disease, *ENDOTHELIAL cells, *NLRP3 protein, *PYROPTOSIS, *HIV protease inhibitors

Abstract

OBJECTIVE: The present study probes into the role and mechanism of ubiquitin specific peptidase 14 (USP14) in coronary heart disease (CHD)-triggered endothelial cell pyroptosis. METHODS: An in vitro CHD model was established by inducing human coronary artery endothelial cells (HCAECs) with oxidized low-density lipoprotein (ox-LDL). HCAECs were transfected with si-USP14, followed by evaluation of cell viability by CCK-8 assay, detection of lactate dehydrogenase (LDH) activity by assay kit, detection of USP14, miR-15b-5p, NLRP3, GSDMD-N, and Cleaved-Caspase-1 expressions by qRT-PCR or Western blot, as well as IL-1β and IL-18 concentrations by ELISA. Co-IP confirmed the binding between USP14 and NLRP3. The ubiquitination level of NLRP3 in cells was measured after protease inhibitor MG132 treatment. Dual-luciferase reporter assay verified the targeting relationship between miR-15b-5p and USP14. RESULTS: USP14 and NLRP3 were highly expressed but miR-15b-5p was poorly expressed in ox-LDL-exposed HCAECs. USP14 silencing strengthened the viability of ox-LDL-exposed HCAECs, reduced the intracellular LDH activity, and diminished the NLRP3, GSDMD-N, Cleaved-Caspase-1, IL-1β, and IL-18 expressions. USP14 bound to NLRP3 protein and curbed its ubiquitination. Repression of NLRP3 ubiquitination counteracted the inhibitory effect of USP14 silencing on HCAEC pyroptosis. miR-15b-5p restrained USP14 transcription and protein expression. miR-15b-5p overexpression alleviated HCAEC pyroptosis by suppressing USP14/NLRP3. CONCLUSION: USP14 stabilizes NLRP3 protein expression through deubiquitination, thereby facilitating endothelial cell pyroptosis in CHD. miR-15b-5p restrains endothelial cell pyroptosis by targeting USP14 expression. [ABSTRACT FROM AUTHOR]

Published

2024

20. Novel diarylpyrimidine subtypes as HIV‐1 nonnucleoside reverse transcriptase inhibitors with improved resistance profile.

Author

Wang, Zhengqiang

Subjects

REVERSE transcriptase inhibitors, EMTRICITABINE, HIV protease inhibitors, HIV, NON-nucleoside reverse transcriptase inhibitors

Abstract

This article discusses the development of novel diarylpyrimidine subtypes as HIV-1 nonnucleoside reverse transcriptase inhibitors (NNRTIs) with improved resistance profiles. The article explains that the virally encoded reverse transcriptase (RT) is a target for HIV drugs, and while nucleos(t)ide RT inhibitors (NRTIs) and first-generation NNRTIs have been approved, RT RNase H has not been targeted. The second-generation NNRTIs, including dapivirine (DPV), have shown improved resistance profiles. The article then focuses on a recent study that identified analog 11b1 as a potent NNRTI with exceptional potency and resistance profile, validating the new DAPY subtype as an important chemical platform for developing improved DAPY NNRTIs. [Extracted from the article]

Published

2024

21. Conformational Polymorphism of Elsulfavirine Sodium Salt.

Author

Volodin, A. D., Vologzhanina, A. V., Peresypkina, E. V., and Korlyukov, A. A.

Subjects

*STACKING interactions, *PHENYL group, *X-ray diffraction, *HIV protease inhibitors, *CONFORMATIONAL analysis

Abstract

The X-ray diffraction analysis of two polymorphs of sodium (cis)-N-((4-(2-(4-bromo-3-(3-chloro-5-cyanophenoxy)-2-fluorophenyl)acetamido)-3-chlorophenyl)sulfonyl)propioimide shows that the organic anion in them is in elongated and globular conformations. Both conformations are characterized by the absence of strong intramolecular interactions. According to the quantum chemical study, both the isolated anion in the globular conformation and the polymorph containing it are more thermodynamically stable, and the difference in free energies of the polymorphs increases with temperature, which is explained by the role of the entropy factor. The elongated conformation is stabilized in the crystal by interanionic Hal...π interactions and stacking interactions involving the phenyl groups. [ABSTRACT FROM AUTHOR]

Published

2024

22. Enhanced antifungal activity of posaconazole against Candida auris by HIV protease inhibitors, atazanavir and saquinavir.

Author

Elgammal, Yehia, Salama, Ehab A., and Seleem, Mohamed N.

Subjects

*ATAZANAVIR, *HIV protease inhibitors, *CANDIDA, *ANTIFUNGAL agents

Abstract

The increasing incidence and dissemination of multidrug-resistant Candida auris represents a serious global threat. The emergence of pan-resistant C. auris exhibiting resistance to all three classes of antifungals magnifies the need for novel therapeutic interventions. We identified that two HIV protease inhibitors, atazanavir and saquinavir, in combination with posaconazole exhibited potent activity against C. auris in vitro and in vivo. Both atazanavir and saquinavir exhibited a remarkable synergistic activity with posaconazole against all tested C. auris isolates and other medically important Candida species. In a time-kill assay, both drugs restored the fungistatic activity of posaconazole, resulting in reduction of 5 and 5.6 log10, respectively. Furthermore, in contrast to the individual drugs, the two combinations effectively inhibited the biofilm formation of C. auris by 66.2 and 81.2%, respectively. Finally, the efficacy of the two combinations were tested in a mouse model of C. auris infection. The atazanavir/posaconazole and saquinavir/posaconazole combinations significantly reduced the C. auris burden in mice kidneys by 2.04- (99.1%) and 1.44-log10 (96.4%) colony forming unit, respectively. Altogether, these results suggest that the combination of posaconazole with the HIV protease inhibitors warrants further investigation as a new therapeutic regimen for the treatment of C. auris infections. [ABSTRACT FROM AUTHOR]

Published

2024

23. Conformational diversity and protein–protein interfaces in drug repurposing in Ras signaling pathway.

Author

Sayin, Ahenk Zeynep, Abali, Zeynep, Senyuz, Simge, Cankara, Fatma, Gursoy, Attila, and Keskin, Ozlem

Subjects

*DRUG repositioning, *CELLULAR signal transduction, *HIV protease inhibitors, *ALZHEIMER'S disease, *CYTOSKELETAL proteins

Abstract

We focus on drug repurposing in the Ras signaling pathway, considering structural similarities of protein–protein interfaces. The interfaces formed by physically interacting proteins are found from PDB if available and via PRISM (PRotein Interaction by Structural Matching) otherwise. The structural coverage of these interactions has been increased from 21 to 92% using PRISM. Multiple conformations of each protein are used to include protein dynamics and diversity. Next, we find FDA-approved drugs bound to structurally similar protein–protein interfaces. The results suggest that HIV protease inhibitors tipranavir, indinavir, and saquinavir may bind to EGFR and ERBB3/HER3 interface. Tipranavir and indinavir may also bind to EGFR and ERBB2/HER2 interface. Additionally, a drug used in Alzheimer's disease can bind to RAF1 and BRAF interface. Hence, we propose a methodology to find drugs to be potentially used for cancer using a dataset of structurally similar protein–protein interface clusters rather than pockets in a systematic way. [ABSTRACT FROM AUTHOR]

Published

2024

24. Pharmacological Inhibition of the Cysteine Protease Cathepsin C Improves Graft Function after Heart Transplantation in Rats.

Author

Liu, B., Korkmaz, B., Kraft, P., Mayer, T., Sayour, A., Grundl, M., Karck, M., Szabó, G., and Korkmaz-Icöz, S.

