Functionally Relevant Residues of Cdr1p: A Multidrug ABC Transporter of Human Pathogenic <i>Candida albicans</i>

<table class="table-group" id="tab1"><tr><td><table class="table"><tr><td class="thead-hr" colspan="3"><hr/></td></tr><tr><td align="left">Substrates</td><td align="left">Fluconazole, ketoconazole, voriconazole, Itraconazole, miconazole, lipids, steroids, R6G, cycloheximide, rhodamine 123, cerulenin, trifluoperazine, nigericin, tamoxifen, verapamil, cycloheximide, propanil, diuron, linuron, disulfiram, anisomycin, doxorubicin, 4-nitroquinoline –N-oxide, benomyl, yohimbine HCl, quinidine, etoposide, chlorobromuron, vinblastine, tamoxifen, gefitinib, fluphenazine, topotecan, daunorubicin, DM-11, AT-12 niguldipine, dexamethasone, berberine, terbinafine, tritylmazole</td><td align="center">[<a href="/journals/jaa/2011/531412/#B7">7</a>, <a href="/journals/jaa/2011/531412/#B53">53</a>] </td></tr><tr><td align="center" colspan="3"><hr/></td></tr><tr><td align="left">Inhibitors/modulators</td><td align="left">Milbemycins, enniatin, FK506, FK520, unnarmicins, curcumin, disulfiram</td><td align="center">[<a href="/journals/jaa/2011/531412/#B54">54</a>–<a href="/journals/jaa/2011/531412/#B57">57</a>]</td></tr><tr class="table-tr"><td colspan="3"><hr class="tbody-hr"/></td></tr></table></td></tr></table>

Substrates and inhibitors of CaCDR1 substrates.

Journal of Amino Acids

tab1

Table 1

Table 1: Functionally Relevant Residues of Cdr1p: A Multidrug ABC Transporter of Human Pathogenic <i>Candida albicans</i> 

Journal of Amino Acids

Functionally Relevant Residues of Cdr1p: A Multidrug ABC Transporter of Human Pathogenic Candida albicans

Table 1