Your search keyword '"indinavir"' showing total 37 results

1. Biocompatible Palladium Telluride Quantum Dot-Amplified Biosensor for HIV Drug.

Author

Feleni, Usisipho, Sidwaba, Unathi, Ntshongontshi, Nomaphelo, Wilson, Lindsay, and Iwuoha, Emmanuel

Abstract

Indinavir (IDV) is a potent and well-tolerated protease inhibitor antiretroviral (ARV) drug used as a component of the highly active antiretroviral therapy (HAART) of human immunodeficiency virus (HIV). It undergoes hepatic first-pass metabolism that is catalysed by microsomal cytochrome P450-3A4 enzyme (CYP3A4), which results in pharmacokinetics that may be favourable or adverse. Therapeutic drug monitoring (TDM) of IDV during HIV treatment is therefore critical, in order to prevent the adverse effects of its first-pass metabolism and optimise an individual's dosage regime. Biosensors are now the preferred diagnostic tools for TDM assessment at point-of-care, due to their high sensitivity and real-time response. An electrochemical biosensor for IDV was prepared by depositing a thin film of CYP3A4 (a thiolate enzyme) and thioglycolic acid-capped palladium telluride quantum dot (TGA-PdTeQD) on a cysteamine-functionalised gold disk electrode (Cyst|Au) using a combination of thiol and carbodiimide covalent bonding chemistries. The electrochemical signatures of the biosensor (CYP3A4|TGA-PdTeQD|Cyst|Au) were determined by cyclic voltammetry (CV) that was performed at a scan rate of 500 mV s−1, and the sensor responses at the characteristic reduction peak potential value of − 0.26 V were recorded. The sensitivity, linear range (LR) and limit of detection (LOD) values of the indinavir biosensor were 4.45 ± 0.11 μA nM−1 IDV, 0.5–1.0 nM IDV (i.e. 3.6 × 10−4–7.1 × 10−4 mg L−1 IDV) and 4.5 × 10−4 mg L−1 IDV, respectively. The values of the two analytical parameters (LR and LOD) of the biosensor were by up to four orders of magnitude lower than the maximum plasma concentration (Cmax) values of indinavir (0.13–8.6 mg L−1 IDV). The IDV biosensor was successfully used to detect IDV in human serum samples containing dissolved indinavir tablet. This, therefore, indicates the indinavir biosensor's suitability for TDM applications, using samples obtained within 1–2 h of drug intake at point-of-care, for which very low levels of the drug are expected. [ABSTRACT FROM AUTHOR]

Published

2020

2. Drug-Induced Kidney Stones and Crystalline Nephropathy: Pathophysiology, Prevention and Treatment.

Author

Daudon, Michel, Frochot, Vincent, Bazin, Dominique, and Jungers, Paul

Subjects

*KIDNEY disease prevention, *KIDNEY disease treatments, *KIDNEY physiology, *URINARY calculi, *CALCIUM, *CRYSTALLIZATION, *DIETARY supplements, *CLINICAL drug trials, *KIDNEY stones, *KIDNEY diseases, *URINALYSIS, *VITAMIN D, *CALCIUM compounds, *CONTROL groups, *INDINAVIR, *DIAGNOSIS

Abstract

Drug-induced calculi represent 1–2% of all renal calculi. The drugs reported to produce calculi may be divided into two groups. The first one includes poorly soluble drugs with high urine excretion that favour crystallisation in the urine. Among them, drugs used for the treatment of patients with human immunodeficiency, namely atazanavir and other protease inhibitors, and sulphadiazine used for the treatment of cerebral toxoplasmosis, are the most frequent causes. Besides these drugs, about 20 other molecules may induce nephrolithiasis, such as ceftriaxone or ephedrine-containing preparations in subjects receiving high doses or long-term treatment. Calculi analysis by physical methods including infrared spectroscopy or X-ray diffraction is needed to demonstrate the presence of the drug or its metabolites within the calculi. Some drugs may also provoke heavy intra-tubular crystal precipitation causing acute renal failure. Here, the identification of crystalluria or crystals within the kidney tissue in the case of renal biopsy is of major diagnostic value. The second group includes drugs that provoke the formation of urinary calculi as a consequence of their metabolic effects on urinary pH and/or the excretion of calcium, phosphate, oxalate, citrate, uric acid or other purines. Among such metabolically induced calculi are those formed in patients taking uncontrolled calcium/vitamin D supplements, or being treated with carbonic anhydrase inhibitors such as acetazolamide or topiramate. Here, diagnosis relies on a careful clinical inquiry to differentiate between common calculi and metabolically induced calculi, of which the incidence is probably underestimated. Specific patient-dependent risk factors also exist in relation to urine pH, volume of diuresis and other factors, thus providing a basis for preventive or curative measures against stone formation. [ABSTRACT FROM AUTHOR]

Published

2018

3. Late treatment failures in cerebrospinal fluid in patients on long-term maintenance ART with ritonavir-boosted protease PI monotherapy.

Author

Kahlert, C., Bregenzer, A., Gutmann, C., Otterbech, S., Hoffmann, M., Schmid, P., and Vernazza, P.

Subjects

ANTIRETROVIRAL agents, RITONAVIR, HIV protease inhibitors, HIV infections, TREATMENT effectiveness, ATAZANAVIR, LOPINAVIR-ritonavir, DESCRIPTIVE statistics, INDINAVIR, THERAPEUTICS

Abstract

Background: Antiretroviral treatment (ART) with ritonavir-boosted protease inhibitor monotherapy (rb-PMT) remains a potentially attractive strategy for treatment simplification in HIV-infected individuals. However, long-term follow-up in particular with respect to HIV-RNA suppression in cerebrospinal fluids (CSF) is still lacking. Methods: Patients who participated in one of the three monotherapy trials [indinavir/r, ATARITMO (atazanavir/r), MOST (lopinavir/r)] at our HIV clinic and remained successfully suppressed during the entire trial (plasma < 50 copies/mL, CSF < 100 copies/mL) were offered to continue their monotherapy under close monitoring. While on rb-PMT, patients were asked to provide CSF samples in yearly or 2-yearly intervals. All patients fully suppressed in plasma and CSF for at least 12 months were included in the analysis. Patients demonstrating any failure in plasma or CSF resumed triple combined ART. Results: A total of 27 patients (5 women and 22 men) fulfilled the entry criteria. The median follow-up time was 4.8 (1.1-10.9) years with an overall experience of 139 patient-years on monotherapy. Eleven of 27 (41 %) patients (2 women and 9 men) developed virologic failure (1 in plasma only, 4 in CSF only, 4 both in plasma and CSF and 2 in plasma with CSF not available). Plasma failure occurred in 7 patients after a median follow-up of 25 (13-32) months, and CSF failure in 8 patients after a median follow-up of 30 (14-64) months. Seven patients are still on rb-PMT with atazanavir/r. Failure was associated with shorter duration of fully suppressed plasma viral load prior to starting ( p < 0.022). Conclusion: For selected patients, rb-PMT might be a valid long-term treatment strategy. Nevertheless, even after 12 months of full HIV-RNA suppression, more than 1/3 of patients may still develop failure in either plasma or CSF. Given the observation of isolated CSF failure, treatment monitoring with regular lumbar puncture should be recommended in rb-PMT. Only monotherapy with atazanavir/r was successful beyond 39 months. Monotherapy failure was significantly associated with a shorter duration of complete HIV-RNA suppression in plasma prior to rb-PMT start. Further investigation is needed to better identify predictors for patients that will qualify for successful long-term rb-PMT. [ABSTRACT FROM AUTHOR]

Published

2016

4. The HIV protease inhibitor indinavir down-regulates the expression of the pro-angiogenic MT1-MMP by human endothelial cells.