Subjects

*HEART transplantation, *RATS, *CYSTEINE, *LABORATORY rats, *BONE marrow cells, *HIV protease inhibitors, *LEUCOCYTE elastase

Abstract

This article, published in the journal Thoracic & Cardiovascular Surgeon, explores the potential benefits of inhibiting the cysteine protease cathepsin C (CatC) in improving graft function after heart transplantation (HTX) in rats. The study found that the CatC inhibitor BI-9740 decreased the proteolytic activity of neutrophil serine proteases and improved both systolic and diastolic function in the transplanted hearts. Additionally, the inhibitor was associated with a shorter graft re-beating time. These findings suggest that pharmacological inhibition of CatC may be a promising approach to enhance graft function after HTX. [Extracted from the article]

Published

2024

25. Impact of Protease Inhibitor-Based Highly Active Antiretroviral Therapy on Fetal Subcutaneous Fat Tissue in HIV-Pregnant Women in a Middle-Income Country.

Author

Borboa-Olivares, Hector, Estrada-Gutierrez, Guadalupe, Martinez-Portilla, Raigam Jafet, Espino-y-Sosa, Salvador, Flores-Pliego, Arturo, Espejel-Nuñez, Aurora, Camacho-Arroyo, Ignacio, Solis-Paredes, Juan Mario, Villafan-Bernal, Jose Rafael, and Torres-Torres, Johnatan

Subjects

*HIV protease inhibitors, *HIGHLY active antiretroviral therapy, *ADIPOSE tissues, *MIDDLE-income countries, *CHILDBEARING age, *FAT, *BODY composition

Abstract

Background: HIV infection continues to be a global public health challenge, affecting approximately 1.7 million reproductive-aged women. Protease inhibitor-based highly active antiretroviral therapy (PI-HAART) has significantly reduced the risk of vertical transmission of HIV from mother to child. Nevertheless, concerns linger regarding the long-term effects, particularly on body composition, notably subcutaneous fat tissue (SFT). Although HIV-associated lipodystrophy syndrome (LS) has been well documented in adults and older children, its impact on fetuses exposed to PI-HAART remains underexplored. This study aims to evaluate SFT in the fetuses of HIV-pregnant women exposed to PI-HAART, assessing the potential clinical implications. Methods: We conducted a comparative study between HIV-pregnant women receiving PI-HAART and an HIV-negative control group. Fetometry measurements were obtained via 3D ultrasound. SFT in the fetal arm and thigh segments was assessed. Data were analyzed using lineal multivariate regression and receiver-operating characteristics (ROC)-curve analysis. Results: Fetuses exposed to PI-HAART exhibited a significant reduction in subcutaneous fat, particularly in the proximal third-middle union of the femur (coefficient: −2.588, p = 0.042). This reduction was correlated with lower newborn serum glucose levels (65.7 vs. 56.1, p = 0.007; coefficient: −1.277, p = 0.045). Conclusions: Our study sheds light on the connection between PI-HAART, fetal subcutaneous fat, and neonatal health. These findings might reveal the long-lasting effects of PI-HAART on newborns and children's well-being. Our results emphasize the need for a more balanced approach to managing pregnant women with HIV in developing countries and open new venues for research on the impact of intrauterine PI-HAART exposure on energy metabolism and fetal programming. [ABSTRACT FROM AUTHOR]

Published

2024

26. Computer-Aided Prediction of the Interactions of Viral Proteases with Antiviral Drugs: Antiviral Potential of Broad-Spectrum Drugs.

Author

Ren, Pengxuan, Li, Shiwei, Wang, Shihang, Zhang, Xianglei, and Bai, Fang

Subjects

*ANTIVIRAL agents, *HIV protease inhibitors, *PROTEASE inhibitors, *DNA-binding proteins, *VIRUS diseases, *PROTEIN-protein interactions, *PROTEOLYTIC enzymes

Abstract

Human society is facing the threat of various viruses. Proteases are promising targets for the treatment of viral infections. In this study, we collected and profiled 170 protease sequences from 125 viruses that infect humans. Approximately 73 of them are viral 3-chymotrypsin-like proteases (3CLpro), and 11 are pepsin-like aspartic proteases (PAPs). Their sequences, structures, and substrate characteristics were carefully analyzed to identify their conserved nature for proposing a pan-3CLpro or pan-PAPs inhibitor design strategy. To achieve this, we used computational prediction and modeling methods to predict the binding complex structures for those 73 3CLpro with 4 protease inhibitors of SARS-CoV-2 and 11 protease inhibitors of HCV. Similarly, the complex structures for the 11 viral PAPs with 9 protease inhibitors of HIV were also obtained. The binding affinities between these compounds and proteins were also evaluated to assess their pan-protease inhibition via MM-GBSA. Based on the drugs targeting viral 3CLpro and PAPs, repositioning of the active compounds identified several potential uses for these drug molecules. As a result, Compounds 1–2, modified based on the structures of Ray1216 and Asunaprevir, indicate potential inhibition of DENV protease according to our computational simulation results. These studies offer ideas and insights for future research in the design of broad-spectrum antiviral drugs. [ABSTRACT FROM AUTHOR]

Published

2024

27. Pharmacokinetics of Atazanavir Boosted With Cobicistat in Pregnant and Postpartum Women With HIV

Author

Momper, Jeremiah D, Wang, Jiajia, Stek, Alice, Shapiro, David E, Powis, Kathleen M, Paul, Mary E, Badell, Martina L, Browning, Renee, Chakhtoura, Nahida, Denson, Kayla, Rungruengthanakit, Kittipong, George, Kathleen, Capparelli, Edmund V, Mirochnick, Mark, Best, Brookie M, and Team, for the IMPAACT P1026s Protocol

Subjects

Reproductive Medicine, Biomedical and Clinical Sciences, Perinatal Period - Conditions Originating in Perinatal Period, Pediatric Research Initiative, Pediatric, Clinical Research, Prevention, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Reproductive health and childbirth, Anti-HIV Agents, Atazanavir Sulfate, Child, Cobicistat, Female, HIV Infections, HIV Protease Inhibitors, Humans, Infectious Disease Transmission, Vertical, Placenta, Postpartum Period, Pregnancy, Pregnancy Complications, Infectious, Prospective Studies, atazanavir, cobicistat, HIV, pharmacokinetics, perinatal transmission, pregnancy, IMPAACT P1026s Protocol Team, Clinical Sciences, Public Health and Health Services, Virology, Clinical sciences, Epidemiology, Public health

Abstract

BackgroundThis study evaluated atazanavir and cobicistat pharmacokinetics during pregnancy compared with postpartum and in infant washout samples.SettingA nonrandomized, open-label, parallel-group, multicenter prospective study of atazanavir and cobicistat pharmacokinetics in pregnant women with HIV and their children.MethodsIntensive steady-state 24-hour pharmacokinetic profiles were performed after administration of 300 mg of atazanavir and 150 mg of cobicistat orally in fixed-dose combination once daily during the second trimester, third trimester, and postpartum. Infant washout samples were collected after birth. Atazanavir and cobicistat were measured in plasma by validated high-performance liquid chromatography-ultraviolet and liquid chromatography-tandem mass spectrometry assays, respectively. A 2-tailed Wilcoxon signed-rank test (α = 0.10) was used for paired within-participant comparisons.ResultsA total of 11 pregnant women enrolled in the study. Compared with paired postpartum data, atazanavir AUC0-24 was 26% lower in the second trimester [n = 5, P = 0.1875, geometric mean of ratio (GMR) = 0.739, 90% CI: 0.527 to 1.035] and 54% lower in the third trimester (n = 6, GMR = 0.459, P = 0.1563, 90% CI: 0.190 to 1.109), whereas cobicistat AUC0-24 was 35% lower in the second trimester (n = 5, P = 0.0625, GMR = 0.650, 90% CI: 0.493 to 0.858) and 52% lower in the third trimester (n = 7, P = 0.0156, GMR = 0.480, 90% CI: 0.299 to 0.772). The median (interquartile range) 24-hour atazanavir trough concentration was 0.21 μg/mL (0.16-0.28) in the second trimester, 0.21 μg/mL (0.11-0.56) in the third trimester, and 0.61 μg/mL (0.42-1.03) in postpartum. Placental transfer of atazanavir and cobicistat was limited.ConclusionsStandard atazanavir/cobicistat dosing during pregnancy results in lower exposure which may increase the risk of virologic failure and perinatal transmission.

