Pharmacology and toxicology of mycophenolate in organ transplant recipients: an update

Staatz, C. E.; Tett, S. E.

doi:10.1007/s00204-014-1247-1

Cited by 165 publications

(189 citation statements)

References 244 publications

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“…There are other presumed mechanisms for immunomodulator effects of this agent. MPA can inhibit monocyte chemoattraction, destroy activated lymphocytes and induce immune tolerance by affecting regulatory Tcell/helper Tcell balance [59] .…”

Section: Maintenance Immunosuppressionmentioning

confidence: 99%

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Review on immunosuppression in liver transplantation

Moini

Schilsky

Tichy

2015

WJH

193

160

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Section: Maintenance Immunosuppressionmentioning

confidence: 99%

“…Higher doses may be required but are not usually recommended. There are also reports on the non-linear pharmacokinetics of MPA with decreasing the bioavailability of drug by increasing the dose [59] . The major adverse side effects of MPA are hematologic and gastrointestinal (GI).…”

Section: Maintenance Immunosuppressionmentioning

confidence: 99%

Review on immunosuppression in liver transplantation

Moini

Schilsky

Tichy

2015

WJH

193

160

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“…As with other immunosuppressive agents, MMF has a significant adverse effect profile, including diarrhea, cytopenias (anemia and leukopenia) and increased risk of bacterial, pneumocystis and CMV infections [42]. MMF is used as part of the standard immunosuppressive regimen along with calcineurin inhibitors and steroids as an antiproliferative agent [33].…”

Section: Mycophenolatemofetil (Mmf)mentioning

confidence: 99%

Drugs for the Prevention and Treatment of Cardiac Allograft Vasculopathy

Gupta¹

2014

Cardiol Pharmacol

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Cardiac allograft vasculopathy (CAV) of heart transplants is responsible for up to one-third of deaths at 5 years following cardiac transplantation. Risk factors for CAV include both traditional risk factors and immune factors. Drugs used for prevention and treatment of CAV include statins, calcium channel blockers and immunosuppressive agents. This review discusses the currently available drugs for CAV, the evidence behind their use, and future targets of therapy.

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“…One kind of inhibitor, including 6-chloropurine riboside ribavirin and mizoribine, targets the binding pocket of the natural substrate, inosine monophosphate (IMP). Another kind of inhibitor (e.g., mycophenolic acid and thiazole-4-carboxamide adenine dinucleotide) targets the site of the cofactor, NAD + / NADH, which usually leads to low selectivity or even side effects in clinical trials, such as diarrhea and leukopenia (10,11). Moreover, a third ligand has been speculated to bind to a possible site far from the IMP and NAD + pockets as an allosteric inhibitor.…”

mentioning

confidence: 99%

Highly selective inhibition of IMPDH2 provides the basis of antineuroinflammation therapy

Liao

Song

Wang

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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Inosine monophosphate dehydrogenase (IMPDH) of human is an attractive target for immunosuppressive agents. Currently, smallmolecule inhibitors do not show good selectivity for different IMPDH isoforms (IMPDH1 and IMPDH2), resulting in some adverse effects, which limit their use. Herein, we used a small-molecule probe specifically targeting IMPDH2 and identified Cysteine residue 140 (Cys140) as a selective druggable site. On covalently binding to Cys140, the probe exerts an allosteric regulation to block the catalytic pocket of IMPDH2 and further induces IMPDH2 inactivation, leading to an effective suppression of neuroinflammatory responses. However, the probe does not covalently bind to IMPDH1. Taken together, our study shows Cys140 as a druggable site for selectively inhibiting IMPDH2, which provides great potential for development of therapy agents for autoimmune and neuroinflammatory diseases with less unfavorable tolerability profile.nosine monophosphate dehydrogenase (IMPDH) is a major rate-limiting enzyme involved in guanosine and deoxyguanosine biosynthesis and widely expressed in immunocytes (1). There exist two IMPDH isoforms (IMPDH1 and IMPDH2), which are encoded by distinct genes (2, 3). Many inflammation-relevant diseases have been specially characterized by the high expression of isoform II of IMPDH (IMPDH2) in rapidly proliferating immunocytes, rather than the "housekeeping" type I isoform (IMPDH1) in normal human leukocytes and lymphocytes (4, 5). Therefore, selective targeting of IMPDH2 with small molecules is an attractive topic for development of antiinflammation agents with low side effects.Both IMPDH isoforms contain two major domains: the catalytic domain for substrate interaction and the Bateman domain, which is not required for catalytic activity but exerts an important allosteric regulation effect on IMPDH activity by communicating with the catalytic domain (6, 7). By influencing catalytic domain activity, the Bateman domain can regulate IMPDH function and further blocks the downstream-of-inflammation signaling pathways (8, 9). Currently, IMPDH inhibitors are divided into two major categories. One kind of inhibitor, including 6-chloropurine riboside ribavirin and mizoribine, targets the binding pocket of the natural substrate, inosine monophosphate (IMP). Another kind of inhibitor (e.g., mycophenolic acid and thiazole-4-carboxamide adenine dinucleotide) targets the site of the cofactor, NAD + / NADH, which usually leads to low selectivity or even side effects in clinical trials, such as diarrhea and leukopenia (10, 11). Moreover, a third ligand has been speculated to bind to a possible site far from the IMP and NAD + pockets as an allosteric inhibitor. However, an allosteric site for designing selective IMPDH2 inhibitors has been largely unexplored.Natural small molecules remain promising drug sources (12, 13). In the present study, we report that a natural small-molecule probe, sappanone A (SA, Fig.1A), demonstrated significant inhibitory effects on neuroinflammation by directly targetin...

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Pharmacology and toxicology of mycophenolate in organ transplant recipients: an update

Cited by 165 publications

References 244 publications

Review on immunosuppression in liver transplantation

Review on immunosuppression in liver transplantation

Drugs for the Prevention and Treatment of Cardiac Allograft Vasculopathy

Highly selective inhibition of IMPDH2 provides the basis of antineuroinflammation therapy

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