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Lack of a Significant Drug Interaction between Raltegravir and Tenofovir

Wenning, Larissa A. ; Friedman, Evan J. ; Kost, James T. ; [et al.]

American Society for Microbiology ; 2008

In: Antimicrobial Agents and Chemotherapy Vol. 52, No. 9 ( 2008-09), p. 3253-3258

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In: Antimicrobial Agents and Chemotherapy, American Society for Microbiology, Vol. 52, No. 9 ( 2008-09), p. 3253-3258

Abstract: Raltegravir is a novel human immunodeficiency virus type 1 (HIV-1) integrase inhibitor with potent in vitro activity (95% inhibitory concentration of 31 nM in 50% human serum). This article reports the results of an open-label, sequential, three-period study of healthy subjects. Period 1 involved raltegravir at 400 mg twice daily for 4 days, period 2 involved tenofovir disoproxil fumarate (TDF) at 300 mg once daily for 7 days, and period 3 involved raltegravir at 400 mg twice daily plus TDF at 300 mg once daily for 4 days. Pharmacokinetic profiles were also determined in HIV-1-infected patients dosed with raltegravir monotherapy versus raltegravir in combination with TDF and lamivudine. There was no clinically significant effect of TDF on raltegravir. The raltegravir area under the concentration time curve from 0 to 12 h (AUC 0-12 ) and peak plasma drug concentration ( C max ) were modestly increased in healthy subjects (geometric mean ratios [GMRs], 1.49 and 1.64, respectively). There was no substantial effect of TDF on raltegravir concentration at 12 h postdose ( C 12 ) in healthy subjects (GMR [TDF plus raltegravir-raltegravir alone], 1.03; 90% confidence interval [CI] , 0.73 to 1.45), while a modest increase (GMR, 1.42; 90% CI, 0.89 to 2.28) was seen in HIV-1-infected patients. Raltegravir had no substantial effect on tenofovir pharmacokinetics: C 24 , AUC, and C max GMRs were 0.87, 0.90, and 0.77, respectively. Coadministration of raltegravir and TDF does not change the pharmacokinetics of either drug to a clinically meaningful degree. Raltegravir and TDF may be coadministered without dose adjustments.

Type of Medium: Online Resource

ISSN: 0066-4804 , 1098-6596

URL: Article

DOI: 10.1128/AAC.00005-08

RVK:

XA 24552

Language: English

Publisher: American Society for Microbiology

Publication Date: 2008

detail.hit.zdb_id: 1496156-8

SSG: 12

SSG: 15,3

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Lack of a Clinically Important Effect of Moderate Hepatic Insufficiency and Severe Renal Insufficiency on Raltegravir Pharmacokinetics

Iwamoto, Marian ; Hanley, William D. ; Petry, Amelia S. ; [et al.]

American Society for Microbiology ; 2009

In: Antimicrobial Agents and Chemotherapy Vol. 53, No. 5 ( 2009-05), p. 1747-1752

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In: Antimicrobial Agents and Chemotherapy, American Society for Microbiology, Vol. 53, No. 5 ( 2009-05), p. 1747-1752

Abstract: Raltegravir is a human immunodeficiency virus type 1 integrase strand transfer inhibitor with potent activity in vitro and in vivo. Raltegravir is primarily cleared by hepatic metabolism via glucuronidation (via UDP glucuronosyltransferase 1A1), with a minor component of elimination occurring via the renal pathway. Since the potential exists for raltegravir to be administered to patients with hepatic or renal insufficiency, two studies were conducted to evaluate the influence of moderate hepatic insufficiency (assessed by using the Child-Pugh criteria) and severe renal insufficiency (creatinine clearance, 〈 30 ml/min/1.73 m 2 ) on the pharmacokinetics of raltegravir. Study I evaluated the pharmacokinetics of 400 mg raltegravir in eight patients with moderate hepatic insufficiency and eight healthy, matched control subjects. Study II evaluated the pharmacokinetics of 400 mg raltegravir in 10 patients with severe renal insufficiency and 10 healthy, matched control subjects. All participants received a single 400-mg dose of raltegravir in the fasted state. In study I, the geometric mean ratios (GMR; mean value for the group with moderate hepatic insufficiency/mean value for the healthy controls) and 90% confidence intervals (CIs) for the area under the concentration-time curve from time zero to infinity (AUC 0-∞ ), the maximum concentration of drug in plasma ( C max ), and the concentration at 12 h ( C 12 ) were 0.86 (90% CI, 0.41, 1.77), 0.63 (90% CI, 0.23, 1.70), and 1.26 (90% CI, 0.65, 2.43), respectively. In study II, the GMRs (mean value for the group with renal insufficiency/mean value for the healthy controls) and 90% CIs for AUC 0-∞ , C max , and C 12 were 0.85 (90% CI, 0.49, 1.49), 0.68 (90% CI, 0.35, 1.32), and 1.28 (90% CI, 0.79, 2.06), respectively. Raltegravir was generally well tolerated by patients with moderate hepatic or severe renal insufficiency, and there was no clinically important effect of moderate hepatic or severe renal insufficiency on the pharmacokinetics of raltegravir. No adjustment in the dose of raltegravir is required for patients with mild or moderate hepatic or renal insufficiency.