Published

2022

28. Interactions between etonogestrel-releasing contraceptive implant and 3 antiretroviral regimens

Author

Kreitchmann, Regis, Stek, Alice, Best, Brookie M, Capparelli, Edmund, Wang, JiaJia, Shapiro, David, Chakhtoura, Nahida, Mirochnick, Mark, Eke, Ahizechukwu C, and team, for the IMPAACT P1026s protocol

Subjects

Reproductive Medicine, Biomedical and Clinical Sciences, Prevention, Infectious Diseases, HIV/AIDS, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Infection, Good Health and Well Being, Anti-HIV Agents, Atazanavir Sulfate, Contraceptive Agents, Desogestrel, Drug Combinations, Female, HIV Infections, HIV Protease Inhibitors, Humans, Ritonavir, Long-acting reversible contraceptives, Etonogestrel, Efavirenz, Atazanavir, Lopinavir, Pharmacokinetics, IMPAACT P1026s protocol team, Clinical Sciences, Paediatrics and Reproductive Medicine, Public Health and Health Services, Obstetrics & Reproductive Medicine, Clinical sciences, Reproductive medicine, Health services and systems

Abstract

ObjectivesLong-acting reversible contraceptives are effective contraceptives for women with HIV, but there are limited data on etonogestrel implant and antiretroviral therapy pharmacokinetic drug-drug interactions. We evaluated etonogestrel/antiretroviral therapy drug-drug interactions, and the effects of etonogestrel on ritonavir-boosted-atazanavir, ritonavir-boosted-lopinavir, and efavirenz pharmacokinetics.Study designWe enrolled postpartum women using etonogestrel implants and receiving ritonavir-boosted-atazanavir, ritonavir-boosted-lopinavir, or efavirenz-based regimens between 2012 and 2015. Etonogestrel implants were inserted 2 to 12 weeks postpartum. We performed pharmacokinetic sampling pre-etonogestrel insertion and 6 to 7 weeks postinsertion. We measured antiretroviral concentrations pre and postetonogestrel insertion, and compared etonogestrel concentrations between antiretroviral regimens. We considered a minimum serum etonogestrel concentration of 90 pg/mL adequate for ovulation suppression.ResultsWe collected pharmacokinetic data for 74 postpartum women, 22 on ritonavir-boosted-atazanavir, 26 on ritonavir-boosted-lopinavir, and 26 on efavirenz. The median serum concentrations of etonogestrel when co-administered were highest with etonogestrel/ritonavir-boosted-atazanavir (604 pg/mL) and etonogestrel/ritonavir-boosted-lopinavir (428 pg/mL), and lowest with etonogestrel/efavirenz (125 pg/mL); p < 0.001. Minimum concentration (Cmin) of ritonavir-boosted-atazanavir and ritonavir-boosted-lopinavir were lower after etonogestrel implant insertion, but overall exposure, predose concentrations, clearance, and half-lives were unchanged. We found no significant change in efavirenz exposure after etonogestrel insertion.ConclusionsUnlike efavirenz, ritonavir-boosted-atazanavir and ritonavir-boosted-lopinavir were not associated with significant decreases in etonogestrel concentrations. Efavirenz was associated with a significant decrease in etonogestrel concentrations.ImplicationsThe findings demonstrate no interactions between etonogestrel and ritonavir-boosted-lopinavir or ritonavir-boosted-atazanavir, but confirm the decreased efficacy of etonogestrel with efavirenz-based antiretrovirals. This information should be used to counsel women with HIV who desire long-acting reversible contraceptives.

Published

2022

29. Poorer Muscle Quality and Quantity With ART Initiation Is Associated With Greater Inflammation and Immune Activation

Author

Kousari, Arianna, Moser, Carlee, Olefsky, Maxine, Brown, Todd T, Currier, Judith S, McComsey, Grace A, Scherzinger, Ann, Stein, James H, Lake, Jordan E, and Erlandson, Kristine M

Subjects

Clinical Research, Anti-HIV Agents, Antiretroviral Therapy, Highly Active, Biomarkers, C-Reactive Protein, HIV Infections, HIV Protease Inhibitors, Humans, Immune System, Inflammation, Interleukin-6, Lipopolysaccharide Receptors, Muscle, Skeletal, Treatment Outcome, inflammation, immune activation, muscle, HIV, antiretroviral therapy, ectopic fat, Clinical Sciences, Public Health and Health Services, Virology

Abstract

BackgroundWe have previously shown that the initiation of antiretroviral therapy (ART) is associated with a decrease in skeletal muscle density (greater fat accumulation), suggesting that gains in lean body mass seen in many ART studies may reflect gains in low quality, fatty muscle. Here, we explore whether skeletal muscle density and area are associated with markers of inflammation and immune activation.MethodsART-naïve people with HIV were randomized to raltegravir or ritonavir-boosted atazanavir or darunavir, each with tenofovir disoproxil fumarate/emtricitabine. Abdominal computed tomography scans from baseline and week 96 were reanalyzed for psoas density and area and correlations explored with inflammation [interleukin-6 (IL-6) and high-sensitivity C-reactive protein] and immune activation [soluble CD14 (sCD14), soluble CD163 (sCD163), and %CD38+HLADR+ on CD4+ or CD8+ T cells].ResultsTwo hundred twenty-two participants had available inflammation/immune activation markers and paired computed tomography scans. At baseline, lower psoas density (greater fat) correlated with higher IL-6 (r = -0.26, P < 0.001) and sCD163 (r -0.15, P = 0.03) and lower lean psoas area correlated with higher IL-6, high-sensitivity C-reactive protein, sCD14, sCD163, and %CD38+HLADR+ on CD4+ T cells (r = -0.30-0.13; all P ≤ 0.05). From baseline to week 96, greater percent decrease in total psoas density (more fat) correlated with greater increase in IL-6 (r = -0.14; P = 0.04); greater % decrease in lean psoas area correlated greater increases in IL-6, sCD14, sCD163, and %CD38+HLADR+ on CD8+ T cells (r = -0.15 to -0.18; all P < 0.04).ConclusionsGreater fat infiltration within the psoas muscle (lower density) and greater loss in lean psoas muscle area were associated with higher inflammation and immune activation, which may portend important effects on muscle function and cardiometabolic risk.

