Comparative analyses and structural insights of the novel cytochrome P450 fusion protein family CYP5619 in Oomycetes

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作者
Hans Denis Bamal
Wanping Chen
Samson Sitheni Mashele
David R. Nelson
Abidemi Paul Kappo
Rebamang Anthony Mosa
Jae-Hyuk Yu
Jack A. Tuszynski
Khajamohiddin Syed
机构
[1] Central University of Technology,Unit for Drug Discovery Research, Department of Health Sciences
[2] Huazhong Agricultural University,College of Food Science and Technology
[3] University of Tennessee Health Science Center,Department of Microbiology, Immunology and Biochemistry
[4] University of Zululand,Department of Biochemistry and Microbiology, Faculty of Science and Agriculture
[5] University of Wisconsin-Madison,Department of Bacteriology
[6] 3155 MSB,Department of Physics
[7] University of Alberta,Cross Cancer Institute, Department of Oncology
[8] University of Alberta,undefined
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摘要
Phylogenetic and structural analysis of P450 proteins fused to peroxidase/dioxygenase has not been reported yet. We present phylogenetic and in silico structural analysis of the novel P450 fusion family CYP5619 from the deadliest fish pathogenic oomycete, Saprolegnia diclina. Data-mining and annotation of CYP5619 members revealed their unique presence in oomycetes. CYP5619 members have the highest number of conserved amino acids among eukaryotic P450s. The highest number of conserved amino acids (78%) occurred in the peroxidase/dioxygenase domain compared to the P450 domain (22%). In silico structural analysis using a high-quality CYP5619A1 model revealed that CYP5619A1 has characteristic P450 structural motifs including EXXR and CXG. However, the heme-binding domain (CXG) in CYP5619 members was found to be highly degenerated. The in silico substrate binding pattern revealed that CYP5619A1 have a high affinity to medium chain fatty acids. Interestingly, the controlling agent of S. diclina malachite green was predicted to have the highest binding affinity, along with linoleic acid. However, unlike fatty acids, none of the active site amino acids formed hydrogen bonds with malachite green. The study’s results will pave the way for assessing CYP5619A1’s role in S. diclina physiology, including the nature of malachite green binding.
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