Kinetic and Structural Analysis for Potent Antifolate Inhibition of Pneumocystis jirovecii, Pneumocystis carinii, and Human Dihydrofolate Reductases and Their Active-Site Variants

Cody, Vivian; Pace, Jim; Queener, Sherry F.; Adair, Ona O.; Gangjee, Aleem

doi:10.1128/aac.00172-13

Cited by 15 publications

(17 citation statements)

References 28 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…The homology data for the pjDHFR complex with OAAG324 ( Fig. 1) and NADPH reveals that this compound is displaced above the plane of the pyrido [2,3-d]pyrimidine ring compared to the crystal structure data (15). Similar modeling of pjDHFR with TMP and NADPH is consistent with the crystal structure of pcDHFR with TMP and NADPH (18).…”

Section: Fig 1 Schematics Of the Pjdhfr Inhibitors Trimethoprim And Osupporting

confidence: 67%

“…1) to assess whether resistance to one antifolate was likely to confer resistance to the class. OAAG324 was chosen as the experimental antifolate because it differed significantly in structure from trimethoprim (14) and the compound was already known to be longer and more flexible than trimethoprim, such that the dichlorophenyl ring can adopt alternate conformations within the active site (15).…”

Section: Fig 1 Schematics Of the Pjdhfr Inhibitors Trimethoprim And Omentioning

confidence: 99%

“…The deduced structure of P. jirovecii DHFR was calculated by homology modeling to the crystal structure of the P. carinii DHFR ternary complex with methotrexate and NADPH (15)(16)(17). The homology data for the pjDHFR complex with OAAG324 ( Fig.…”

Section: Fig 1 Schematics Of the Pjdhfr Inhibitors Trimethoprim And Omentioning

confidence: 99%

See 2 more Smart Citations

Trimethoprim Resistance of Dihydrofolate Reductase Variants from Clinical Isolates of Pneumocystis jirovecii

Queener

Cody

Pace

et al. 2013

Antimicrob Agents Chemother

View full text Add to dashboard Cite

dPneumocystis jirovecii is an opportunistic pathogen that causes serious pneumonia in immunosuppressed patients. Standard therapy and prophylaxis include trimethoprim (TMP)-sulfamethoxazole; trimethoprim in this combination targets dihydrofolate reductase (DHFR). Fourteen clinically observed variants of P. jirovecii DHFR were produced recombinantly to allow exploration of the causes of clinically observed failure of therapy and prophylaxis that includes trimethoprim. Six DHFR variants (S31F, F36C, L65P, A67V, V79I, and I158V) showed resistance to inhibition by trimethoprim, with K i values for trimethoprim 4-fold to 100-fold higher than those for the wild-type P. jirovecii DHFR. An experimental antifolate with more conformational flexibility than trimethoprim showed strong activity against one trimethoprim-resistant variant. The two variants that were most resistant to trimethoprim (F36C and L65P) also had increased K m values for dihydrofolic acid (DHFA). The catalytic rate constant (k cat ) was unchanged for most variant forms of P. jirovecii DHFR but was significantly lowered in F36C protein; one naturally occurring variant with two amino acid substitutions (S106P and E127G) showed a doubling of k cat , as well as a K m for NADPH half that of the wild type. The strongest resistance to trimethoprim occurred with amino acid changes in the binding pocket for DHFA or trimethoprim, and the strongest effect on binding of NADPH was linked to a mutation involved in binding the phosphate group of the cofactor. This study marks the first confirmation that naturally occurring mutations in the gene for DHFR from P. jirovecii produce variant forms of DHFR that are resistant to trimethoprim and may contribute to clinically observed failures of standard therapy or prophylaxis.

show abstract

Section: Fig 1 Schematics Of the Pjdhfr Inhibitors Trimethoprim And Osupporting

confidence: 67%

Section: Fig 1 Schematics Of the Pjdhfr Inhibitors Trimethoprim And Omentioning

confidence: 99%

See 1 more Smart Citation

Trimethoprim Resistance of Dihydrofolate Reductase Variants from Clinical Isolates of Pneumocystis jirovecii

Queener

Cody

Pace

et al. 2013

Antimicrob Agents Chemother

View full text Add to dashboard Cite

show abstract

“…1, top). The moderate divergence between these two closely related species is not unexpected, as several features in the mitochondrial DNA of P. murina and P. carinii diverge from those of P. jirovecii (56), and this pattern of sequence similarity has also been observed between P. carinii and P. jirovecii dihydrofolate reductases (47,57). In addition, there appears to be significant genetic diversity at several regions among P. jirovecii isolates, based on genetic analyses (58)(59)(60)(61).…”