Published

2021

30. SLPI for Prostate Cancer

Author

Istituto per lo Studio, la Prevenzione e la Rete Oncologica, Azienda Ospedaliero-Universitaria Careggi, and Simone Morselli, PhD Student

Published

2022

31. HIV protease inhibitor saquinavir inhibits toll-like receptor 4 activation by targeting receptor dimerization.

Author

Kai Yao, Zheng Wang, Cheng Peng, Yong Wang, Bichen Xue, Yulin Tang, Zhichao Wang, and Hongbo Xu

Subjects

*HIV protease inhibitors, *TOLL-like receptors, *TOLL-like receptor agonists, *DIMERIZATION, *BINDING sites

Abstract

Objective: Toll-like receptor 4 (TLR4) is crucial in induction of innate immune response through recognition of invading pathogens or endogenous alarming molecules. Ligand-triggered dimerization of TLR4 is essential for the activation of NF-κB and IRF3 through MyD88- or TRIF-dependent pathways. Saquinavir (SQV), an FDA-approved HIV protease inhibitor, has been shown to attenuate the activation of NF-κB induced by HMGB1 by blocking TLR4-MyD88 association in proteasome independent pathway. This study aims to define whether SQV is an HMGB1-specific and MyD88-dependent TLR4 signaling inhibitor and which precise signaling element of TLR4 is targeted by SQV. Materials and Methods: PMA differentiated human THP-1 macrophages or reconstituted HEK293 cells were pretreated with SQV before stimulated by different TLR agonists. TNF-a level was evaluated through ELISA assay. NF-κB activation was analyzed using NF-κB SEAP reporting system. The levels of MyD88/TRIF pathways-related factors were examined by immunoblot. TLR4 endocytosis was assessed by immunocytochemistry. TLR4 dimerization was determined using immunoprecipitation between different tagged TLR4 and an in silico molecular docking experiment was performed to explore the possible binding site of SQV on its target. Results: Our data showed that SQV suppresses both MyD88- and TRIF-dependent pathways in response to lipopolysaccharide (LPS), a critical sepsis inducer and TLR4 agonist, leading to downregulation of NF-κB and IRF3. SQV did not suppress MyD88-dependent pathway triggered by TLR1/2 agonist Pam3csk4. In the only TRIF-dependent pathway, SQV did not alleviate IRF3 phosphorylation induced by TLR3 agonist Poly(I:C). Furthermore, dimerization of TLR4 following LPS or HMGB1 stimulation was decreased by SQV. Conclusion: We concluded that TLR4 receptor complex is one of the mammalian targets of SQV, and TLR4-mediated immune responses and consequent risk for uncontrolled inflammation could be modulated by FDA-approved drug SQV. [ABSTRACT FROM AUTHOR]

Published

2023

32. Disparate viral pandemics from COVID19 to monkeypox and beyond: a simple, effective and universal therapeutic approach hiding in plain sight.

Author

Johnson, Howard M. and Ahmed, Chulbul M.

Subjects

COVID-19, MONKEYPOX, PANDEMICS, MOLECULAR biology, SUPPRESSORS of cytokine signaling, HIV protease inhibitors

Abstract

The field of antiviral therapeutics is fixated on COVID19 and rightly so as the fatalities at the height of the pandemic in the United States were almost 1,000,000 in a twelve month period spanning parts of 2020/2021. A coronavirus called SARS-CoV2 is the causative virus. Development of a vaccine through molecular biology approaches with mRNA as the inducer of virus spike protein has played a major role in driving down mortality and morbidity. Antivirals have been of marginal value in established infections at the level of hospitalization. Thus, the current focus is on early symptomatic infection of about the first five days. The Pfizer drug paxlovid which is composed of nirmatrelvir, a peptidomimetic protease inhibitor of SARS-CoV2 Mpro enzyme, and ritonavir to retard degradation of nirmatrelvir, is the current FDA recommended treatment of early COVID19. There is no evidence of broad antiviral activity of paxlovid against other diverse viruses such as the influenza virus, poxviruses, as well as a host of respiratory viruses. Although type I interferons (IFNs) are effective against SARS-CoV2 in cell cultures and in early COVID19 infections, they have not been broadly recommended as therapeutics for COVID19. We have developed stable peptidomimetics of both types I and II IFNs based on our noncanonical model of IFN signaling involving the C-terminus of the IFNs. We have also identified two members of intracellular checkpoint inhibitors called suppressors of cytokine signaling (SOCS), SOCS1 and SOCS3 (SOCS1/3), and shown that they are virus induced intrinsic virulence proteins with activity against IFN signaling enzymes JAK2 and TYK2. We developed a peptidomimetic antagonist, based on JAK2 activation loop, against SOCS1/3 and showed that it synergizes with the IFN mimetics for potent broad spectrum antiviral activity without the toxicity of intact IFN molecules. IFN mimetics and the SOCS1/3 antagonist should have an advantage over currently used antivirals in terms of safety and potency against a broad spectrum of viruses. [ABSTRACT FROM AUTHOR]

Published

2023

33. Identification and quantitative analysis of bioactive components from Potentilla kleiniana Wight et Arn with anti HIV-1 proteases activity.

Author

Zhou, Yong Qiang, Li, Su Mei, Wei, Xin, Yang, Xin, Xiao, Jun Wei, Pan, Bo Wen, Xie, Shou Xia, Zhou, Ying, Yang, Jian, and Wei, Ying

Subjects

BIOACTIVE compounds, HIV, HIGH performance liquid chromatography, PROTEOLYTIC enzymes, HIV protease inhibitors, TRADITIONAL medicine

Abstract

Potentilla kleiniana Wight et Arn（PK, 'Wu Pi Feng' in Chinese） was recorded as Miao ethnic medicine for treatment of fever, cough, ulcer, and erysipelas for thousands years. This study aimed to evaluate the antiviral activity of four PK extracts and seven compounds by using HIV-1 protease (HIV-1 PR). In addition, Ultra-High Performance Liquid Chromatography and High Resolution Mass Spectrometry (UPLC-HRMS) was employed to identify the bioactive components. The toxicity assessment of the extracts was done before antiviral screening using a highly specific human aspartyl protease, renin protease by fluorimetric method. As a result, seven compounds and four extracts of PK inhibited HIV-1 PR with IC50 range from 0.009 to 0.36 mg/mL, and did not appreciably inhibit the general human protease renin. This study first demonstrated that four PK extracts, ellagic acid and ursolic acid potent inhibit HIV-1 protease, could be used as an efficacious drug candidate to treat SARS-CoV-2 infection. [ABSTRACT FROM AUTHOR]

Published

2023

34. SARS-CoV-2 main protease inhibitors from the stem barks of Discoglypremna caloneura (Pax) Prain (Euphorbiaceae) and Pterocarpus erinaceus Poir (Fabaceae) and their molecular docking investigation.

Author

Djouonzo, Paul Toukam, Mukim, Md Sofequl Islam, Kemda, Pamela Nangmo, Kowa, Theodora Kopa, Tchinda, Alembert Tiabou, Agbor Agbor, Gabriel, Pan, Cheol-Ho, and Song, Dae-Geun

Subjects

MOLECULAR docking, PROTEASE inhibitors, SARS-CoV-2, LEGUMES, EUPHORBIACEAE, HIV protease inhibitors

Abstract

The main viral protease (Mpro) of SARS-CoV-2 provides an excellent target for antivirals, due to its essential and conserved function in the viral replication cycle. We reported in this study, the SARS-CoV-2 main protease inhibitory effect of twelve compounds isolated from D. caloneura and P. erinaceus together with four derivatives. Among the effectively tested samples, two derivatized compounds displayed significant improvement on the activity from the starting material, friedelin (1) through the acetoreduced (2) to the acetoxy product (3) with respective IC50 values of 42.89, 29.69 and 19.39 µg/mL. The latter displayed the highest activity although lower as compared to that of baicalein, the positive control with IC50 0.41 µg/mL. The molecular docking study showed that an increase in the number of hydrogen bonds between compounds and active site of Mpro resulted in increased inhibition. [ABSTRACT FROM AUTHOR]

Published

2023

35. RAndomized Clinical Trial Of NAfamostat Mesylate, A Potent Transmembrane Protease Serine 2 (TMPRSS2) Inhibitor, in Patients with COVID-19 Pneumonia.