Author

Barillari, Giovanni, Iovane, André, Bacigalupo, Ilaria, Labbaye, Catherine, Chiozzini, Chiara, Sernicola, Leonardo, Quaranta, Maria, Falchi, Mario, Sgadari, Cecilia, and Ensoli, Barbara

Subjects

HIV, PROTEASE inhibitors, GENE expression, VASCULAR endothelial growth factors, ENDOTHELIAL cells, MATRIX metalloproteinases, DISEASE incidence, DISEASE progression

Abstract

In addition to contrast human immunodeficiency virus (HIV) replication, the HIV protease inhibitors (HIV-PI) have reduced tumour incidence or clinical progression in infected patients. In this regard, we have previously shown that, independently of its anti-viral activity, the HIV-PI indinavir (IDV) directly blocks matrix metalloproteinase (MMP)-2 proteolytic activation, thus efficiently inhibiting tumour angiogenesis in vitro, in animal models, and in humans. Herein we investigated the molecular mechanism for IDV anti-angiogenic effect. We found that treatment of human primary endothelial cells with therapeutic IDV concentrations decreases the expression of membrane type (MT)1-MMP, which is the major activator of MMP-2. This occurs for both the constitutive expression of MT1-MMP and that up-regulated by angiogenic factors. In either cases, reduction of MT1-MMP levels by IDV is preceded by the inhibition of the binding of the specificity protein (Sp)1 transcription factor to the promoter region of the MT1-MMP gene in endothelial cell nuclei. As MT1-MMP is key for tumour angiogenesis, these results support the use of IDV or its derivatives in anti-cancer therapy. This is recommended by the low toxicity of the drug, and the large body of data on its pharmacokinetic. [ABSTRACT FROM AUTHOR]

Published

2014

5. Differentiating HIV-associated Nephropathy from Antiretroviral Drug-Induced Nephropathy: A Clinical Challenge.

Author

Kumar, Neelja and Perazella, Mark

Abstract

With the introduction of potent combination antiretroviral therapy (cART) into clinical practice, HIV-infected patients have garnered much benefit. However, kidney disease continues to be a potential complication in this group. Whereas HIV-associated nephropathy (HIVAN) was the major renal complication prior to cART, co-morbid diseases and adverse renal effects of various drugs, in particular cART, now complicate the landscape. Clinicians now must differentiate HIVAN from cART nephrotoxicity. While sometimes this is easy and relatively straightforward, often the clinician faces a difficult challenge distinguishing these two etiologies of kidney disease. This review will discuss HIVAN and cART-related kidney disease and review the clinical and laboratory data that may be useful in differentiating these processes. Often, however, kidney biopsy may be required to differentiate HIVAN from cART nephrotoxicity as well as other kidney lesions associated with concurrent co-morbidities, both infectious and non-infectious. [ABSTRACT FROM AUTHOR]

Published

2014

6. In silico screening of indinavir-based compounds targeting proteolytic activity in HIV PR: binding pocket fit approach.

Author

Selvaraj, Chandrabose, Singh, Sanjeev, Tripathi, Sunil, Reddy, Karnati, and Rama, Murugappan

Abstract

The intense research on small molecule inhibitors of Human immunodeficiency virus (HIV)-protease (PR) has produced a diverse class of chemical scaffolds which includes clinically available HIV PR inhibitors (PRI). Till now, these inhibitors are insignificant for targeting proteolytic activity and few drug molecules on alterations can enhance the inhibition of PR enzyme. Here, we developed a method for screening of new hits from Cambridge structural database, based on binding mode of indinavir interaction participating atoms. Knowledge-based ligand screening technique approximately informs that new hits are also having same binding mode-like indinavir interaction patterns. Considering the importance of ligand fitting in binding pocket, we developed induced-fit models for each compound and we obtained accurate energy values in terms of binding and interaction energy. We found that newly search molecules are interacting better than known drug-indinavir and these new compounds are comparatively having better drug-like property. Finally, we demonstrated that pocket specific docking, energy utilization, interactions, and ADME for screened compounds are showing new hit compounds of indinavir are better HIV PRI and these new compounds can also show better activity in in vivo and in vitro conditions. [ABSTRACT FROM AUTHOR]

Published

2012

7. HIV Therapies and the Kidney: Some Good, Some Not So Good?

Author

Ryom, Lene, Mocroft, Amanda, and Lundgren, Jens

Abstract

Several observational studies have identified tenofovir as an independent risk factor for kidney impairment. Conversely, randomized trials have only demonstrated minor tenofovir-related changes in kidney function, but these studies included patients with normal kidney function and with low underling risk for progression of their renal function, had limited size, and limited follow-up. Several potential mechanisms of tenofovir nephrotoxicity are known. Atazanavir can, equally to indinavir, cause urolithiasis, but both drugs have also been associated with chronic kidney disease (CKD) and fast declining eGFR in persons without clinical symptoms of urolithiasis, especially when the plasma drug concentration is boosted by concomitant ritonavir use. In 2012, only a minority of HIV-positive individuals are affected by drug-induced nephrotoxicity. However, in the future, the clinical impact and hence the requirement for more research in this area will likely increase due to ageing and continued cART exposure of the HIV-positive population. [ABSTRACT FROM AUTHOR]

Published

2012

8. Lack of a pharmacokinetic drug-drug interaction with venlafaxine extended-release/indinavir and desvenlafaxine extended-release/indinavir.

Author

Jann, Michael, Spratlin, Vicky, Momary, Kathryn, Zhang, Hailing, Turner, David, Penzak, Scott, Wright, Alan, and VanDenBerg, Chad

Subjects

*ACADEMIC medical centers, *ANTIDEPRESSANTS, *COMBINATION drug therapy, *CLINICAL trials, *CONTROLLED release preparations, *DRUG interactions, *HIGH performance liquid chromatography, *RESEARCH funding, *STATISTICAL sampling, *T-test (Statistics), *VENLAFAXINE, *DATA analysis software, *DESCRIPTIVE statistics, *INDINAVIR

Abstract

Purpose: To assess the effects of venlafaxine extended-release (XR) capsules and desvenlafaxine extended-release (XR) tablets upon indinavir pharmacokinetic properties when co-administrated to healthy volunteers. Methods: This was an open-label, two-period, fixed-dose study conducted at the clinical research unit located on a university campus. Twenty-four healthy volunteers enrolled in the study (mean age 28.3 ± 8.0 years). Each subject received a single dose of indinavir 800 mg on day 1. Subsequently, subjects were then randomly assigned to either the venlafaxine XR group ( N = 12) or the desvenlafaxine XR group ( N = 12). Starting on day 2, venlafaxine XR was dosed at 37.5 mg/day for 4 days and increased to 75 mg/day for 6 days. Desvenlafaxine XR was dosed at 50 mg/day for 10 days. On day 12, indivanvir 800 mg was co-administered to both the venlafaxine XR and the desvenlafaxine XR groups. The pharmacokinetics of indinavir were determined both before and at the end of antidepressant dosing. Plasma indinavir, venlafaxine, and desvenlafaxine concentrations were assayed by high-performance liquid chromatography with ultra-violet (UV) detection. Indinavir pharmacokinetic parameters were calculated by noncompartmental analysis using validated computer software. Results: Venlafaxine XR and desvenlafaxine XR did not produce any significant changes in indinavir disposition. Both antidepressants were well tolerated by the subjects with only minor adverse side effects. Conclusions: No pharmacokinetic drug-drug interaction was demonstrated between venlafaxine XR and indinavir or between desvenlafaxine XR and indinvair. The lack of interaction could be due to the venlafaxine and desvenlafaxine extended-release formulation. [ABSTRACT FROM AUTHOR]

Published

2012

9. Exposure to HIV-protease inhibitors selects for increased expression of P-glycoprotein (ABCB1) in Kaposi's sarcoma cells.

Author

Lucia, M. B., Anu, R., Handley, M., Gillet, J.-P., Wu, C.-P., De Donatis, G. M., Cauda, R., and Gottesman, M. M.