Type of Medium: Online Resource

ISSN: 0066-4804 , 1098-6596

URL: Article

DOI: 10.1128/AAC.01194-08

RVK:

XA 24552

Language: English

Publisher: American Society for Microbiology

Publication Date: 2009

detail.hit.zdb_id: 1496156-8

SSG: 12

SSG: 15,3

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3

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Effect of Rifampin, a Potent Inducer of Drug-Metabolizing Enzymes, on the Pharmacokinetics of Raltegravir

Wenning, Larissa A. ; Hanley, William D. ; Brainard, Diana M. ; [et al.]

American Society for Microbiology ; 2009

In: Antimicrobial Agents and Chemotherapy Vol. 53, No. 7 ( 2009-07), p. 2852-2856

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In: Antimicrobial Agents and Chemotherapy, American Society for Microbiology, Vol. 53, No. 7 ( 2009-07), p. 2852-2856

Abstract: Raltegravir is a human immunodeficiency virus type 1 integrase strand transfer inhibitor that is metabolized by glucuronidation via UGT1A1 and may be affected by inducers of UGT1A1, such as rifampin (rifampicin). Two pharmacokinetic studies were performed in healthy subjects: study 1 examined the effect of administration of 600-mg rifampin once daily on the pharmacokinetics of a single dose of 400-mg raltegravir, and study 2 examined the effect of 600-mg rifampin once daily on the pharmacokinetics of 800-mg raltegravir twice daily compared to 400-mg raltegravir twice daily without rifampin. Raltegravir coadministered with rifampin resulted in lower plasma raltegravir concentrations: in study 1, the geometric mean ratios (GMRs) and 90% confidence intervals (90% CIs) for the plasma raltegravir concentration determined 12 h postdose ( C 12 ), area under the concentration-time curve from 0 h to ∞ (AUC 0-∞ ), and maximum concentration of drug in plasma ( C max ) (400-mg raltegravir plus rifampin/400-mg raltegravir) were 0.39 (0.30, 0.51), 0.60 (0.39, 0.91), and 0.62 (0.37, 1.04), respectively. In study 2, the GMRs and 90% CIs for raltegravir C 12 , AUC 0-12 , and C max (800-mg raltegravir plus rifampin/400-mg raltegravir) were 0.47 (0.36, 0.61), 1.27 (0.94, 1.71), and 1.62 (1.12, 2.33), respectively. Doubling the raltegravir dose to 800 mg when coadministered with rifampin therefore compensates for the effect of rifampin on raltegravir exposure (AUC 0-12 ) but does not overcome the effect of rifampin on raltegravir trough concentrations ( C 12 ). Coadministration of rifampin and raltegravir is not contraindicated; however, caution should be used, since raltegravir trough concentrations in the presence of rifampin are likely to be at the lower limit of clinical experience.

Type of Medium: Online Resource

ISSN: 0066-4804 , 1098-6596

URL: Article

DOI: 10.1128/AAC.01468-08

RVK:

XA 24552

Language: English

Publisher: American Society for Microbiology

Publication Date: 2009

detail.hit.zdb_id: 1496156-8

SSG: 12

SSG: 15,3

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4

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Minimal Effects of Ritonavir and Efavirenz on the Pharmacokinetics of Raltegravir

Iwamoto, Marian ; Wenning, Larissa A. ; Petry, Amelia S. ; [et al.]