Author

Seccia, Teresa Maria, Shagjaa, Tungalagtamir, Morpurgo, Margherita, Caroccia, Brasilina, Sanga, Viola, Faoro, Sonia, Venturini, Francesca, Iadicicco, Girolama, Lococo, Sara, Mazzitelli, Maria, Farnia, Filippo, Fioretto, Paola, Kobayashi, Yusuke, Gregori, Dario, and Rossi, Gian Paolo

Subjects

*COVID-19, *CLINICAL trials, *DISSEMINATED intravascular coagulation, *SERINE, *COVID-19 treatment, *EMERGENCY contraceptives, *HIV protease inhibitors

Abstract

Even though SARS-CoV-2 was declared by WHO as constituting no longer a public health emergency, the development of effective treatments against SARS-CoV-2 infection remains a critical issue to prevent complications, particularly in fragile patients. The protease inhibitor nafamostat, currently used in Japan and Korea for pancreatitis, owing to its anticoagulant properties for disseminated intravascular coagulation (DIC), is appealing for the treatment of COVID-19 infection, because it potently inhibits the transmembrane protease serine 2 (TMPRSS2) that, after virus binding to ACE-2, allows virus entry into the cells and replication. Moreover, it could prevent the DIC and pulmonary embolism frequently associated with COVID-19 infection. The goal of the RAndomized Clinical Trial Of NAfamostat (RACONA) study, designed as a prospective randomized, double-blind placebo-controlled clinical trial, was to investigate the efficacy and safety of nafamostat mesylate (0.10 mg/kg/h iv for 7 days), on top of the optimal treatment, in COVID-19 hospitalized patients. We could screen 131 patients, but due to the predefined strict inclusion and exclusion criteria, only 15 could be randomized to group 1 (n = 7) or group 2 (n = 8). The results of an ad interim safety analysis showed similar overall trends for variables evaluating renal function, coagulation, and inflammation. No adverse events, including hyperkalemia, were found to be associated with nafamostat. Thus, the RACONA study showed a good safety profile of nafamostat, suggesting that it could be usefully used in COVID-19 hospitalized patients. [ABSTRACT FROM AUTHOR]

Published

2023

36. An Updated Assessment Of Ritonavir: A Protease Inhibitor.

Author

DURAISAMY, NIVEDHA, GOPAL, NAVEENA, MAHENDIRAN, ANBARASU, RAJAMANI, RAJESWARI, SUNDRAMOORTHY, POONGOTHAI, MUTHUVEL, MUTHURAJ, NATARAJAN, VIVEKANANDHAN, SUBRAMANIAN, MOHANRAJ, and ARTHANARI, SARAVANAKUMAR

Subjects

*RITONAVIR, *HIV protease inhibitors, *PROTEASE inhibitors, *HEPATITIS C, *AIDS

Abstract

Ritonavir, a protease inhibitor, is used to treat HIV/AIDS. Rarely does it function as a stand-alone antiviral medication, instead enhancing the antiviral effects of other protease inhibitors. Ritonavir was first created to block the HIV protease, however, research suggests that it also blocks cytochrome P450-3A4. Due to its manner of action, ritonavir is currently being studied for use in treating several types of cancer. It is additionally used in concert with other drugs to treat the Hepatitis C infection. The indications, dose, administration, adverse event profile, modes of action, toxicity, and contraindications of ritonavir are covered in this review. These observations can lead to new therapeutic indications of protease inhibitors to treat several cancers however, substantial extensive research is to be needed before clinical approval. [ABSTRACT FROM AUTHOR]

Published

2023

37. Study to Evaluate Efficacy and Safety of Darunavir/Cobicistat/Emtricitabine/Tenofovir Alafenamide (D/C/F/TAF) Regimen Versus Boosted Protease Inhibitor (bPI) Along With Emtricitabine/Tenofovir Disoproxil Fumarate (FTC/TDF) Regimen in Virologically-Suppressed, HIV-1 Infected Participants

Published

2021

38. A MERS-CoV antibody neutralizes a pre-emerging group 2c bat coronavirus.

Author

Tse, Longping V., Hou, Yixuan J., McFadden, Elizabeth, Lee, Rhianna E., Scobey, Trevor D., Leist, Sarah R., Martinez, David R., Meganck, Rita M., Schäfer, Alexandra, Yount, Boyd L., Mascenik, Teresa, Powers, John M., Randell, Scott H., Zhang, Yi, Wang, Lingshu, Mascola, John, McLellan, Jason S., and Baric, Ralph S.

Subjects

MIDDLE East respiratory syndrome, CORONAVIRUSES, MERS coronavirus, COVID-19, RECOMBINANT viruses, HIV protease inhibitors

Abstract

The repeated emergence of zoonotic human betacoronaviruses (β-CoVs) dictates the need for broad therapeutics and conserved epitope targets for countermeasure design. Middle East respiratory syndrome (MERS)–related coronaviruses (CoVs) remain a pressing concern for global health preparedness. Using metagenomic sequence data and CoV reverse genetics, we recovered a full-length wild-type MERS-like BtCoV/li/GD/2014-422 (BtCoV-422) recombinant virus, as well as two reporter viruses, and evaluated their human emergence potential and susceptibility to currently available countermeasures. Similar to MERS-CoV, BtCoV-422 efficiently used human and other mammalian dipeptidyl peptidase protein 4 (DPP4) proteins as entry receptors and an alternative DPP4-independent infection route in the presence of exogenous proteases. BtCoV-422 also replicated efficiently in primary human airway, lung endothelial, and fibroblast cells, although less efficiently than MERS-CoV. However, BtCoV-422 shows minor signs of infection in 288/330 human DPP4 transgenic mice. Several broad CoV antivirals, including nucleoside analogs and 3C-like/Mpro protease inhibitors, demonstrated potent inhibition against BtCoV-422 in vitro. Serum from mice that received a MERS-CoV mRNA vaccine showed reduced neutralizing activity against BtCoV-422. Although most MERS-CoV–neutralizing monoclonal antibodies (mAbs) had limited activity, one anti-MERS receptor binding domain mAb, JC57-11, neutralized BtCoV-422 potently. A cryo–electron microscopy structure of JC57-11 in complex with BtCoV-422 spike protein revealed the mechanism of cross-neutralization involving occlusion of the DPP4 binding site, highlighting its potential as a broadly neutralizing mAb for group 2c CoVs that use DPP4 as a receptor. These studies provide critical insights into MERS-like CoVs and provide candidates for countermeasure development. Editor's summary: Monoclonal antibodies and antivirals are essential tools to treat SARS-CoV-2 infection, and such approaches could be applied to other coronaviruses. Here, Tse et al. investigated whether antibodies that neutralize MERS-CoV and antivirals that inhibit SARS-CoV-2 could be used against a MERS-like bat coronavirus, BtCoV-422. The authors found that a MERS-CoV neutralizing antibody, JC57-11, efficiently neutralized BtCoV-422. BtCoV-422 replication was also potently inhibited by antivirals such as remdesivir. Together, these data suggest that the toolkit developed to treat SARS-CoV-2 could be used for other coronaviruses should they emerge in human populations. —Courtney Malo [ABSTRACT FROM AUTHOR]

Published

2023

39. Drug Reprofiling to Identify Potential HIV-1 Protease Inhibitors.

Author

Okafor, Sunday N., Meyer, Abigail, Gadsden, Jay, Ahmed, Fadi, Guzmán, Lilian, Ahmed, Hashim, Romero, José A. Fernández, and Angsantikul, Pavimol

Subjects

*PROTEASE inhibitors, *DRUG repositioning, *HIV protease inhibitors, *HIV, *DRUG discovery, *ENDOMETRIOSIS, *UTERINE fibroids, *INVESTIGATIONAL drugs

