2012
DOI: 10.1128/aac.01267-12
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Immunocytochemistry for Vancomycin Using a Monoclonal Antibody That Reveals Accumulation of the Drug in Rat Kidney and Liver

Abstract: bWe prepared monoclonal antibodies against N-(␥-maleimidobutyryloxy)succinimide-conjugated vancomycin (VM). The monoclonal antibody was specific for conjugated or free VM. The monoclonal antibody enabled us to develop an immunocytochemical method for detecting the uptake of VM in the rat kidney and liver. Three hours after a single intravenous (i.v.) injection of VM at the therapeutic dose, the immunocytochemistry revealed that VM accumulated in large amounts in both the S1 and S2 segments and in much smaller … Show more

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Cited by 30 publications
(47 citation statements)
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“…Vancomycin is actively transported across the basolateral membrane into proximal tubule cells via the organic cation transporter system 55, 56 (Figure 3). The visualization of large amounts of vancomycin at the brush border also points to either ongoing secretion or reabsorption of the drug at the apical side (i.e., from the urine) 57, 58 . In support, recent preclinical data have demonstrated vancomycin transport across the brush border membrane by apical endocytosis via dehydropeptidase 59 and megalin 60 and vancomycin‐mediated inhibition of the expression and function of P‐glycoprotein, an efflux transporter 61 .…”
Section: Mechanisms Of Vikimentioning
confidence: 75%
See 1 more Smart Citation
“…Vancomycin is actively transported across the basolateral membrane into proximal tubule cells via the organic cation transporter system 55, 56 (Figure 3). The visualization of large amounts of vancomycin at the brush border also points to either ongoing secretion or reabsorption of the drug at the apical side (i.e., from the urine) 57, 58 . In support, recent preclinical data have demonstrated vancomycin transport across the brush border membrane by apical endocytosis via dehydropeptidase 59 and megalin 60 and vancomycin‐mediated inhibition of the expression and function of P‐glycoprotein, an efflux transporter 61 .…”
Section: Mechanisms Of Vikimentioning
confidence: 75%
“…Endosomes fuse with lysosomes, which leads to accumulation of vancomycin in lysosomes. In 1992, vancomycin accumulation in the lysosomes of proximal tubule cells was first visualized using immunoelectron microscopy 58 ; and later confirmed by another group 57 . This accumulation of vancomycin in lysosomes may trigger a detrimental autophagy process.…”
Section: Mechanisms Of Vikimentioning
confidence: 93%
“…In these patients, loading doses of 15–25 mg/kg should be based on actual body weight [71]. Because vancomycin accumulates in the tissues [58, 72], consideration should be given to empirically reducing the maintenance dose, particularly in patients who are critically ill [9, 29, 68, 70]. Additionally, even though vancomycin is 50% bound to serum albumin [10], clinically dosing vancomycin according to serum albumin concentrations is not performed.…”
Section: Practical Applicationsmentioning
confidence: 99%
“…Complicating the understanding, clinical dosing results in homogenous exposure profiles, and patient comorbidities impact the ability to identify the true toxicodynamic relationship. Thus, there is a renewed interest in controlled laboratory experiments (e.g., animal models) to best discern mechanistic links between pharmacokinetic (PK) exposures and toxicodynamic outcomes . Additionally, there are limited data on toxicity of vancomycin in utero , and these analyses were performed before sensitive biomarkers of vancomycin toxicity were available for study.…”
mentioning
confidence: 99%
“…Thus, there is a renewed interest in controlled laboratory experiments (e.g., animal models) to best discern mechanistic links between pharmacokinetic (PK) exposures and toxicodynamic outcomes. [8][9][10][11][12] Additionally, there are limited data on toxicity of vancomycin in utero, 13 and these analyses were performed before sensitive biomarkers of vancomycin toxicity were available for study.…”
mentioning
confidence: 99%