American Society for Microbiology ; 2008

In: Antimicrobial Agents and Chemotherapy Vol. 52, No. 12 ( 2008-12), p. 4338-4343

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In: Antimicrobial Agents and Chemotherapy, American Society for Microbiology, Vol. 52, No. 12 ( 2008-12), p. 4338-4343

Abstract: Raltegravir is a novel human immunodeficiency virus type 1 (HIV-1) integrase strand transfer inhibitor with potent in vitro activity against HIV-1 (95% inhibitory concentration = 31 nM in 50% human serum). The possible effects of ritonavir and efavirenz on raltegravir pharmacokinetics were separately examined. Two clinical studies of healthy subjects were conducted: for ritonavir plus raltegravir, period 1, 400 mg raltegravir; period 2, 100 mg ritonavir every 12 h for 16 days with 400 mg raltegravir on day 14; for efavirenz plus raltegravir, period 1, 400 mg raltegravir; period 2, 600 mg efavirenz once daily for 14 days with 400 mg raltegravir on day 12. In the presence of ritonavir, raltegravir pharmacokinetics were weakly affected: the plasma concentration at 12 h ( C 12 h ) geometric mean ratio (GMR) (90% confidence interval [CI]) was 0.99 (0.70, 1.40), area under the concentration-time curve from zero to infinity (AUC 0 - ∞ ) was 0.84 (0.70, 1.01), and maximum concentration of drug in serum ( C max ) was 0.76 (0.55, 1.04). In the presence of efavirenz, raltegravir pharmacokinetics were moderately to weakly reduced: C 12 h GMR (90% CI) was 0.79 (0.49, 1.28); AUC 0- ∞ was 0.64 (0.52, 0.80); and C max was 0.64 (0.41, 0.98). There were no substantial differences in the time to maximum concentration of drug in plasma or the half-life. Plasma concentrations of raltegravir were not substantially affected by ritonavir. Though plasma concentrations of raltegravir were moderately to weakly reduced by efavirenz, the degree of this reduction was not clinically meaningful. No dose adjustment is required for raltegravir with coadministration with ritonavir or efavirenz.

Type of Medium: Online Resource

ISSN: 0066-4804 , 1098-6596

URL: Article

DOI: 10.1128/AAC.01543-07

RVK:

XA 24552

Language: English

Publisher: American Society for Microbiology

Publication Date: 2008

detail.hit.zdb_id: 1496156-8

SSG: 12

SSG: 15,3

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5

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A Cyclooxygenase-2 Homologue Encoded by Rhesus Cytomegalovirus Is a Determinant for Endothelial Cell Tropism

Rue, Cary A. ; Jarvis, Michael A. ; Knoche, Amber J. ; [et al.]

American Society for Microbiology ; 2004

In: Journal of Virology Vol. 78, No. 22 ( 2004-11-15), p. 12529-12536

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In: Journal of Virology, American Society for Microbiology, Vol. 78, No. 22 ( 2004-11-15), p. 12529-12536

Abstract: Cyclooxygenase-2 (COX-2) is a cellular enzyme in the eicosanoid synthetic pathway that mediates the synthesis of prostaglandins from arachidonic acid. The eicosanoids function as critical regulators of a number of cellular processes, including the acute and chronic inflammatory response, hemostasis, and the innate immune response. Human cytomegalovirus (HCMV), which does not encode a viral COX-2 isoform, has been shown to induce cellular COX-2 expression. Importantly, although the precise role of COX-2 in CMV replication is unknown, COX-2 induction was shown to be critical for normal HCMV replication. In an earlier study, we identified an open reading frame (Rh10) within the rhesus cytomegalovirus (RhCMV) genome that encoded a putative protein (designated vCOX-2) with high homology to cellular COX-2. In the current study, we show that vCOX-2 is expressed with early-gene kinetics during RhCMV infection, resulting in production of a 70-kDa protein. Consistent with the expression of a viral COX-2 isoform, cellular COX-2 expression was not induced during RhCMV infection. Finally, analysis of growth of recombinant RhCMV with vCOX-2 deleted identified vCOX-2 as a critical determinant for replication in endothelial cells.

Type of Medium: Online Resource

ISSN: 0022-538X , 1098-5514

URL: Article

DOI: 10.1128/JVI.78.22.12529-12536.2004

Language: English

Publisher: American Society for Microbiology

Publication Date: 2004

detail.hit.zdb_id: 1495529-5

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Genomic Deletion Marking an Emerging Subclone of Francisella tularensis subsp. holarctica in France and the Iberian Peninsula

Dempsey, M. P. ; Dobson, M. ; Zhang, C. ; [et al.]

American Society for Microbiology ; 2007

In: Applied and Environmental Microbiology Vol. 73, No. 22 ( 2007-11-15), p. 7465-7470

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In: Applied and Environmental Microbiology, American Society for Microbiology, Vol. 73, No. 22 ( 2007-11-15), p. 7465-7470

Abstract: Francisella tularensis subsp. holarctica is widely disseminated in North America and the boreal and temperate regions of the Eurasian continent. Comparative genomic analyses identified a 1.59-kb genomic deletion specific to F. tularensis subsp. holarctica isolates from Spain and France. Phylogenetic analysis of strains carrying this deletion by multiple-locus variable-number tandem repeat analysis showed that the strains comprise a highly related set of genotypes, implying that these strains were recently introduced or recently emerged by clonal expansion in France and the Iberian Peninsula.