Subjects

*P-glycoprotein, *PROTEASE inhibitors, *KAPOSI'S sarcoma, *MESSENGER RNA, *DOXORUBICIN, *PACLITAXEL, *THERAPEUTICS, *HIV infection complications, *ANTINEOPLASTIC antibiotics, *CELL lines, *DRUG resistance, *DRUG resistance in cancer cells, *DRUG synergism, *FLOW cytometry, *FLUORESCENT antibody technique, *GENES, *GLYCOPROTEINS, *HETEROCYCLIC compounds, *OLIGOPEPTIDES, *POLYMERASE chain reaction, *PYRIDINE, *RESEARCH funding, *WESTERN immunoblotting, *TREATMENT effectiveness, *REVERSE transcriptase polymerase chain reaction, *ANTI-HIV agents, *HIV protease inhibitors, *INDINAVIR, *NELFINAVIR, *RITONAVIR, *PHARMACODYNAMICS

Abstract

Background: Given that HIV-protease inhibitors (HIV-PIs) are substrates/inhibitors of the multidrug transporter ABCB1, can induce ABCB1 expression, and are used in combination with doxorubicin for AIDS-Kaposi's Sarcoma (KS) treatment, the role that ABCB1 plays in mediating multidrug resistance (MDR) in a fully transformed KS cell line (SLK) was explored.Methods: The KS cells were exposed to both acute and chronic treatments of physiological concentrations of different HIV-PIs (indinavir, nelfinavir, atazanavir, ritonavir, or lopinavir), alone or together with doxorubicin. The ABCB1 mRNA and protein expression levels were then assessed by qRT-PCR and western blotting, flow cytometry, and immunofluorescence.Results: Chronic treatment of SLK cells with one of the five HIV-PIs alone or together resulted in increased resistance to doxorubicin. Co-treatment with one of the HIV-PIs in combination with doxorubicin resulted in a synergistic increase in resistance to doxorubicin, and the degree of resistance was found to correlate with the expression of ABCB1. The SLK cells were also revealed to be cross-resistant to the structurally unrelated drug paclitaxel.Conclusion: These studies suggest that ABCB1 is primarily responsible for mediating MDR in SLK cells selected with either HIV-PIs alone or in combination with doxorubicin. Therefore, the roles that ABCB1 and drug cocktails play in mediating MDR in KS in vivo should be evaluated. [ABSTRACT FROM AUTHOR]

Published

2011

10. Fluorescence Spectroscopy as Tool for Bone Development Monitoring in Newborn Rats.

Author

Drzazga, Zofia Krystyna, Kluczewska-Galka, Aneta, Michnik, Anna, Kaszuba, Michał, and Trzeciak, Hanna

Subjects

*FLUORESCENCE spectroscopy, *BONE growth, *MANDIBLE, *FEMUR, *RATS

Abstract

utofluorescence of the mandible and femur bones taken from newborn rats (7-, 14- and 28-day old) was studied. Endogenous fluorophores were excited with 231 nm, 291 nm, 340 nm and 360 nm wavelengths. Modifications in content and microenvironment of both noncolagenous and collagenous constituents of bone tissue as well as metabolic coenzymes during the bone formation with age were reflected in fluorescence emission spectra. The increase of emission from peptide bonds and tryptophan residues was noted with rat age while for collagen and metabolic coenzymes at the first 2 weeks only. After maternal administration of indinavir the changes in fluorescence intensity and shifts in position of peak maximum were found. The distinct drop of emission from peptide bonds and tryptophan residues in studied bones was detected. In the case of collagen and metabolic coenzymes the red shift of peak maximum was revealed. Fluorescence spectroscopy could be used to follow bone development in newborn rats and effect of maternal indinavir administration on offspring. [ABSTRACT FROM AUTHOR]

Published

2011

11. Development of Indinavir Submicron Lipid Emulsions Loaded with Lipoamino Acids- In Vivo Pharmacokinetics and Brain-Specific Delivery.

Author

Bollam, Swetha, Kandadi, Prabhakar, Apte, Shashank, and Veerabrahma, Kishan

Abstract

The aim of our present work was to develop indinavir O/W submicron lipid emulsions (SLEs) loaded with lipoamino acids for specific delivery to brain. Tetradecyl aspartic acid (A) and decyl glutamic acid (G) loaded stable SLEs of indinavir having a mean size range of 210-220 nm and average zeta potential of −23.54 ± 1.2 mV were developed using homogenization and ultrasonication. The cumulative % drug release from different SLEs varied in between 26% and 85%. The formulations, SLE, SLE-A3, and SLE-G3 were stable to the centrifugal stress, dilution stress, and storage at RT. The total drug content and entrapment efficiency were determined by HPLC method. During pharmacokinetic studies in male Wistar rats there was no significant difference in the serum levels of indinavir for SLE, SLE-A3 and SLE-G3 formulations at all time points. In tissue distribution studies, the therapeutic availability (TA) of indinavir in brain and kidneys for SLE-A3 were 4.27- and 2.66-fold whereas for SLE-G3 were 2.94 and 2.12 times, respectively, higher than that of indinavir solution. But when compared with that of SLE, in brain tissue the levels of indinavir from SLE-G3 and SLE-A3 varied in between 2.5- and 3.38-fold. While in case of the kidney, it was between 1.23- and 1.54-fold only. However, the TA is not significantly different in tissues like the heart, liver, and spleen. Thus, brain-specific delivery of indinavir was improved by including tetradecyl aspartic acid and decyl glutamic acid in submicron lipid emulsions. [ABSTRACT FROM AUTHOR]

Published

2011

12. Raman chemical mapping reveals site of action of HIV protease inhibitors in HPV16 E6 expressing cervical carcinoma cells.

Author

Dong-Hyun Kim, Jarvis, Roger M., Allwood, J. William, Batman, Gavin, Moore, Rowan E., Marsden-Edwards, Emma, Hampson, Lynne, Hampson, Ian N., and Goodacre, Royston

Subjects

*PAPILLOMAVIRUSES, *CERVICAL cancer, *CANCER cells, *LOPINAVIR-ritonavir, *PROTEIN analysis

Abstract

It has been shown that the HIV protease inhibitors indinavir and lopinavir may have activity against the human papilloma virus (HPV) type 16 inhibiting HPV E6-mediated proteasomal degradation of p53 in cultured cervical carcinoma cells. However, their mode and site of action is unknown. HPV-negative C33A cervical carcinoma cells and the same cells stably transfected with E6 (C33AE6) were exposed to indinavir and lopinavir at concentrations of 1 mM and 30 μM, respectively. The intracellular distribution of metabolites and metabolic changes induced by these treatments were investigated by Raman microspectroscopic imaging combined with the analysis of cell fractionation products by liquid chromatography-mass spectrometry (LC-MS). A uniform cellular distribution of proteins was found in drug-treated cells irrespective of cell type. Indinavir was observed to co-localise with nucleic acid in the nucleus, but only in E6 expressing cells. Principal components analysis (PCA) score maps generated on the full Raman hypercube and the corresponding PCA loadings plots revealed that the majority of metabolic variations influenced by the drug exposure within the cells were associated with changes in nucleic acids. Analysis of cell fractionation products by LC-MS confirmed that the level of indinavir in nuclear extracts was approximately eight-fold greater than in the cytoplasm. These data demonstrate that indinavir undergoes enhanced nuclear accumulation in E6-expressing cells, which suggests that this is the most likely site of action for this compound against HPV. [ABSTRACT FROM AUTHOR]

Published

2010

13. Severe Impairment of Endothelial Function with the HIV-1 Protease Inhibitor Indinavir is not Mediated by Insulin Resistance in Healthy Subjects.

