Sandbox 124
From Proteopedia
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+ | == Your Heading Here (maybe something like 'Structure') == | ||
+ | <StructureSection load='4dki' size='350' side='right' caption='Structure of HMG-CoA reductase (PDB entry [[1dq8]])' scene=''> | ||
+ | Anything in this section will appear adjacent to the 3D structure and will be scrollable. | ||
+ | ===Introduction> | ||
+ | '''Transpeptidases (TP), also known as penicillin-binding proteins (PBP), | ||
+ | catalyze the cross-linking of peptidoglycan polymers during bacterial cell wall | ||
+ | synthesis. The natural transpeptidase substrate is the D-Ala-D-Ala | ||
+ | peptidoglycan side chain terminus. Beta-lactam (β-lactam) antibiotics, which | ||
+ | include penicillins, cephalosporins and carbapenems, bind and irreversibly | ||
+ | inhibit transpeptidases by mimicking the D-Ala-D-Ala substrate, resulting in | ||
+ | the inhibition of cell wall synthesis and ultimately bacterial cell growth. | ||
+ | Overuse and misuse of β-lactams has led to the generation of methicillinresistant | ||
+ | Staphylococcus aureus (MRSA) isolates that have acquired an | ||
+ | alternative transpeptidase, PBP2a, which is neither bound nor inhibited by β- | ||
+ | lactams. MRSA isolates are resistant to all β-lactams, can be hospital- or | ||
+ | community-acquired, and are often the cause of significant morbidity and | ||
+ | mortality. Furthermore, they are often only susceptible to “last resort | ||
+ | antibiotics”, such as vancomycin. Recently, two cephalosporins - ceftobiprole | ||
+ | and ceftaroline - that bind and inhibit PBP2a have been developed. The | ||
+ | Hostos-Lincoln Academy Students Modeling A Research Topic (SMART) | ||
+ | Team generated a model of the PBP2a/ceftobiprole complex (PDB 4DKI) | ||
+ | using 3D printing technology to illustrate the mechanism of action of | ||
+ | ceftobiprole. Supported by a grant from the Camille and Henry Dreyfus Foundation.''' |
Revision as of 17:44, 23 July 2013
Your Heading Here (maybe something like 'Structure')
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