Abstract

The use of protease inhibitors in human immunodeficiency virus type 1 (HIV-1) treatment is limited by adverse effects, including metabolic complications. To address these challenges, efforts are underway in the pursuit of more potent and less toxic HIV-1 protease inhibitors. Repurposing existing drugs offers a promising avenue to expedite the drug discovery process, saving both time and costs compared to conventional de novo drug development. This study screened FDA-approved and investigational drugs in the DrugBank database for their potential as HIV-1 protease inhibitors. Molecular docking studies and cell-based assays, including anti-HIV-1 in vitro assays and XTT cell viability tests, were conducted to evaluate their efficacy. The study findings revealed that CBR003PS, an antibiotic currently in clinical use, and CBR013PS, an investigational drug for treating endometriosis and uterine fibroids, exhibited significant binding affinity to the HIV-1 protease with high stability. Their EC50 values, measured at 100% cell viability, were 9.4 nM and 36.6 nM, respectively. Furthermore, cell-based assays demonstrated that these two compounds showed promising results, with therapeutic indexes higher than 32. In summary, based on their favorable therapeutic indexes, CBR003PS and CBR013PS show potential for repurposing as HIV-1 protease inhibitors. [ABSTRACT FROM AUTHOR]

Published

2023

40. Anti-HIV crotocascarin ω from Kenyan Croton dichogamus.

Author

Terefe, Ermias Mergia, Okalebo, Faith A., Derese, Solomon, Muriuki, Joseph, Mas-Claret, Eduard, and Langat, Moses K

Subjects

HIV, ACETATES, TWIGS, BENZOATES, HIV protease inhibitors

Abstract

An anti-HIV methanol-soluble fraction of a 1:1 CH2Cl2:CH3OH extract of twigs of a Kenyan Croton dichogamus yielded seven compounds, the new crotocascarin ω (1), the known β-oplopanone (2), dihydroconiferyl acetate (3), 3'(4"-hydroxyphenyl)-propyl benzoate (4), lupeol, sitosterol and stigmasterol. Crotocascarin ω (90%) inhibited HIV-1 replication with an IC50 value of 5.3 nM, and the compound was cytotoxic towards MT-4 cells presenting an IC50 value of 84 µM. In silico modelling showed that the anti-HIV activity for compound 1 could be through the HIV-1 protease inhibition. [ABSTRACT FROM AUTHOR]

Published

2023

41. Managing nirmatrelvir/ritonavir (Paxlovid) interactions in general practice.

Author

MIROWSKA-GUZEL, DAGMARA, NIEDZIELKO, MAGDALENA, and KUŁAKOWSKI, RAFAŁ

Subjects

*HIV infections, *ANTI-HIV agents, *COMBINATION drug therapy, *FAMILY medicine, *HIV protease inhibitors, *ANTIVIRAL agents, *MEDICATION therapy management, *RITONAVIR, *DRUG interactions, *PHARMACY information services

Abstract

Nirmatrelvir/ritonavir (Paxlovid) is indicated in patients who are at high risk of progressing to severe COVID-19. Many of these patients are concomitantly prescribed various medications for other indications. Ritonavir has no activity against SARS-CoV-2, but, administered with nirmatrelvir, acts as a pharmacokinetic booster, increasing nirmatrelvir’s efficacy. Ritonavir can simultaneously change other medicines’ plasma levels, affecting their safety and therapeutic effects. Ritonavir’s potential to cause clinically significant interactions is well documented, as it has a long history of being used as a pharmacokinetic enhancer with other antiviral agents. Pharmacokinetic drug-drug interactions (DDIs) are a well-known phenomenon, but data on the clinical impact of Paxlovid DDIs is still insufficient. Ritonavir in the treatment of COVID-19 is only administered for 5 days; therefore, uncertainty exists on how the coadministration of various medicines should be managed. Numerous Paxlovid DDIs can lead to serious adverse drug reactions; therefore, careful analysis of all concomitantly prescribed medicines is essential to ensure treatment safety. This article aims to summarise currently available information on Paxlovid DDIs that may be relevant for general practitioners. It explains the main mechanisms leading to pharmacokinetic interactions and possible options for DDIs management. The authors indicate sources of information that may be helpful to prescribers when weighing the benefits and risks of Paxlovid co-administration with other medicines. [ABSTRACT FROM AUTHOR]

Published

2023

42. Repurposing Anti-Dengue Compounds against Monkeypox Virus Targeting Core Cysteine Protease.

Author

Imran, Mohd, Abida, Alotaibi, Nawaf M., Thabet, Hamdy Khamees, Alruwaili, Jamal Alhameedi, Eltaib, Lina, Alshehri, Ahmed, Alsaiari, Ahad Amer, Kamal, Mehnaz, and Alshammari, Abdulmajeed Mohammed Abdullah

Subjects

MONKEYPOX, MACHINE learning, CYSTEINE proteinase inhibitors, MOLECULAR docking, DRUG design, CYSTEINE, HIV protease inhibitors

Abstract

The monkeypox virus (MPXV) is an enveloped, double-stranded DNA virus belonging to the genus Orthopox viruses. In recent years, the virus has spread to countries where it was previously unknown, turning it into a worldwide emergency for public health. This study employs a structural-based drug design approach to identify potential inhibitors for the core cysteine proteinase of MPXV. During the simulations, the study identified two potential inhibitors, compound CHEMBL32926 and compound CHEMBL4861364, demonstrating strong binding affinities and drug-like properties. Their docking scores with the target protein were −10.7 and −10.9 kcal/mol, respectively. This study used ensemble-based protein–ligand docking to account for the binding site conformation variability. By examining how the identified inhibitors interact with the protein, this research sheds light on the workings of the inhibitors' mechanisms of action. Molecular dynamic simulations of protein–ligand complexes showed fluctuations from the initial docked pose, but they confirmed their binding throughout the simulation. The MMGBSA binding free energy calculations for CHEMBL32926 showed a binding free energy range of (−9.25 to −9.65) kcal/mol, while CHEMBL4861364 exhibited a range of (−41.66 to −31.47) kcal/mol. Later, analogues were searched for these compounds with 70% similarity criteria, and their IC50 was predicted using pre-trained machine learning models. This resulted in identifying two similar compounds for each hit with comparable binding affinity for cysteine proteinase. This study's structure-based drug design approach provides a promising strategy for identifying new drugs for treating MPXV infections. [ABSTRACT FROM AUTHOR]

Published

2023

43. Weight gain among treatment‐naïve persons with HIV starting integrase inhibitors compared to non‐nucleoside reverse transcriptase inhibitors or protease inhibitors in a large observational cohort in the United States and Canada

Author

Bourgi, Kassem, Jenkins, Cathy A, Rebeiro, Peter F, Shepherd, Bryan E, Palella, Frank, Moore, Richard D, Althoff, Keri N, Gill, John, Rabkin, Charles S, Gange, Stephen J, Horberg, Michael A, Margolick, Joseph, Li, Jun, Wong, Cherise, Willig, Amanda, Lima, Viviane D, Crane, Heidi, Thorne, Jennifer, Silverberg, Michael, Kirk, Gregory, Mathews, William C, Sterling, Timothy R, Lake, Jordan, Koethe, John R, and Research and Design, for the North American AIDS Cohort Collaboration on

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Prevention, Infectious Diseases, HIV/AIDS, Clinical Research, Sexually Transmitted Infections, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Adult, CD4 Lymphocyte Count, Canada, Cohort Studies, Female, HIV Infections, HIV Integrase Inhibitors, HIV Protease Inhibitors, Heterocyclic Compounds, 3-Ring, Humans, Male, Middle Aged, Oxazines, Piperazines, Pyridones, Reverse Transcriptase Inhibitors, United States, Weight Gain, integrase inhibitors, weight gain, obesity, metabolic, HIV, North America, North American AIDS Cohort Collaboration on Research and Design, Public Health and Health Services, Other Medical and Health Sciences, Clinical sciences, Epidemiology, Public health