Author

Dubé, Michael P., Gorski, Jude Christopher, and Changyu Shen

Subjects

GLUCOSE, HYPOGLYCEMIC agents, DIABETES complications, DRUG resistance, INSULIN resistance

Abstract

Endothelial dysfunction may contribute to increased cardiovascular events among HIV-1-infected patients receiving antiretroviral therapy. The HIV-1 protease inhibitor indinavir causes both vascular dysfunction and insulin resistance, but the relationship between the two disturbances is not established. Endothelium-dependent vasodilation (EDV), insulin-mediated vasodilation (IMV), and whole body and leg glucose uptake during a euglycemic hyperinsulinemic clamp (40 mU/m²/min) were measured before and after four weeks of indinavir in nine healthy men. EDV fell from 270 ± 67% above basal to 124 ± 30% (P = 0.04) and IMV from 56 ± 14% above basal to 8 ± 8% (P = 0.001) with indinavir. During the clamp, arteriovenous glucose difference and leg glucose uptake were not significantly different after indinavir and whole-body glucose uptake was only modestly reduced (8.0 ± 0.8 vs. 7.2 ± 0.8 mg/kg/min, P = 0.04). The change in EDV did not correlate with the change in whole- body glucose uptake after indinavir (r = 0.21, P = 0.6). Despite marked impairment of endothelial function and IMV with indinavir, only modest, inconsistent reductions in measures of insulin-stimulated glucose uptake occurred. This suggests that indinavir's effects on glucose metabolism are not directly related to indinavir-associated endothelial dysfunction. Studies of the vascular effects of newer protease inhibitors are needed. [ABSTRACT FROM AUTHOR]

Published

2008

14. Megestrol Acetate NCD Oral Suspension — Par Pharmaceutical.

Published

2007

15. Maintenance of indinavir by dose adjustment in HIV-1-infected patients with indinavir-related toxicity.

Author

Wasmuth, J.-C., Lambertz, I., Voigt, E., Vogel, M., Hoffmann, C., Burger, D., and Rockstroh, J. K.

Subjects

*HIV-positive persons, *TOXICITY testing, *NEPHROTOXICOLOGY, *SKIN abnormalities, *DRUG monitoring, *ANTIVIRAL agents

Abstract

Treatment with indinavir/ritonavir (IDV/RTV) is very effective but hampered by frequent development of IDV-associated adverse events (mainly nephrotoxicity and skin changes). We tested whether dose reduction of IDV guided by therapeutic drug monitoring resulted in improved tolerability without compromising antiviral efficacy. HIV-infected patients with any IDV/RTV regimen who suffer from IDV-related adverse events were included. Viral load had to be adequately controlled for at least 2 months prior to inclusion. Dose reduction from 800 mg to 600 or 400 mg IDV b.i.d. followed a specified protocol. IDV-related toxicity and IDV plasma concentrations were monitored for 24 weeks. IDV concentrations were quantified with a validated high performance liquid chromatography method. Twenty patients were included. Reasons for inclusion were: skin abnormalities 11, nephrotoxicity five, metabolic disturbances three, and hypertension one. IDV dose could be lowered to 400 mg b.i.d. in 13, to 600 mg b.i.d. in two patients. Five patients discontinued the treatment. Overall tolerability improved with respect to incidence and severity of adverse events. Median trough concentrations decreased from 1.02 mg/l (range 0.08–7.1) at baseline to 0.48 mg/l (0.11–1.4) after 24 weeks ( p = 0.03) and remained above the critical threshold of 0.1 mg/l at any time after dose reduction. There was no change of CD4 cell counts or viral suppression. There were no significant changes in other laboratory parameters (creatinine, bilirubin, triglycerides, cholesterol, blood count, and urinalysis). Dose reduction of IDV improved tolerability of IDV-containing highly active antiretroviral treatment (HAART). Sufficient IDV trough concentrations were maintained in all patients as was virologic control. [ABSTRACT FROM AUTHOR]

Published

2007

16. Nanotechnology: A Focus on Nanoparticles as a Drug Delivery System.

Author

Kingsley, Jeffrey, Dou, Huanyu, Morehead, Justin, Rabinow, Barrett, Gendelman, Howard, and Destache, Christopher

Abstract

This review will provide an in-depth discussion on the previous development of nanoparticle-based drug delivery systems (DDS) and discuss original research data that includes the therapeutic enhancement of antiretroviral therapy. The use of nanoparticle DDS will allow practitioners to use drugs to target specific areas of the body. In the treatment of malignancies, the use of nanoparticles as a DDS is making measurable treatment impact. Medical imaging will also utilize DDS to illuminate tumors, the brain, or other cellular functions in the body. The utility of nanoparticle DDS to improve human health is potentially enormous. [ABSTRACT FROM AUTHOR]

Published

2006

17. HIV protease inhibitor therapy reverses neutrophil apoptosis in AIDS patients by direct calpain inhibition.

Author

Lichtner, M., Mengoni, F., Mastroianni, C. M., Sauzullo, I., Rossi, R., De Nicola, M., Vullo, V., and Ghibelli, L.

Subjects

NEUTROPHILS, APOPTOSIS, CELL death, CALPAIN, CYSTEINE proteinases, THERAPEUTICS

Abstract

The reduction of neutrophils apoptosis is one of the main non-virological effects of protease inhibitor (PI) therapy. We explore here whether this may be due to the cross-inhibition of calpain, an important non-virological target of PI in vitro. We found that the high basal level of neutrophils apoptosis in AIDS patients is strictly related to an increased intracellular calpain activity. Both alterations disappear after PI treatment, with apoptosis and calpain going back to normal levels after 3 months of PI therapy, independently of a proficient antiviral effect. PI drugs exerted a similar antiapoptotic and anticalpain effects on neutrophils in ex vivo experiments: strikingly, the effects were mimicked by commercially available calpain inhibitors. This study shows, for the first time, that apoptosis of neutrophils in AIDS patients is mediated by calpain, and that neutrophil survival in PI treated AIDS patients is a non virological effect due to calpain inhibition. [ABSTRACT FROM AUTHOR]

Published

2006

18. High variability of indinavir and nelfinavir pharmacokinetics in HIV-infected patients with a sustained virological response on highly active antiretroviral therapy.

Author

Goujard, Cécile, Legrand, Mayeule, Panhard, Xavière, Diquet, Bertrand, Duval, Xavier, Peytavin, Gilles, Vincent, Isabelle, Katlama, Christine, Leport, Catherine, Bonnet, Bénédicte, Salmon-Céron, Dominique, Mentré, France, Taburet, Anne-Marie, Goujard, Cécile, Panhard, Xavière, Bonnet, Bénédicte, Salmon-Céron, Dominique, Mentré, France, and COPHAR1-ANRS 102 Study Group

Subjects

*PHARMACOKINETICS, *HIV-positive persons, *ANTIRETROVIRAL agents, *THERAPEUTICS, *PROTEASE inhibitors, *LINEAR statistical models, *CLINICAL trials, *COMPARATIVE studies, *HIV infections, *LONGITUDINAL method, *RESEARCH methodology, *MEDICAL cooperation, *PATIENT compliance, *RESEARCH, *VIRAL load, *EVALUATION research, *HIGHLY active antiretroviral therapy, *HIV protease inhibitors, *INDINAVIR, *NELFINAVIR, *RITONAVIR

