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Featured researches published by Irja Lutsar.


Clinical Infectious Diseases | 1998

Antibiotic pharmacodynamics in cerebrospinal fluid

Irja Lutsar; George H. McCracken; Ian R. Friedland

The CSF half-lives of lipophilic agents, such as quinolones, are similar to those in serum and peak concentrations in CSF are achieved relatively quickly. In contrast, the pharmacokinetics of hydrophilic agents (beta-lactams and vancomycin) in CSF often differ from those in serum. In particular, the half-lives of these agents in CSF tend to be extended, and the time to achieve peak concentrations in CSF is delayed. Hydrophilic antibiotics, such as beta-lactams, penetrate poorly through the BBB, but CSF penetration is significantly increased in the presence of inflammation. In contrast, lipophilic antibiotics, such as quinolones, enter the CSF more efficiently and their penetration is not inflammation dependent. The pharmacodynamic properties of antibiotics in CSF are generally similar to those in other body sites; beta-lactam agents and vancomycin are time-dependent, whereas the quinolones and aminoglycosides are concentration-dependent. However, a notable difference from infections in other sites is that quinolones have a short PAE in CSF and need to continually exceed the MBC for maximal effectiveness. Thus, in CSF, quinolones demonstrate features of both concentration-dependency and time-dependency, evidence that the AUC/MBC is an important predictor of effectiveness. With the exception of quinolones, many antibiotics appear to have prolonged sub-MIC effects and longer half-lives in CSF than in serum, suggesting that dosing intervals longer than those used traditionally would be effective in meningitis. However, this requires clinical verification.


Apmis | 2000

Buffy coat PCR for diagnosis of experimental pneumococcal pneumonia

Winston Ng; Kurt Olsen; Irja Lutsar; Loretta Wubbel; Faryal Ghaffar; Hasan S. Jafri; George H. McCracken; I. R. Friedland

An immunocompetent murine model of pneumococcal pneumonia and bacteremia was used to evaluate a PCR assay based on amplification of the pneumolysin gene. Mice were treated with trovafioxacin to determine the decline in sensitivity of PCR as lung bacterial concentrations decreased and blood cultures became sterile. Forty‐three mice were studied for up to 120 h after start of antibiotic treatment. PCR of buffy coat specimens was more sensitive than PCR of plasma. Only 21% of animals had a positive blood culture, whereas 77% of PCR buffy coat assays were positive. After 48 h of therapy all blood culture specimens were sterile, whereas buffy coat PCR was positive in 57.8% of specimens. PCR of buffy coat specimens was negative in all mice colonized nasally with Streptococcus pneumoniae and in rabbits with Escherichia coli bacteremia. Our results demonstrate that our PCR technique using buffy coat specimens is highly specific for invasive pneumococcal disease and remains positive in the majority of animals for at least 48 h after start of antibiotic therapy.


Antimicrobial Agents and Chemotherapy | 1999

Pharmacodynamics of vancomycin for the treatment of experimental penicillin- and cephalosporin-resistant pneumococcal meningitis.

Amina Ahmed; Hasan S. Jafri; Irja Lutsar; Cynthia C. McCoig; Mónica Trujillo; Loretta Wubbel; Sharon Shelton; George H. McCracken


Antimicrobial Agents and Chemotherapy | 1998

Pharmacodynamics of Gatifloxacin in Cerebrospinal Fluid in Experimental Cephalosporin-Resistant Pneumococcal Meningitis

Irja Lutsar; Ian R. Friedland; Loretta Wubbel; Cynthia C. McCoig; Hasan S. Jafri; Winston Ng; Faryal Ghaffar; George H. McCracken


Antimicrobial Agents and Chemotherapy | 1997

Pharmacodynamics and bactericidal activity of ceftriaxone therapy in experimental cephalosporin-resistant pneumococcal meningitis.

Irja Lutsar; Amina Ahmed; Ian R. Friedland; Mónica Trujillo; Loretta Wubbel; Kurt Olsen; George H. McCracken


Journal of Antimicrobial Chemotherapy | 2003

Factors influencing the anti-inflammatory effect of dexamethasone therapy in experimental pneumococcal meningitis

Irja Lutsar; I. R. Friedland; Hasan S. Jafri; Loretta Wubbel; Amina Ahmed; Mónica Trujillo; Cynthia C. McCoig; George H. McCracken


Journal of Antimicrobial Chemotherapy | 1999

Pharmacodynamics of trovafloxacin in experimental pneumococcal meningitis : basis for dosage selection in children with meningitis

Cynthia C. McCoig; Loretta Wubbel; Hasan S. Jafri; Irja Lutsar; Rafael Bastero; Kurt Olsen; Sharon Shelton; Ian R. Friedland; George H. McCracken


Antimicrobial Agents and Chemotherapy | 1999

Efficacy of Gatifloxacin in Experimental Escherichia coli Meningitis

Irja Lutsar; Ian R. Friedland; Hasan S. Jafri; Loretta Wubbel; Winston Ng; Faryal Ghaffar; George H. McCracken


Journal of Antimicrobial Chemotherapy | 1999

Pharmacodynamics of trovafloxacin in a mouse model of cephalosporin-resistant Streptococcus pneumoniae pneumonia

Winston Ng; Irja Lutsar; Loretta Wubbel; Faryal Ghaffar; Hasan S. Jafri; George H. McCracken; Ian R. Friedland


Annales Nestle | 1997

Pathogenesis of bacterial meningitis

Irja Lutsar; I. R. Friedland; G H Jr McCracken

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George H. McCracken

University of Texas Southwestern Medical Center

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Loretta Wubbel

University of Texas Southwestern Medical Center

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Ian R. Friedland

University of Texas Southwestern Medical Center

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Cynthia C. McCoig

University of Texas Southwestern Medical Center

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Kurt Olsen

University of Texas Southwestern Medical Center

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Amina Ahmed

Carolinas Medical Center

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Faryal Ghaffar

University of Texas Southwestern Medical Center

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I. R. Friedland

University of Texas Southwestern Medical Center

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Mónica Trujillo

University of Texas Southwestern Medical Center

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