Abstract

IntroductionWeight gain following antiretroviral therapy (ART) initiation is common, potentially predisposing some persons with HIV (PWH) to cardio-metabolic disease. We assessed relationships between ART drug class and weight change among treatment-naïve PWH initiating ART in the North American AIDS Cohort Collaboration on Research and Design (NA-ACCORD).MethodsAdult, treatment-naïve PWH in NA-ACCORD initiating integrase strand transfer inhibitor (INSTI), protease inhibitor (PI) or non-nucleoside reverse-transcriptase inhibitor (NNRTI)-based ART on/after 1 January 2007 were followed through 31 December 2016. Multivariate linear mixed effects models estimated weight up to five years after ART initiation, adjusting for age, sex, race, cohort site, HIV acquisition mode, treatment year, and baseline weight, plasma HIV-1 RNA level and CD4+ cell count. Due to shorter follow-up for PWH receiving newer INSTI drugs, weights for specific INSTIs were estimated at two years. Secondary analyses using logistic regression and all covariates from primary analyses assessed factors associated with >10% weight gain at two and five years.ResultsAmong 22,972 participants, 87% were male, and 41% were white. 49% started NNRTI-, 31% started PI- and 20% started INSTI-based regimens (1624 raltegravir (RAL), 2085 elvitegravir (EVG) and 929 dolutegravir (DTG)). PWH starting INSTI-based regimens had mean estimated five-year weight change of +5.9kg, compared to +3.7kg for NNRTI and +5.5kg for PI. Among PWH starting INSTI drugs, mean estimated two-year weight change was +7.2kg for DTG, +5.8kg for RAL and +4.1kg for EVG. Women, persons with lower baseline CD4+ cell counts, and those initiating INSTI-based regimens had higher odds of >10% body weight increase at two years (adjusted odds ratio = 1.37, 95% confidence interval: 1.20 to 1.56 vs. NNRTI).ConclusionsPWH initiating INSTI-based regimens gained, on average, more weight compared to NNRTI-based regimens. This phenomenon may reflect heterogeneous effects of ART agents on body weight regulation that require further exploration.

Published

2020

44. Fosamprenavir with Ritonavir Pharmacokinetics during Pregnancy.

Author

Eke, Ahizechukwu C, Wang, Jiajia, Amin, Khadija, Shapiro, David E, Stek, Alice, Smith, Elizabeth, Chakhtoura, Nahida, Basar, Michael, George, Kathleen, Knapp, Katherine M, João, Esaú C, Rungruengthanakit, Kittipong, Capparelli, Edmund, Burchett, Sandra, Mirochnick, Mark, Best, Brookie M, and P1026s Protocol Team

Subjects

P1026s Protocol Team, Humans, Pregnancy Complications, Infectious, HIV Infections, Sulfonamides, Carbamates, Furans, Ritonavir, RNA, Viral, HIV Protease Inhibitors, Viral Load, Area Under Curve, Maternal Age, Pregnancy, Pregnancy Trimesters, Adult, Female, AIDS, amprenavir, fosamprenavir, human immunodeficiency virus, pharmacokinetics, postpartum, pregnancy, ritonavir, Prevention, Genetics, 6.1 Pharmaceuticals, Microbiology, Medical Microbiology, Pharmacology and Pharmaceutical Sciences

Abstract

The purpose of this study was to evaluate the pharmacokinetics of ritonavir-boosted fosamprenavir during pregnancy and postpartum. Amprenavir (the active moiety of fosamprenavir) and ritonavir intensive pharmacokinetic evaluations were performed at steady state during the second and third trimesters of pregnancy and postpartum. Plasma concentrations of amprenavir and ritonavir were measured using high-performance liquid chromatography. The target amprenavir area under the concentration-versus-time curve (AUC) was higher than the 10th percentile (27.7 μg · h/ml) of the median area under the curve for ritonavir-boosted fosamprenavir in adults receiving twice-daily fosamprenavir-ritonavir at 700 mg/100 mg. Twenty-nine women were included in the analysis. The amprenavir AUC from time zero to 12 h (AUC0-12) was lower (geometric mean ratio [GMR], 0.60 [confidence interval {CI}, 0.49 to 0.72] [P

Published

2020

45. Association of Pharmacogenetic Markers With Atazanavir Exposure in HIV‐Infected Women

Author

Tamraz, Bani, Huang, Yong, French, Audrey L, Kassaye, Seble, Anastos, Kathryn, Nowicki, Marek J, Gange, Stephen, Gustafson, Deborah R, Bacchetti, Peter, Greenblatt, Ruth M, Hysi, Pirro G, Aouizerat, Bradley E, and Study, Women's Interagency HIV

Subjects

Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, ATP Binding Cassette Transporter, Subfamily B, Area Under Curve, Atazanavir Sulfate, Chromatography, High Pressure Liquid, Citrus sinensis, Cytochrome P-450 CYP3A Inhibitors, Diarrhea, Dose-Response Relationship, Drug, Female, Genotype, HIV Infections, HIV Protease Inhibitors, Hair, Heroin Dependence, Humans, Hydrogen-Ion Concentration, Longitudinal Studies, MicroRNAs, Polymorphism, Single Nucleotide, Racial Groups, Receptors, Cell Surface, Tandem Mass Spectrometry, Women's Interagency HIV Study, Pharmacology & Pharmacy, Pharmacology and pharmaceutical sciences

Abstract

SORCS2 rs73208473 was recently associated with decreased atazanavir (ATV) concentration in the hair of women with seropositive HIV. Herein, we report on a pharmacogenetic study of women with seropositive HIV demonstrating a similar association between rs73208473 and dose-adjusted plasma ATV concentration in African Americans.

Published

2020

46. Effects of Ledipasvir/Sofosbuvir on the Pharmacokinetics and Renal Safety of Tenofovir Alafenamide (TAF)

Published

2021

47. Proteases, protease inhibitors and radiation carcinogenesis.

Author

Kennedy, Ann R.

Subjects

*RADIATION carcinogenesis, *PROTEASE inhibitors, *PROTEOLYTIC enzymes, *ANTICARCINOGENIC agents, *INVESTIGATIONAL drugs, *HIV protease inhibitors

Abstract

Purpose: The purpose of the studies described in this mini review article was to identify nontoxic compounds that could prevent or suppress the radiation induced malignant transformation of cells and be useful as human cancer preventive agents. Conclusions: (1) Many different types of potential anticarcinogenic substances were evaluated initially for their abilities to prevent or suppress radiation induced malignant transformation in vitro, and certain anticarcinogenic protease inhibitors (APIs) were observed to be the most powerful anticarcinogenic agents at suppressing this surrogate endpoint biomarker of radiation carcinogenesis. (2) Within the category of APIs, those that inhibited the activity of chymotrypsin were effective at far lower molar concentrations than other APIs. The soybean-derived protease inhibitor known as the Bowman-Birk inhibitor (BBI) is a particularly powerful chymotrypsin inhibitor that is able to prevent radiation induced transformation in vitro (at concentrations down to nanomolar levels) as well as radiation induced carcinogenesis in vivo without toxicity. (3) There were many other unusual characteristics of APIs that led to the selection of one of these APIs, BBI, as the most appropriate compound for us to develop as a human cancer preventive agent. As one example, the APIs have an irreversible effect on carcinogenesis, while the effects are reversible for most anticarcinogenic agents when they are removed from carcinogenesis assay systems. (4) Numerous studies were performed in attempts to determine the potential mechanisms by which the APIs could prevent or suppress radiation induced carcinogenesis in in vitro and in vivo systems, and the results of these studies are described in this review article. The APIs and the proteases which interact with them appear to play important roles in radiation carcinogenesis. (5) Preparations for human trials using BBI began decades ago. The cost of preparing purified BBI was far too high to consider performing human trials with this agent, so BBI Concentrate (BBIC), a soybean extract enriched in BBI, was developed for the specific purpose of performing human trials with BBI. BBIC achieved Investigational New Drug (IND) Status with the Food and Drug Administration in April, 1992, and human BBIC trials began at that time. (6) Several human trials were performed using BBIC and they indicated many potentially beneficial health effects produced by BBIC administration to people in various forms (e.g. tablets). 7) It is hypothesized that BBI takes the place of a-1-antichymotrypsin, an important regulatory compound in the human body, and helps to maintain homeostasis. [ABSTRACT FROM AUTHOR]

Published

2023

48. Dipeptidyl peptidase-1 inhibition with brensocatib reduces the activity of all major neutrophil serine proteases in patients with bronchiectasis: results from the WILLOW trial.