Abstract

Objectives: To describe plasma concentrations of indinavir alone or combined with ritonavir, and of nelfinavir and its active metabolite M8, and to measure their variabilities in HIV-infected patients treated with a stable antiretroviral regimen and experiencing a sustained virological response for at least 12 months. Patients and methods: In this prospective trial, blood samples were drawn during a 6-hour time interval between two doses at enrolment to assess protease inhibitor (PI) pharmacokinetic parameters, and 4 months later to assess plasma trough and peak concentrations. Safety and adherence assessments and laboratory data were collected during an 8-month period. PI pharmacokinetic characteristics were analysed using a non-compartmental approach. Inter- and intrapatient variabilities were estimated using a linear mixed-effect model. The impact of different covariates on plasma trough concentrations was investigated. Eighty-eight patients were analysed: 42 treated with indinavir and 46 with nelfinavir. Results: The interquartile range (IQR) of the plasma trough concentration corrected for the sampling time (Ccalc) was 116–374 μg/L for indinavir alone and 163–508 μg/L for indinavir/ritonavir. Ritonavir significantly increased indinavir elimination half-life and plasma exposure. For nelfinavir, the IQR of Ccalc was 896–2059 μg/L for three-times-daily administration and 998–2124 μg/L for twice-daily administration. Variabilities were high for both PIs. Intrapatient variability for indinavir alone (and indinavir + ritonavir) was 76% (107%) and interpatient variability was 58% (10%) in adherent patients. Intrapatient variability for nelfinavir three times daily (and twice daily) was 41% (74%) and interpatient variability was 62% (50%). Intrapatient variability was lowered in patients with a high adherence level. Conclusion: Although performed in a homogeneous population, this study documented a high interpatient but also intrapatient variability of indinavir and nelfinavir pharmacokinetics, which should be taken into account when interpreting therapeutic drug monitoring. Once patients have reached a sustained virological response, plasma PI monitoring may have a limited impact. [ABSTRACT FROM AUTHOR]

Published

2005

19. Evaluation of a Liquid Chromatographic Method for Analysis of Indinavir and Degradation Products Arising from Hydrolysis of its Amide Bond.

Author

Jancic, B., Medenica, M., Ivanovic, D., and Malenovic, A.

Abstract

Indinavir, an antiviral drug, is a member of the novel hydroxyaminopentane amides class of HIV-1 protease inhibitors. It is the active substance in capsules which contain 400 mg indinavir as the sulfate salt and degradation products, a lactone and cis-aminoindanol, arising as a result of hydrolysis of its amide bond (at most 1.5% of the lactone and 0.5% cis-aminoindanol). RP HPLC has been evaluated as a method for qualitative and a quantitative analysis of indinavir and its degradation products in capsules. During method development the effects of several stationary and mobile phases on the separation were investigated. Separations were performed on an X Terra RP18, 150 mm × 4.6 mm, 5 µm particle size, column at 20°C. The mobile phase was 35:65 ( v/ v) mixture of acetonitrile and an aqueous solution of sodium lauryl sulfate and triethylamine. UV detection was performed at 214 nm. Important statistical data were determined for validation of the selectivity/specificity, linearity, precision, robustness, limit of detection, and limit of quantitation of the method. The validated method was then used for determination of amounts of indinavir (recovery between 100.6 and 103.1%) and compounds resulting from hydrolysis of its amide bond (the lactone, 0.265%, and cis-aminoindanol, 0.07%). The method is suitable for simultaneous determination of indinavir and its degradation products in pharmaceuticals and the bulk drug. [ABSTRACT FROM AUTHOR]

Published

2005

20. Pharmacokinetics of antiretroviral therapy in HIV-1-infected children.

Author

Fraaij, Pieter L. A., van Kampen, Jeroen J. A., Burger, David M., and de Groot, Ronald

Subjects

*PHARMACOLOGY, *ANTIVIRAL agents, *HIV infections, *DRUG dosage, *THERAPEUTICS, *CHEMICAL kinetics, *COMPARATIVE studies, *HIV, *RESEARCH methodology, *MEDICAL cooperation, *MEDICAL protocols, *RESEARCH, *EVALUATION research, *ANTI-HIV agents

Abstract

The initiation of antiretroviral therapy has resulted in an impressive reduction in the rate of disease progression in AIDS and HIV-1-related deaths in children; however, there are still several major challenges to be faced in order to improve therapy. A major topic that needs to be dealt with is the establishment of the optimal dosage of antiretroviral therapy for children. This review presents the currently available peer-reviewed data on the pharmacokinetics of nucleoside reverse transcriptase inhibitors (NRTIs), non-nucleoside reverse transcriptase inhibitors (NNRTIs), protease inhibitors (PIs) and fusion inhibitors (FIs) in children. In addition, the data are discussed in relation to the currently available European and US guidelines and the US FDA-approved drug labels. High intra- and interpatient variability in pharmacokinetics are often observed for all antiretroviral drugs. The number of children included in the pharmacokinetic studies is often small and children are often divided into divergent groups using different dosage levels and/or drug formulations. For a substantial number of antiretroviral drugs, dosage recommendations, especially for young children, are still absent in the European and US guidelines. The recommended drug dosages in the guidelines are often different from that in the officially approved drug product label. In addition, the recommended drug dosages may deviate between the European and US guidelines. Thus, while practioners aim to meet the recommendations in the official guidelines, patients may receive highly divergent dosages of medication. The high intra- and interpatient variability in pharmacokinetics of antiretroviral drugs in children hampers the application of fixed dosages of antiretroviral drugs. For PIs and NNRTIs, plasma drug levels correlate with viral suppression and drug toxicity. NRTIs are prodrugs that are intracellularly converted to their active triphosphate form and, therefore, plasma NRTI levels correlate poorly with viral suppression. Therapeutic drug monitoring of PIs and NNRTIs should be considered to optimise HIV therapy in children. [ABSTRACT FROM AUTHOR]

Published

2005

21. Application and impact of population pharmacokinetics in the assessment of antiretroviral pharmacotherapy.

Author

Barrett, Jeffrey S., Labbé, Line, Pfister, Marc, and Labbé, Line

Subjects

*PHARMACOKINETICS, *DRUG therapy, *DRUG monitoring, *HIV-positive persons, *CLINICAL trials, *CLINICAL drug trials

Abstract

Population pharmacokinetics has been an important technique used to explore and define relevant sources of variation in drug exposure and response in patient populations. This has been especially true in the area of antiretroviral therapy where the assurance of adequate and sustained drug exposure of multiple agents is highly correlated with therapeutic success. Population pharmacokinetic analyses across the four drug classes and 20 US FDA-approved products used to treat HIV have been published to date. The published reports were predominantly based on actual clinical trials conducted in HIV-infected patients with one or more agents administered. Modelling and simulation approaches have been used in the evaluation of antiretroviral agent outcomes incorporating problematic design and analysis factors such as sparse plasma sampling, data imbalance and censored data. Additional benefits of population modelling approaches applied to the investigation of antiretroviral agents include the ability to assess dosing compliance, understanding and quantifying drug-drug interactions in order to select dosing regimens and the screening of new drug candidates. Pharmacokinetic/pharmacodynamic models have been used to characterise the relationship between drug exposure and virological and immunological response, and to predict clinical outcome. These models offer the best opportunity for individualising and optimising patient therapy, particularly when adjusted for adherence/compliance. The impact of population pharmacokinetics in the area of antiretroviral therapy can be directly assessed by its role in the validation of surrogate markers such as viral RNA load, therapeutic drug monitoring and the management of individual patient outcomes via exposure-toxicity relationships. Each of these population pharmacokinetic outcomes has contributed to the current regulatory environment, specifically in the area of accelerated approval of new antiretroviral agents. [ABSTRACT FROM AUTHOR]

Published

2005

22. Milk thistle and indinavir: a randomized controlled pharmacokinetics study and meta-analysis.

Author

Mills, Edward, Wilson, Kumanan, Clarke, Mike, Foster, Brian, Walker, Scott, Rachlis, Beth, DeGroot, Nick, Montori, Victor M., Gold, Wayne, Phillips, Elizabeth, Myers, Stephen, and Gallicano, Keith

Subjects

*MILK thistle, *SILYBUM, *INGESTION, *CLINICAL trials, *META-analysis, *PHARMACOKINETICS