Type of Medium: Online Resource

ISSN: 0099-2240 , 1098-5336

URL: Article

DOI: 10.1128/AEM.00646-07

RVK:

WA 15000

Language: English

Publisher: American Society for Microbiology

Publication Date: 2007

detail.hit.zdb_id: 223011-2

detail.hit.zdb_id: 1478346-0

SSG: 12

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7

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SARS-CoV-2 Spike Protein Stabilized in the Closed State Induces Potent Neutralizing Responses

Carnell, George W. ; Ciazynska, Katarzyna A. ; Wells, David A. ; [et al.]

American Society for Microbiology ; 2021

In: Journal of Virology Vol. 95, No. 15 ( 2021-07-12)

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In: Journal of Virology, American Society for Microbiology, Vol. 95, No. 15 ( 2021-07-12)

Abstract: The majority of SARS-CoV-2 vaccines in use or advanced development are based on the viral spike protein (S) as their immunogen. S is present on virions as prefusion trimers in which the receptor binding domain (RBD) is stochastically open or closed. Neutralizing antibodies have been described against both open and closed conformations. The long-term success of vaccination strategies depends upon inducing antibodies that provide long-lasting broad immunity against evolving SARS-CoV-2 strains. Here, we have assessed the results of immunization in a mouse model using an S protein trimer stabilized in the closed state to prevent full exposure of the receptor binding site and therefore interaction with the receptor. We compared this with other modified S protein constructs, including representatives used in current vaccines. We found that all trimeric S proteins induced a T cell response and long-lived, strongly neutralizing antibody responses against 2019 SARS-CoV-2 and variants of concern P.1 and B.1.351. Notably, the protein binding properties of sera induced by the closed spike differed from those induced by standard S protein constructs. Closed S proteins induced more potent neutralizing responses than expected based on the degree to which they inhibit interactions between the RBD and ACE2. These observations suggest that closed spikes recruit different, but equally potent, immune responses than open spikes and that this is likely to include neutralizing antibodies against conformational epitopes present in the closed conformation. We suggest that closed spikes, together with their improved stability and storage properties, may be a valuable component of refined, next-generation vaccines. IMPORTANCE Vaccines in use against SARS-CoV-2 induce immune responses against the spike protein. There is intense interest in whether the antibody response induced by vaccines will be robust against new variants, as well as in next-generation vaccines for use in previously infected or immunized individuals. We assessed the use as an immunogen of a spike protein engineered to be conformationally stabilized in the closed state where the receptor binding site is occluded. Despite occlusion of the receptor binding site, the spike induces potently neutralizing sera against multiple SARS-CoV-2 variants. Antibodies are raised against a different pattern of epitopes to those induced by other spike constructs, preferring conformational epitopes present in the closed conformation. Closed spikes, or mRNA vaccines based on their sequence, can be a valuable component of next-generation vaccines.

Type of Medium: Online Resource

ISSN: 0022-538X , 1098-5514

URL: Article

DOI: 10.1128/JVI.00203-21

Language: English

Publisher: American Society for Microbiology

Publication Date: 2021

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8

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Structure of Campylobacter jejuni Lipopolysaccharides Determines Antiganglioside Specificity and Clinical Features of Guillain-Barré and Miller Fisher Patients

Ang, C. W. ; Laman, J. D. ; Willison, H. J. ; [et al.]

American Society for Microbiology ; 2002

In: Infection and Immunity Vol. 70, No. 3 ( 2002-03), p. 1202-1208

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In: Infection and Immunity, American Society for Microbiology, Vol. 70, No. 3 ( 2002-03), p. 1202-1208

Abstract: Ganglioside mimicry in the lipopolysaccharide (LPS) fraction of Campylobacter jejuni isolated from Guillain-Barré syndrome (GBS) and Miller Fisher syndrome (MFS) patients was compared with isolates from patients with an uncomplicated enteritis. The antibody response to C. jejuni LPS and gangliosides in neuropathy patients and controls was compared as well. LPS from GBS and MFS-associated isolates more frequently contained ganglioside-like epitopes compared to control isolates. Almost all neuropathy patients showed a strong antibody response against LPS and multiple gangliosides in contrast to enteritis patients. Isolates from GBS patients more frequently had a GM1-like epitope than isolates from MFS patients. GQ1b-like epitopes were present in all MFS-associated isolates and was associated with anti-GQ1b antibody reactivity and the presence of oculomotor symptoms. These results demonstrate that the expression of ganglioside mimics is a risk factor for the development of post- Campylobacter neuropathy. This study provides additional evidence for the hypothesis that the LPS fraction determines the antiganglioside specificity and clinical features in post- Campylobacter neuropathy patients.