Author

Cipolla, David, Zhang, Jimin, Korkmaz, Brice, Chalmers, James D., Basso, Jessica, Lasala, Daniel, Fernandez, Carlos, Teper, Ariel, Mange, Kevin C., Perkins, Walter R., and Sullivan, Eugene J.

Subjects

*LEUCOCYTES, *LEUCOCYTE elastase, *NEUTROPHILS, *BRONCHIECTASIS, *WILLOWS, *SERINE proteinases, *HIV protease inhibitors

Abstract

Background: Brensocatib is an oral, selective, reversible inhibitor of dipeptidyl peptidase-1 (DPP-1), responsible for activating neutrophil serine proteases (NSPs) including neutrophil elastase (NE), proteinase 3 (PR3), and cathepsin G (CatG). In chronic inflammatory lung diseases such as non-cystic fibrosis bronchiectasis (NCFBE), neutrophils accumulate in the airways resulting in excess active NSPs that cause damaging inflammation and lung destruction. Methods: The 24-week WILLOW trial (NCT03218917) was a randomized, double-blind, placebo-controlled, parallel-group trial in patients with NCFBE conducted at 116 sites across 14 countries. In this trial, treatment with brensocatib was associated with improvements in clinical outcomes including time to first exacerbation, reduction in exacerbation frequency and a reduction in NE activity in sputum. An exploratory analysis of NE activity in white blood cell (WBC) extracts and NE, PR3 and CatG activity in sputum was conducted to further characterize brensocatib's effect and identify potential correlated effects. Results: NE, PR3 and CatG activities were reduced in sputum and NE activity was reduced in WBC extracts in a dose-dependent manner after four weeks of brensocatib treatment, with a return to baseline four weeks after the end of treatment. Brensocatib produced the greatest reduction in the sputum activity of CatG, followed by NE and then PR3. Positive correlations among the sputum NSPs were observed both at baseline and in response to treatment, with the strongest correlation among the sputum NSPs for NE and CatG. Conclusions: These results suggest a broad anti-inflammatory effect of brensocatib underlying its clinical efficacy observed in NCFBE patients. Trial registration: The study was approved by the corresponding ethical review boards of all participating centers. The trial was approved by the Food and Drug Administration and registered at clinicaltrials.gov (NCT03218917) on July 17, 2017 and approved by the European Medicines Agency and registered at the European Union Clinical trials Register (EudraCT No. 2017-002533-32). An independent, external data and safety monitoring committee (comprising physicians with pulmonary expertise, a statistician experienced in the evaluation of clinical safety, and experts in periodontal disease and dermatology) reviewed all adverse events. [ABSTRACT FROM AUTHOR]

Published

2023

49. Clinical Perspective on Human Immunodeficiency Virus Care of Ukrainian War Refugees in Poland.

Author

Parczewski, Miłosz, Jabłonowska, Elżbieta, Wójcik-Cichy, Kamila, Zhyvytsia, Dmytro, Witak-Jędra, Magdalena, Leszczyszyn-Pynka, Magdalena, Aksak-Wąs, Bogusz, Siwak, Ewa, Cielniak, Iwona, Olczak, Anita, Szymczak, Aleksandra, Szetela, Bartosz, Bociąga-Jasik, Monika, Kalinowska-Nowak, Anna, Mularska, Elżbieta, Witor, Adam, Jakubowski, Paweł, Hlebowicz, Maria, Rozpłochowski, Błażej, and Łojewski, Władysław

Subjects

*EVALUATION of medical care, *DIAGNOSIS of HIV infections, *HEPATITIS C diagnosis, *AIDS diagnosis, *HIV infections, *ANTI-HIV agents, *VIRAL antigens, *HEPATITIS B, *DRUG efficacy, *HIV integrase inhibitors, *SEQUENCE analysis, *GENETIC mutation, *HEALTH services accessibility, *WAR, *REVERSE transcriptase inhibitors, *VIRAL load, *UKRAINIANS, *HIV protease inhibitors, *SYMPTOMS, *REFUGEES, *MIXED infections, *CD4 lymphocyte count, *MULTIDRUG resistance, *DESCRIPTIVE statistics, *RESEARCH funding, *DRUG resistance in microorganisms, *VIRAL antibodies, *AIDS, *HIV

Abstract

Background The Russian invasion of Ukraine forced migration for safety, protection, and assistance. Poland is the primary sheltering country for Ukrainian refugees, providing support including medical care, which resulted in the rapid ∼15% increase in the number of followed-up people with human immunodeficiency virus (HIV) (PWH) in the country. Here, we present the national experience on HIV care provided for refugees from Ukraine. Methods Clinical, antiretroviral, immunological, and virologic data from 955 Ukrainian PWH entering care in Poland since February 2022 were analyzed. The dataset included both antiretroviral-treated (n = 851) and newly diagnosed (n = 104) patients. In 76 cases, protease/reverse transcriptase/integrase sequencing was performed to identify drug resistance and subtype. Results Most (70.05%) of the patients were female, with a predominance of heterosexual (70.3%) transmissions. Anti–hepatitis C antibody and hepatitis B antigen were present in 28.7% and 2.9% of the patients, respectively. A history of tuberculosis was reported in 10.1% of cases. Among previously treated patients, the viral suppression rate was 89.6%; 77.3% of newly HIV diagnosed cases were diagnosed late (with lymphocyte CD4 count <350 cells/μL or AIDS). The A6 variant was observed in 89.0% of sequences. Transmitted mutations in the reverse transcriptase were found in 15.4% treatment-naive cases. Two patients with treatment failure exhibited multiclass drug resistance. Conclusions Migration from Ukraine influences the characteristics of HIV epidemics in Europe, with an increase in the proportion of women and hepatitis C coinfected patients. Antiretroviral treatment efficacy among previously treated refugees was high, with new HIV cases frequently diagnosed late. The A6 subtype was the most common variant. [ABSTRACT FROM AUTHOR]

Published

2023

50. AI-Aided Search for New HIV-1 Protease Ligands.

Author

Arrigoni, Roberto, Santacroce, Luigi, Ballini, Andrea, and Palese, Luigi Leonardo

Subjects

*ARTIFICIAL intelligence, *HIV, *LIGANDS (Biochemistry), *DRUG accessibility, *LIFE cycles (Biology), *PROTEOLYTIC enzymes

Abstract

The availability of drugs capable of blocking the replication of microorganisms has been one of the greatest triumphs in the history of medicine, but the emergence of an ever-increasing number of resistant strains poses a serious problem for the treatment of infectious diseases. The search for new potential ligands for proteins involved in the life cycle of pathogens is, therefore, an extremely important research field today. In this work, we have considered the HIV-1 protease, one of the main targets for AIDS therapy. Several drugs are used today in clinical practice whose mechanism of action is based on the inhibition of this enzyme, but after years of use, even these molecules are beginning to be interested by resistance phenomena. We used a simple artificial intelligence system for the initial screening of a data set of potential ligands. These results were validated by docking and molecular dynamics, leading to the identification of a potential new ligand of the enzyme which does not belong to any known class of HIV-1 protease inhibitors. The computational protocol used in this work is simple and does not require large computational power. Furthermore, the availability of a large number of structural information on viral proteins and the presence of numerous experimental data on their ligands, with which it is possible to compare the results obtained with computational methods, make this research field the ideal terrain for the application of these new computational techniques. [ABSTRACT FROM AUTHOR]

Published

2023