Abstract

To determine whether ingestion of milk thistle affects the pharmacokinetics of indinavir. We conducted a three-period, randomized controlled trial with 16 healthy participants. We randomized participants to milk thistle or control. All participants received initial dosing of indinavir, and baseline indinavir levels were obtained (AUC0-8) (phase I). The active group were then given 450 mg milk-thistle extract capsules to be taken t.i.d. from day 2 to day 30. The control group received no plant extract. On day 29 and day 30, indinavir dosing and sampling was repeated in both groups as before (phase II). After a wash-out period of 7 days, indinavir dosing and sampling were repeated as before (phase III). All participants completed the trial, but two were excluded from analysis due to protocol violation. There were no significant between-group differences. Active group mean AUC0-8 indinavir decreased by 4.4% (90% CI, -27.5% to -26%, P=0.78) from phase I to phase II in the active group, and by 17.3% (90% CI, -37.3% to +9%, P=0.25) in phase III. Control group mean AUC0-8 decreased by 21.5% (90% CI, -43% to +8%, P=0.2) from phase I to phase II and by 38.5% (90% CI, -55.3% to -15.3%, P=0.01) of baseline at phase III. To place our findings in context, milk thistle-indinavir trials were identified through systematic searches of the literature. A meta-analysis of three milk thistle-indinavir trials revealed a non-significant pooled mean difference of 1% in AUC0-8 (95% CI, -53% to 55%, P=0.97). Indinavir levels were not reduced significantly in the presence of milk thistle. [ABSTRACT FROM AUTHOR]

Published

2005

23. HAART drugs induce mitochondrial damage and intercellular gaps and gp 120 causes apoptosis.

Author

Fiala, Milan, Murphy, Thomas, MacDougall, James, Yang, Wendy, Luque, Alfonso, Iruela-Arispe, Luisa, Cashman, John, Buga, Georgette, Byrns, Russel, Barbaro, Giuseppe, and Arthos, James

Abstract

HIV-1 infection is associated with serious cardiovascular complications, but the roles of HIV-1, viral proteins, and highly active antiretroviral therapy (HAART) drugs are not understood. HAART decreases the overall risk of heart disease but leads to metabolic disturbances and possibly coronary artery disease. We investigated toxicities of HIV-1, HIV-1 glycoprotein 120 (gp 120), and HAART drugs for human coronary artery endothelial cells (CAECs), brain microvascular endothelial cells, and neonatal rat ventricular myocytes (NRVMs). HIV-1 and gp 120, but not azidothymidine (AZT), induced apoptosis of NRVMs and CAECs. Ethylisothiourea, an inhibitor of nitric oxide synthase, inhibited apoptosis induction by gp 120. AZT, HIV-1, and gp 120 all damaged mitochondria of cardiomyocytes. HAART drugs, AZT, and indinavir, but not HIV-1, produced intercellular gaps between confluent endothelial cells and decreased transendothelial electrical resistance. In conclusion, HIV-1 and gp 120 induce toxicity through induction of cardiomyocyte and endothelial cell apoptosis. HAART drugs disrupt endothelial cell junctions and mitochondria and could cause vascular damage. [ABSTRACT FROM AUTHOR]

Published

2004

24. Pharmacokinetics of antiretrovirals in pregnant women.

Author

Mirochnick, Mark and Capparelli, Edmund

Subjects

*PREGNANCY, *OBSTETRICS, *HIV-positive women, *PHARMACOLOGY, *AIDS prevention, *PHARMACOKINETICS

Abstract

Antiretroviral treatment of HIV-infected pregnant women is widely used to prevent mother-to-child HIV transmission and as primary therapy of maternal HIV infection. The physiological changes associated with pregnancy have a large impact on drug disposition, and changes in antiretroviral pharmacokinetics during pregnancy must be understood for these drugs to be used safely and effectively in pregnant women. Zidovudine and didanosine, two of the nucleoside reverse transcriptase inhibitors, demonstrate an increase in clearance and decrease in area under the concentration-time curve during pregnancy. The clinical significance of these changes is unknown due to the lack of a clear relationship between plasma concentrations of nucleoside reverse transcriptase inhibitors and clinical effects. Pharmacokinetic parameters of lamivudine, stavudine and abacavir are not significantly changed during pregnancy. There are no data describing the effect of pregnancy on the pharmacokinetics of the other nucleoside/nucleotide analogues (zalcitabine, emtricitabine and tenofovir). Pregnancy does not appear to have a significant effect on the pharmacokinetics of the non-nucleoside reverse transcriptase inhibitor nevirapine and there are no data describing the pharmacokinetics of the other non-nucleoside reverse transcriptase inhibitors (efavirenz and delavirdine) during pregnancy. Reduced plasma concentrations during pregnancy have been described for several of the protease inhibitors, including nelfinavir (with administration of 750mg three times daily), indinavir, saquinavir and Kaletra® (a co-formulation of lopinavir and ritonavir). Plasma concentrations equivalent to those in nonpregnant adults have been reported in pregnant women receiving nelfinavir at doses of 1250mg twice daily, and the addition of ritonavir to saquinavir greatly increases saquinavir exposure to therapeutic concentrations in pregnant women. No pregnancy pharmacokinetic data are available for the newer protease inhibitors atazanavir and fosamprenavir, or with other dual protease inhibitor combinations that include low dose ritonavir to boost concentrations of the coadministered protease inhibitor. Further investigations of antiretroviral pharmacology during pregnancy, including protein binding studies, are urgently needed. [ABSTRACT FROM AUTHOR]

Published

2004

25. Practical guidelines to interpret plasma concentrations of antiretroviral drugs.

Author

Kappelhoff, Bregt S., Crommentuyn, Kristel M. L., de Maat, Monique M. R., Mulder, Jan W., Huitema, Alwin D. R., and Beijnen, Jos H.

Subjects

*ANTIRETROVIRAL agents, *DRUG monitoring, *HIV-positive persons, *PATIENT monitoring, *REVERSE transcriptase, *DRUGS

Abstract

Several relationships have been reported between antiretroviral drug concentrations and the efficacy of treatment, and toxicity. Therefore, therapeutic drug monitoring (TDM) may be a valuable tool in improving the treatment of HIV-1-infected patients in daily practice. In this regard, several measures of exposure have been studied, e.g. trough and maximum concentrations, concentration ratios and the inhibitory quotient. However, it has not been unambiguously established which pharmacokinetic parameter should be monitored to maintain optimal viral suppression. Each pharmacokinetic parameter has its pros and cons. Many factors can affect the pharmacokinetics of antiretroviral agents, resulting in variability in plasma concentrations between and within patients. Therefore, plasma concentrations should be considered on several occasions. In addition, the interpretation of the drug concentration of a patient should be performed on an individual basis, taking into account the clinical condition of the patient. Important factors herewith are viral load, immunology, occurrence of adverse events, resistance pattern and comedication. In spite of the described constraints, the aim of this review is to provide a practical guide for TDM of antiretroviral agents. This article outlines pharmacokinetic target values for the HIV protease inhibitors amprenavir, atazanavir, indinavir, lopinavir, nelfinavir, ritonavir and saquinavir, and the non-nucleoside reverse transcriptase inhibitors efavirenz and nevirapine. Detailed advice is provided on how to interpret the results of TDM of these drugs. [ABSTRACT FROM AUTHOR]

Published

2004

26. Indinavir-Urolithiasis bei HIV-positiven Patienten.

Author

Kalaitzis, C., Touloupidis, S., Patris, E., Lehrich, K., and Kuntz, R.

Abstract

Copyright of Der Urologe A is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2004

27. Therapeutic Drug Monitoring of Indinavir in H IV-Infected Patients Undergoing HAART.

Author

Langmann, P., Zilly, M., Weißbrich, B., Desch, S., Väth, T., and Klinker, H.

