Inflammation and Drug Idiosyncrasy—Is There a Connection?

Roth, Robert A.; Luyendyk, James P.; Maddox, Jane F.; Ganey, Patricia E.

doi:10.1124/jpet.102.041624

Cited by 120 publications

(65 citation statements)

References 43 publications

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“…56 On the other hand, inflammatory stress might sensitize the liver to xenobiotics-induced injury. 57 Hence, we might be able to suggest that inflammatory stress occurring during antimalarial drug therapy might participate in antimalarial drugs-induced liver injury in patients and enhance the sensitivity to antimalarial drugs. Investigating the effect of inflammation on antimalarial drugs hepatotoxicity in a broader time frame will enhance our understanding of the mechanism of toxicity and the pathological pattern of liver injury induced by…”

Section: Discussionmentioning

confidence: 99%

Concurrent Inflammation Augments Antimalarial Drugs-Induced Liver Injury in Rats

et al. 2016

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Section: Discussionmentioning

confidence: 99%

Concurrent Inflammation Augments Antimalarial Drugs-Induced Liver Injury in Rats

et al. 2016

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“…Roth found that cotreatment of animals with lipopolysaccaride (LPS) and drugs such as ranitidine causes immediate hepatic damage (42). He has proposed that we are commonly exposed to inflammagens such as LPS, and it is the combination of drug and inflammagen that leads to hepatic damage.…”

Section: Inflammagen Hypothesismentioning

confidence: 99%

Idiosyncratic Drug Reactions: Past, Present, and Future

Uetrecht

2007

Chem. Res. Toxicol.

237

190

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Although the major working hypothesis for the mechanism of idiosyncratic drug reactions (IDRs), the hapten hypothesis, has not changed since 1987, several hypotheses have been added, for example, the danger hypothesis and the pharmaceutical interaction hypothesis. Genetic studies have found that several IDRs are linked to specific HLA genes, providing additional evidence that they are immune-mediated. Evidence that most IDRs are caused by reactive metabolites has led pharmaceutical companies to avoid drug candidates that form significant amounts of reactive metabolites; however, at least one IDR, ximelagatran-induced liver toxicity, does not appear to be caused by a reactive metabolite. It is possible that there are biomarkers such as those related to cell stress that would predict that a drug candidate would cause a significant incidence of IDRs; however, there has been no systematic study of the changes in gene expression induced by drugs known to cause IDRs. A major impediment to the study of the mechanisms of IDRs is the paucity of valid animal models, and if we had a better mechanistic understanding, it should be easier to develop such models. There is growing evidence that these adverse reactions are more varied and complex than previously recognized, and it is unlikely that a quick fix will be achieved. However, IDRs are an important cause of patient morbidity and mortality and markedly increase the uncertainty of drug development; therefore, continued basic research in this area is essential.

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“…Despite the lesser attention to the gut, an estimated 16,500 or more people die annually in the U.S. from complications associated with long term NSAID use (e.g., intestinal ulceration, bleeding, perforations, and strictures (Hirschowitz, 1994;Laney et al, 1994)), especially among elderly, arthritic patients (Wolfe et al, 1999). Moreover, an appreciated aspect of persistent low-level LPS exposure due to NSAID use is elevated risk of drug-induced idiosyncratic hepatic injuries (Roth et al, 2003), atherosclerosis (Blake and Ridker 2001;Shishehbor and Bhatt, 2004) and alcohol-induced hepatic injury (Mathurin et al, 2000;Schafer et al, 2002). To this point, pretreatment of rats with a mild APR inducing dose of LPS followed by a dose of ranitidine that in naïve animals is only mildly hepatotoxic synergistically increases hepatic injury (Luyendyk et al, 2003).…”

Section: Drug Signatures For the Acute Phase Responsementioning

confidence: 99%

NSAID-Induced Acute Phase Response is Due to Increased Intestinal Permeability and Characterized by Early and Consistent Alterations in Hepatic Gene Expression

Tugendreich

Pearson

Sagartz³

et al. 2006

Toxicol Pathol

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Toxicogenomics using a reference database can provide a better understanding and prediction of toxicity, largely by creating biomarkers that tie gene expression to actual pathology events. During the course of building a toxicogenomic database, an observation was made that a number of non-steroidal anti-inflammatory compounds (NSAIDs) at supra-pharmacologic doses induced an acute phase response (APR) and displayed hepatic gene expression patterns similar to that of intravenous lipopolysaccharide (LPS). Since NSAIDs are known to cause injury along the gastrointestinal tract, it has been suggested that NSAIDs increase intestinal permeability, allowing LPS and/or bacteria into the systemic circulation and stimulating an APR detectable in the liver. A short term study was subsequently conducted examining the effects of aspirin, indomethacin, ibuprofen, and rofecoxib to rats and a variety of endpoints were examined that included serum levels of inflammatory cytokines, histologic evaluation, and hepatic gene expression. Both indomethacin and ibuprofen injured the gastrointestinal tract, induced an APR, and increased serum levels of LPS, while rofecoxib and aspirin did not affect the GI tract or induce an APR. In treatments that eventually showed a systemic inflammatory response, hepatic expression of many inflammatory genes was noted as early as 6 hours after treatment well before alterations in traditional clinical pathology markers were detected. This finding led to the creation of a hepatic gene expression biomarker of APR that was effectively shown to be an early identifier of imminent inflammatory injury. In terms of the relative gastrointestinal safety and the NSAIDs studied, an important safety distinction can be made between the presumptive efficacious dose and the APR-inducing dose for indomethacin (1-2-fold), ibuprofen (5-fold), and rofecoxib (∼250-fold). Our data support the notion that NSAID-induced intestinal injury results in leakage of commensural bacteria and/or LPS into the circulation, provoking a systemic inflammatory response and that hepatic gene expression-based biomarkers can be used as early and sensitive biomarkers of APR onset.[The table referenced in this paper is not printed in this issue of Toxicologic Pathology. It is available as a downloadable text file in the online edition of Toxicologic Pathology, 34(2). In order to access the full article online, you must have either an individual subscription or a member subscription accessed through www.toxpath.org.]

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Inflammation and Drug Idiosyncrasy—Is There a Connection?

Cited by 120 publications

References 43 publications

Concurrent Inflammation Augments Antimalarial Drugs-Induced Liver Injury in Rats

Concurrent Inflammation Augments Antimalarial Drugs-Induced Liver Injury in Rats

Idiosyncratic Drug Reactions: Past, Present, and Future

NSAID-Induced Acute Phase Response is Due to Increased Intestinal Permeability and Characterized by Early and Consistent Alterations in Hepatic Gene Expression

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