The Crystal Structure of D7r4, a Salivary Biogenic Amine-binding Protein from the Malaria Mosquito Anopheles gambiae

Ben J Mans,Eric Calvo,José M.C Ribeiro,John F Andersen

doi:10.1074/jbc.m706410200

Abstract

The D7-related (D7r) proteins of the malaria vector Anopheles gambiae have been shown to bind the biogenic amines serotonin, norepinephrine, and histamine with high affinity. One member of the group (D7r1 or hamadarin) has also been shown to have an anticoagulant/antikinin activity. To understand the mechanistic details of its antihemostatic/anti-inflammatory effects, we have determined the crystal structure of one member of this group, D7r4, along with the structures of ligand complexes with serotonin, tryptamine, histamine, and norepinephrine. The D7 fold consists of an arrangement of eight alpha-helices stabilized by three disulfide bonds. The structure is similar to those of the arthropod odorant-binding proteins, a relationship that had been predicted based on sequence comparisons. Although odorant-binding proteins commonly have six alpha-helices, D7r4 has eight, resulting in significantly different positioning and structure of the ligand binding pocket. The pocket itself is lined by hydrophobic side chains along with polar and charged groups oriented to form hydrogen bonds with the aliphatic amino group and with groups on the aromatic portions of the ligands. These structures, along with accompanying mutagenesis studies, have allowed us to identify critical residues for biogenic amine binding and to predict which members of the large D7 protein family found in blood-feeding nematocerous Diptera will function as biogenic amine-binding proteins.

Highlights

Anopheles gambiae is the major African vector of the malaria parasite Plasmodium falciparum that infects 300 –500 million people and causes 1–2 million deaths annually
Saliva from female A. gambiae contains a plethora of potent antihemostatic proteins, including the thrombin inhibitor anophelin [2], the platelet aggregation inhibitor apyrase [3, 4], and catechol oxidase-peroxidase, which serves as a vasodilator [5, 6]
The serotonin and tryptamine complexes were obtained by cocrystallization of protein and ligand, whereas the norepinephine and histamine complexes were obtained by soaking crystals with ligand-containing solutions

Summary

Mean B value for all atoms

18.4/21.8 a Data collection at two wavelengths on a single crystal, with values for the second data set being in parentheses. 0.010 1.15 93.1/100 42.7 18.3/25.0 relationship between the D7/D7r proteins and the arthropod odorant (or pheromone)-binding protein (OBP) family [8]. We describe the three-dimensional structure of D7r4 along with the structures of a number of ligand complexes. Details of the structures reveal how the D7r proteins act to inhibit hemostatic and inflammatory processes by binding a diverse set of ligands with high affinity. The study confirms the relationship of the D7r proteins with the OBPs, suggesting a possible origin for the group

EXPERIMENTAL PROCEDURES

RESULTS AND DISCUSSION

Details of the Ligand Binding