Subjects

DRUG monitoring, ANTIRETROVIRAL agents, HIV-positive persons, PROTEASE inhibitors, CLINICAL drug trials, BLOOD plasma

Abstract

Background: Therapeutic drug monitoring (TDM) of protease inhibitors (PI) is gaining increasing importance for the management of HIV-infected patients undergoing highly active antiretroviral. therapy (HAART). The PI indinavir (IDV) is widely used in HAART regimens. Combinations of IDV with ritonavir (RTV) have been used to increase the plasma concentration of IDV. However, the desirable IDV concentration range in clinical, practice remains to be elucidated. Patients and Methods: To study the value of TDM for IDV in clinical, practice, a retrospective analysis of 501 plasma samples of patients treated with IDV in various dosages was performed. IDV level were determined during routine outpatient visits. Analysis was performed by high pressure liquid chromatography (H PLC) with UV detection. Results: A widespread range of IDV plasma concentrations was seen both within and between patients. The mean IDV level during therapy with IDV 2.4 g/d was 3,260 ng/ml (95% CI: 2,903 ng/ml.; 3,618 ng/ml). IDV level at a dose of IDV 1.6g/d in combination with RTV resulted in a mean IDV plasma concentration of 4,191 ng/ml (95% CI: 3,356 ng/ml; 5,026 ng/ml). There was no significant difference between plasma level at the doses of 2.4 g/d and 1.6 g/d. 35 of all 130 patients treated with IDV reached only suboptimal IDV plasma concentrations below the limit of 150 ng/ml. There was no statistically significant difference between the number of patients below an IDV plasma concentration of 150 ng/ml in the various dosage regimens. Conclusion: During therapy with IDV in a b.i.d. scheme, similar IDV plasma concentrations and a comparable number of patients with subinhibitory plasma concentrations were observed when compared to a therapeutic regimen with t.i.d. dosing. In this study, even at various times of plasma sampling after oral ingestion, TCM facilitated the surveillance of patients compliance. [ABSTRACT FROM AUTHOR]

Published

2002

28. Meal Composition Effects on the Oral Bioavailability of Indinavir in HIV-Infected Patients.

Author

Carver, Peggy, Fleisher, David, Zhou, Simon, Kaul, Daniel, Kazanjian, Powel, and Li, Cheng

Abstract

Purpose. To study the influence of large-volume high-calorie protein, fat, and carbohydrate meals and a non-caloric hydroxypropylmethyl cellulose (HPMC) viscous meal on the oral bioavailability of indinavir in HIV-infected subjects. Methods. Seven male HIV-infected subjects received caloric meal treatments and control meals in a randomized crossover fashion and the viscosity meal as a final treatment. The total volume of each meal treatment was 500 mL and the caloric meals each contained 680 kcal. Gastric pH was also monitored by radiotelemetry from one hour before to four hours after drug and caloric meal administration. A single Crixivan™ (indinavir sulfate) dose equivalent to 600 mg indinavir was administrated orally with 100 mL of water immediately following meal administration. Indinavir plasma concentrations were obtained using reverse-phase HPLC. Results. All meal treatments significantly decreased the extent of indinavir absorption as compared to fasted control. AUC0−∞ decreased by 68%, 45%, 34%, and 30% for protein, carbohydrate, fat, and viscosity meal treatments versus fasted control, respectively (p < 0.05). The mean Cmax was significantly decreased 74%, 59%, 46% and 36% (p < 0.05) and the mean tmax was significantly delayed from 1 hr in fasted controls to 3.8, 3.6, 2.1 and 2.0 hrs (p < 0.05) for protein, carbohydrate, fat, and viscosity meal treatments, respectively. The elimination half-life of indinavir determined in the fasted state was decreased in HIV-infected subjects as compared to the reported half-life in normal healthy subjects. Conclusions. Reductions in indinavir plasma concentrations compared to drug administration in the fasted state are most severe with the high-calorie protein meal. This is consistent with an influence of elevated gastric pH on drug precipitation. Significant drug plasma concentration reductions observed with administration of the other meals in the absence of appreciably elevated gastric pH profile indicate that other factors are playing a role in the meal effects. The similarity in indinavir plasma profiles with protein and carbohydrate versus fat and viscosity suggests that the latter meals may reduce the impact of drug precipitation compared to the former meals. [ABSTRACT FROM AUTHOR]

Published

1999

29. Clinical pharmacology of HIV protease inhibitors: focus on saquinavir, indinavir, and ritonavir.

Author

Hoetelmans, R.M.W., Koks, C.H.W., Beijnen, J.H., Meenhorst, P.L., Mulder, J.W., and Burger, D.M.

Abstract

In this review the clinical pharmacology of HIV protease inhibitors, a new class of antiretroviral drugs, is discussed. After considering HIV protease function and structure, the development of inhibitors of HIV protease is presented. Three protease inhibitors are reviewed in more detail: saquinavir, indinavir, and ritonavir. Clinical trial results with these agents are evaluated. Furthermore, adverse effects, resistance, dosage and administration, clinical pharmacokinetics, pharmacokinetic-pharmacodynamic relationships, and drug interactions are discussed. [ABSTRACT FROM AUTHOR]

Published

1997

30. Despite limitations, therapeutic drug monitoring may be of value in antiretroviral treatment in HIV-infected patients.

Author

Adis International Limited

Subjects

*DRUG monitoring, *DRUG analysis, *HIV-positive persons, *HIV infections, *THERAPEUTICS, *ANTIRETROVIRAL agents

Abstract

Focuses on the benefits of therapeutic drug monitoring (TDM) in the treatment of HIV-infected patients. Factors influencing the risk of failure of antiretroviral therapy; Usefulness of TDM; Objective of TDM.

Published

2005

31. Indinavir Alters the Pharmacokinetics of Lamivudine Partially via Inhibition of Multidrug and Toxin Extrusion Protein 1 (MATE1)

Author

Li, Qing, Ye, Zhi, Zhu, Peng, Guo, Dong, Yang, Hong, Huang, Jin, Zhang, Wei, Polli, James E., and Shu, Yan

Published

2018

32. Cobicistat/elvitegravir/emtricitabine/tenofovir-alafenamide/indinavir/simvastatin interactions.

Subjects

*TENOFOVIR, *INDINAVIR, *DRUG interactions

Published

2019

33. Papillary Necrosis Associated with the HIV Protease Inhibitor Indinavir.

Author

Dieleman, J. P., van der Feltz, M., Bangma, C. H., Stricker, B. H. C., and van der Ende, M. E.

Subjects

NECROSIS, GANGRENE, KIDNEY diseases, KIDNEY stones, ACUTE kidney failure, INTERSTITIAL nephritis

Abstract

The HIV protease inhibitor indinavir may cause nephrolithiasis and interstitial nephritis. The renal consequences of indinavir-associated nephrotoxicity are uncertain. We report a case of papillary necrosis in a patient treated with indinavir. An asymptomatic HIV-infected woman experienced rightsided renal colicky pain during treatment with indinavir. She passed a non-solid stone and continued indinavir treatment. Intravenous pyelogram performed 20 months later following an episode of left-sided colicky pain showed right-sided papillary necrosis. Indinavir-associated nephrolithiasis and chronic interstitial nephritis were the only possible causes identified in this patient. Physicians should be aware that indinavir nephrolithiasis may cause papillary necrosis. [ABSTRACT FROM AUTHOR]

Published

2001

34. Osteoporosis: case report.

Subjects

*INDINAVIR

Abstract

The article presents a case study of a 45-year-old HIV carrier man who developed osteoporosis while receiving treatment with indinavir.