Section: Resultsmentioning

confidence: 88%

“…Pneumocystis is challenging to treat with standard antifun-gals, and the use of the available agents can be limited by drugrelated toxicities. Accordingly, efficacious anti-Pneumocystis agents with minimal human toxicities still represent an unmet clinical need, despite significant efforts over the course of several decades (44)(45)(46)(47)(48)(49).…”

mentioning

confidence: 99%

Pneumocystis jirovecii Rtt109, a Novel Drug Target for Pneumocystis Pneumonia in Immunosuppressed Humans

Dahlin

Kottom

Han

et al. 2014

Antimicrob Agents Chemother

View full text Add to dashboard Cite

f Pneumocystis pneumonia (PcP) is a significant cause of morbidity and mortality in immunocompromised patients. In humans, PcP is caused by the opportunistic fungal species Pneumocystis jirovecii. Progress in Pneumocystis research has been hampered by a lack of viable in vitro culture methods, which limits laboratory access to human-derived organisms for drug testing. Consequently, most basic drug discovery research for P. jirovecii is performed using related surrogate organisms such as Pneumocystis carinii, which is derived from immunosuppressed rodents. While these studies provide useful insights, important questions arise about interspecies variations and the relative utility of identified anti-Pneumocystis agents against human P. jirovecii. Our recent work has identified the histone acetyltransferase (HAT) Rtt109 in P. carinii (i.e., PcRtt109) as a potential therapeutic target for PcP, since Rtt109 HATs are widely conserved in fungi but are absent in humans. To further address the potential utility of this target in human disease, we now demonstrate the presence of a functional Rtt109 orthologue in the clinically relevant fungal pathogen P. jirovecii (i.e., PjRtt109). In a fashion similar to that of Pcrtt109, Pjrtt109 restores H3K56 acetylation and genotoxic resistance in rtt109-null yeast. Recombinant PjRtt109 is an active HAT in vitro, with activity comparable to that of PcRtt109 and yeast Rtt109. PjRtt109 HAT activity is also enhanced by the histone chaperone Asf1 in vitro. PjRtt109 and PcRtt109 showed similar low micromolar sensitivities to two reported small-molecule HAT inhibitors in vitro. Together, these results demonstrate that PjRtt109 is a functional Rtt109 HAT, and they support the development of anti-Pneumocystis agents directed at Rtt109-catalyzed histone acetylation as a novel therapeutic target for human PcP.

show abstract

Probing the origin of dihydrofolate reductase inhibition via proteochemometric modeling

Hariri

Ghasemi

Shirini

et al. 2018

Journal of Chemometrics

View full text Add to dashboard Cite

Dihydrofolate reductase (DHFR) is an essential enzyme in the folate metabolism pathway and an important target of antineoplastic, antimicrobial, antiprotozoal, and antiinflammatory drugs. Despite the clinical effectiveness of current antifolate treatments, new drugs are needed to be designed due to developing resistance of this enzyme through multiple‐site mutagenesis. Understanding the factors affecting the ligand binding selectivity profiles among DHFR families is critical for the design of novel potent and selective inhibitors, with the least side effects, against DHFR of pathogens. Hybrid scaffolds containing pyrimidine ring are effective in DHFR inhibition. In this study, using proteochemometric (PCM) modeling, we designed and evaluated new potent pyrimidine scaffold‐based inhibitors via 3‐dimensional alignment‐free GRid‐INdependent Descriptors (GRIND), VolSurf molecular, and sequence‐based (z‐scale) descriptors to provide ligand and receptor descriptors, respectively. Validation and robustness of the model were confirmed by venetian blinds cross‐validation and Y‐scrambling approaches, respectively. Applicability domain (AD) analysis was performed to estimate the likelihood of reliable prediction for compounds. To show the applicability of the PCM model, new ligands were designed using structural data retrieved from this model. Inhibitory activities of the designs were then predicted, and selectivity ratio profiles were investigated. Finally, potent and highly selective inhibitors were identified regarding the protozoan parasite Toxoplasma gondii, followed by evaluating the ADMET parameters of the ligands.

show abstract

Kinetic and Structural Analysis for Potent Antifolate Inhibition of Pneumocystis jirovecii, Pneumocystis carinii, and Human Dihydrofolate Reductases and Their Active-Site Variants

Cited by 15 publications

References 28 publications

Trimethoprim Resistance of Dihydrofolate Reductase Variants from Clinical Isolates of Pneumocystis jirovecii

Trimethoprim Resistance of Dihydrofolate Reductase Variants from Clinical Isolates of Pneumocystis jirovecii

Pneumocystis jirovecii Rtt109, a Novel Drug Target for Pneumocystis Pneumonia in Immunosuppressed Humans

Probing the origin of dihydrofolate reductase inhibition via proteochemometric modeling

Contact Info

Product

Resources

About