Type of Medium: Online Resource

ISSN: 0019-9567 , 1098-5522

URL: Article

DOI: 10.1128/IAI.70.3.1202-1208.2002

RVK:

XA 10000

Language: English

Publisher: American Society for Microbiology

Publication Date: 2002

detail.hit.zdb_id: 1483247-1

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9

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Effect of Tipranavir-Ritonavir on Pharmacokinetics of Raltegravir

Hanley, William D. ; Wenning, Larissa A. ; Moreau, Allison ; [et al.]

American Society for Microbiology ; 2009

In: Antimicrobial Agents and Chemotherapy Vol. 53, No. 7 ( 2009-07), p. 2752-2755

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In: Antimicrobial Agents and Chemotherapy, American Society for Microbiology, Vol. 53, No. 7 ( 2009-07), p. 2752-2755

Abstract: Raltegravir (RAL) is a novel and potent human immunodeficiency virus type 1 integrase inhibitor that is predominantly metabolized via glucuronidation. The protease inhibitor combination tipranavir (TPV) at 500 mg and ritonavir (RTV) at 200 mg (TPV-RTV) has inhibitory and inductive effects on metabolic enzymes, which includes the potential to induce glucuronosyltransferase. Because RAL may be coadministered with TPV-RTV, there is the potential for the induction of RAL metabolism. Consequently, we assessed the effect of TPV-RTV on the pharmacokinetics of RAL and the safety and tolerability of this combination. Eighteen healthy adults were enrolled in this open-label study. The participants received RAL at 400 mg twice daily for 4 days (period 1) and TPV-RTV twice daily for 7 days (period 2), followed immediately by 400 mg RAL with TPV-RTV twice daily for 4 days (period 3). Under steady-state conditions, the RAL concentration at 12 h ( C 12 ) was decreased when RAL was administered with TPV-RTV (geometric mean ratio [GMR], 0.45; 90% confidence interval [CI] 0.31, 0.66; P = 0.0021); however, the area under the concentration-time curve from time zero to 12 h (GMR, 0.76; 90% CI, 0.49, 1.19; P = 0.2997) and the maximum concentration in serum (GMR, 0.82; 90% CI, 0.46, 1.46; P = 0.5506) were not substantially affected. There were no serious adverse experiences or discontinuations due to study drug-related adverse experiences, and RAL coadministered with TPV-RTV was generally well tolerated. Although the RAL C 12 was decreased with TPV-RTV in this study, favorable efficacy data collected in phase III studies substantiate that TPV-RTV may be coadministered with RAL without dose adjustment.

Type of Medium: Online Resource

ISSN: 0066-4804 , 1098-6596

URL: Article

DOI: 10.1128/AAC.01486-08

RVK:

XA 24552

Language: English

Publisher: American Society for Microbiology

Publication Date: 2009

detail.hit.zdb_id: 1496156-8

SSG: 12

SSG: 15,3

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10

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Genome Sequences of Four Subcluster L2 Mycobacterium Phages, Finemlucis, Miley16, Wilder, and Zakai

Herren, Christopher D. ; Peister, Alexandra ; Breton, Timothy S. ; [et al.]

American Society for Microbiology ; 2017

In: Genome Announcements Vol. 5, No. 46 ( 2017-11-16)

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In: Genome Announcements, American Society for Microbiology, Vol. 5, No. 46 ( 2017-11-16)

Abstract: Four subcluster L2 mycobacteriophages, Finemlucis, Miley16, Wilder, and Zakai, that infect Mycobacterium smegmatis mc 2 155 were isolated. The four phages are closely related to each other and code for 12 to 14 tRNAs and 130 to 132 putative protein-coding genes, including tyrosine integrases, cro , immunity repressors, and excise genes involved in the establishment of lysogeny.

Type of Medium: Online Resource

ISSN: 2169-8287

URL: Article

DOI: 10.1128/genomeA.01233-17

Language: English

Publisher: American Society for Microbiology

Publication Date: 2017

detail.hit.zdb_id: 2968655-6

detail.hit.zdb_id: 2704277-7

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