Published

2016

35. Predictors of first-line antiretroviral therapy discontinuation due to drug-related adverse events in HIV-infected patients: a retrospective cohort study

Author

Iuri Fanti, Alessandro D'Avino, Annalisa Mondi, Simona Di Giambenedetto, Manuela Colafigli, Mauro Zaccarelli, Roberto Cauda, Mattia Prosperi, Massimiliano Fabbiani, and Alberto Borghetti

Subjects

Adult, Male, medicine.medical_specialty, HAART, Time Factors, Efavirenz, Drug-Related Side Effects and Adverse Reactions, HIV Infections, lcsh:Infectious and parasitic diseases, Cohort Studies, chemistry.chemical_compound, Pregnancy, Indinavir, Antiretroviral Therapy, Highly Active, Internal medicine, medicine, Humans, lcsh:RC109-216, Risk factor, Side effects, Adverse effect, Didanosine, Retrospective Studies, Toxicity, business.industry, Stavudine, HIV, Prognosis, Discontinuation, Infectious Diseases, Anti-Retroviral Agents, Withholding Treatment, chemistry, Immunology, Female, Ritonavir, Therapy-naïve, business, Research Article, medicine.drug

Abstract

Background Drug-related toxicity has been one of the main causes of antiretroviral treatment discontinuation. However, its determinants are not fully understood. Aim of this study was to investigate predictors of first-line antiretroviral therapy discontinuation due to adverse events and their evolution in recent years. Methods Patients starting first-line antiretroviral therapy were retrospectively selected. Primary end-point was the time to discontinuation of therapy due to adverse events, estimating incidence, fitting Kaplan-Meier and multivariable Cox regression models upon clinical/demographic/chemical baseline patients’ markers. Results 1,096 patients were included: 302 discontinuations for adverse events were observed over 1,861 person years of follow-up between 1988 and 2010, corresponding to an incidence (95% CI) of 0.16 (0.14-0.18). By Kaplan-Meier estimation, the probabilities (95% CI) of being free from an adverse event at 90 days, 180 days, one year, two years, and five years were 0.88 (0.86-0.90), 0.85 (0.83-0.87), 0.79 (0.76-0.81), 0.70 (0.67-0.74), 0.55 (0.50-0.61), respectively. The most represented adverse events were gastrointestinal symptoms (28.5%), hematological (13.2%) or metabolic (lipid and glucose metabolism, lipodystrophy) (11.3%) toxicities and hypersensitivity reactions (9.3%). Factors associated with an increased hazard of adverse events were: older age, CDC stage C, female gender, homo/bisexual risk group (vs. heterosexual), HBsAg-positivity. Among drugs, zidovudine, stavudine, zalcitabine, didanosine, full-dose ritonavir, indinavir but also efavirenz (actually recommended for first-line regimens) were associated to an increased hazard of toxicity. Moreover, patients infected by HIV genotype F1 showed a trend for a higher risk of adverse events. Conclusions After starting antiretroviral therapy, the probability of remaining free from adverse events seems to decrease over time. Among drugs associated with increased toxicity, only one is currently recommended for first-line regimens but with improved drug formulation. Older age, CDC stage, MSM risk factor and gender are also associated with an increased hazard of toxicity and should be considered when designing a first-line regimen.

36. Drug susceptibility to etravirine and darunavir among Human Immunodeficiency Virus Type 1-derived pseudoviruses in treatment-experienced patients with HIV/AIDS in South Korea

Author

Mina Park, Ju-yeon Choi, Mee-Kyung Kee, Ohkyung Kwon, Hye-Ri Oh, Jee Eun Rhee, and Sung Soon Kim

Subjects

Efavirenz, Genotype, Anti-HIV Agents, Etravirine, HIV Infections, Treatment-experienced, Microbial Sensitivity Tests, Drug resistance, Biology, gag Gene Products, Human Immunodeficiency Virus, Inhibitory Concentration 50, Amprenavir, chemistry.chemical_compound, Acquired immunodeficiency syndrome (AIDS), Indinavir, Antiretroviral Therapy, Highly Active, Virology, Drug Resistance, Viral, Nitriles, Republic of Korea, medicine, Humans, Genotypic drug resistance, Protein Precursors, Darunavir, Recombination, Genetic, Acquired Immunodeficiency Syndrome, Korea, Phenotypic drug susceptibility, Research, virus diseases, Raltegravir, medicine.disease, Pyridazines, Phenotype, Pyrimidines, Infectious Diseases, chemistry, pol Gene Products, Human Immunodeficiency Virus, Mutation, HIV-1, medicine.drug

Abstract

Background In South Korea, about 20 types of antiretroviral drugs are used in the treatment of patients with human immunodeficiency virus/acquired immune deficiency syndrome. Since 2010, raltegravir, etravirine, and darunavir have been spotlighted as new drugs for highly active antiretroviral therapy (HAART)-experienced adults with resistant HIV-1 in South Korea. In this study, we investigated potential susceptibility of pseudoviruses derived from treatment-experienced Korean patients to etravirine vs efavirenz and to darunavir vs amprenavir and indinavir using a modified single-round assay. Methods Pseudoviruses derived from nine treatment-experienced patients infected with HIV-1 were investigated by comparison with the wild-type strain pNL4-3. The 50% inhibitory concentration (IC50) values were calculated and drug susceptibility was compared. The intensity of genotypic drug resistance was classified based on the ‘SIR’ interpretation of the Stanford data base. Results Drug susceptibility was generally higher for etravirine and darunavir compared with efavirenz, amprenavir, and indinavir in pseudoviruses derived from treatment-experienced patients. Pseudoviruses derived from patients KRB4025 and KRB8014, who exhibited long-term use of protease inhibitors, showed an outside of tested drug concentration, especially for amprenavir and indinavir. However, they exhibited a lower fold-change in resistance to darunavir. Conclusions Etravirine and darunavir have been used in HAART since 2010 in South Korea. Therefore, these antiretroviral drugs together with other newly introduced antiretroviral drugs are interesting for the optimal treatment of patients with treatment failure. This study may help to find a more effective HAART in the case of HIV-1 infected patients that have difficulty being treated.

37. Osteomalacia in an HIV-infected man receiving rifabutin, a cytochrome P450 enzyme inducer: a case report

Author

Mark G. Thomas, Anne Horne, Mark J Bolland, and Andrew Grey

Subjects

Male, Microbiology (medical), Rifabutin, Mycobacterium avium-intracellulare infection, lcsh:QR1-502, HIV Infections, Case Report, Drug resistance, Biology, lcsh:Microbiology, lcsh:Infectious and parasitic diseases, Cytochrome P-450 Enzyme System, Bone Density, Indinavir, medicine, Humans, lcsh:RC109-216, Mycobacterium avium-intracellulare Infection, chemistry.chemical_classification, Osteomalacia, AIDS-Related Opportunistic Infections, fungi, lcsh:RM1-950, food and beverages, Cytochrome P450, General Medicine, Middle Aged, Alkaline Phosphatase, Vitamin D Deficiency, medicine.disease, Virology, Anti-Bacterial Agents, Enzyme, lcsh:Therapeutics. Pharmacology, Infectious Diseases, chemistry, Immunology, biology.protein, Hyperparathyroidism, Secondary, Ritonavir, medicine.drug

Abstract

Introduction People infected with human immunodeficiency virus are frequently treated with medications that can induce or inhibit cytochrome P450 enzymes. Case presentation A 59 year old man treated with zidovudine, lamivudine, indinavir, and ritonavir for infection with human immunodeficiency virus volunteered to take part in a study of bone loss. He was found to have vitamin D insufficiency with secondary hyperparathyroidism and received vitamin D and calcium supplementation. He suffered a recurrence of infection with Mycobacterium avium intracellulare for which he received treatment with ciprofloxacin, rifabutin, and ethambutol. Subsequently, he developed worsening vitamin D deficiency with hypocalcaemia, secondary hyperparathyroidism and elevated markers of bone turnover culminating in an osteomalacic vertebral fracture. Correction of the vitamin D deficiency required 100,000 IU of cholecalciferol monthly. Rifabutin is a cytochrome P450 inducer, and vitamin D and its metabolites are catabolised by cytochrome P450 enzymes. We therefore propose that treatment with rifabutin led to the induction of cytochrome P450 enzymes catabolising vitamin D, thereby causing vitamin D deficiency and osteomalacia. This process might be mediated through the steroid and xenobiotic receptor (SXR). Conclusion Treatment with rifabutin induces the cytochrome P450 enzymes that metabolise vitamin D and patients treated with rifabutin might be at increased risk of vitamin D deficiency. In complex medication regimens involving agents that induce or inhibit cytochrome P450 enzmyes, consultation with a clinical pharmacist or pharmacologist may be helpful in predicting and/or preventing potentially harmful interactions.