| Literature DB >> 25886468 |
Kakularam Kumar Reddy1, Veena Kumari Vidya Rajan2, Ashish Gupta3, Polamarasetty Aparoy4, Pallu Reddanna5,6.
Abstract
BACKGROUND: Cyclooxygenase (COXs) and Lipoxygenase (LOXs) pathways are the two major enzymatic pathways in arachidonic acid (AA) metabolism. The term eicosanoid is used to describe biologically active lipid mediators including prostaglandins, thromboxanes, leukotrienes and other oxygenated derivatives, which are produced primarily from AA. Eicosanoids generated in a tissue specific manner play a key role in inflammation and cancer. As AA is the substrate common to variety of COXs and LOXs, inhibition of one pathway results in diversion of the substrate to other pathways, which often is responsible for undesirable side effects. Hence there is need for development of not only isozyme specific inhibitors but also dual/multi enzyme inhibitors. Understanding the interactions of AA and characterizing its binding sites in these enzymes therefore is crucial for developing enzyme specific and multi enzyme inhibitors for enhancing therapeutic efficacy and/or overcoming side effects.Entities:
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Year: 2015 PMID: 25886468 PMCID: PMC4416244 DOI: 10.1186/s13104-015-1101-4
Source DB: PubMed Journal: BMC Res Notes ISSN: 1756-0500
Figure 1Common physiochemical parameters identified for 5-LOX (white) and COX-2 (green). ALI, PII, ACC, DON, DAC interacting groups at the AA binding site are labeled.
MultiBind data on pairwise alignments of COX-2 binding site with all six enzymes
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| COX-2 – COX-1 | 36 | 90.4106 |
| COX-2 – 5-LOX | 15 | 33.4303 |
| COX-2 – 12-LOX | 10 | 32.6815 |
| COX-2 – 15-LOX | 12 | 41.8927 |
| COX-2 – LOX-1 | 8 | 19.6051 |
| COX-2 – LOX-3 | 11 | 35.3228 |
Pair wise alignments of 5-LOX binding site with other LOXs using MultiBind
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| 5-LOX– 12-LOX | 10 | 35.3112 |
| 5-LOX– 15-LOX | 14 | 41.9221 |
| 5-LOX– LOX-1 | 8 | 24.9893 |
| 5-LOX– LOX-3 | 15 | 36.8885 |
Figure 2Common physiochemical parameters identified for 5-LOX, 12-LOX and 15-LOX. The amino acids of 5-LOX (green), 12-LOX (red) and 15-LOX (blue) contributing to the common properties are shown.
Alignments of individual LOXs with COXs using MultiBind
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| 1 | COX1-COX2-sLOX3 | 10 | 40.4966 |
| 2 | sLOX1-COX1-COX2 | 6 | 32.5165 |
| 3 | 15LOX-COX1-COX2 | 10 | 47.1464 |
| 4 | 12LOX-COX1-COX2 | 10 | 40.7187 |
| 5 | 5LOX-COX1-COX2 | 13 | 45.4904 |
Common physiochemical parameters identified for COX-1, COX-2, 5-LOX, 12-LOX and 15-LOX
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| Glu 357 | ACC | Glu 356 | ACC | Gln 363 | ACC | Ser 530 | DAC | Ser 530 | DAC |
| His 361 | DAC | His 360 | DAC | His 367 | DAC | Ala 527 | DON | Ala 527 | DON |
| His 361 | PII | His 360 | PII | His 367 | PII | Gly 526 | PII | Gly 526 | PII |
| Leu 362 | ALI | Leu 361 | ALI | Leu 368 | ALI | Met 522 | ALI | Met 522 | ALI |
| Leu 408 | ALI | Val190 | ALI | Ile 415 | ALI | Leu 352 | ALI | Leu 352 | ALI |
Figure 3Licofelone in the binding site of A) COX-2 and B) 5-LOX.
Figure 4Receptor based pharmacophore of all the LOXs and COXs was studied. Aliphatic groups are shown in grey; Acceptor groups are shown in red; Donor/Acceptor groups are shown in blue; Aromatic pi contacts are shown in orange.
Figure 5ABT-761 in the binding site of 5-LOX.