Sequencing of P. argentipes and P. perniciosus salivary gland cDNA libraries
From the P. argentipes salivary gland cDNA library, we sequenced 603 randomly selected clones from which 135 unique clusters of related sequences were obtained. Out of the 135 clusters, we found 45 clusters (1.11 sequences per cluster) of transcripts coding for housekeeping genes. We found 111 sequences, arranged in 55 clusters (1.8 sequences per cluster) that were not similar to other genes in the NCBI databank and lacked a secretory signal peptide. The most abundant transcripts in this cDNA library contained putative secretory proteins. We found 438 cDNA with potentially secreted proteins signals arranged in 30 clusters (an average of 14.36 sequences per cluster). The number of cDNA coding for secretory proteins is 9 times greater than the cDNA coding for housekeeping genes and 4 times greater than the cDNA coding for non-secreted proteins with unknown function. The transcripts coding for secretory proteins represent 73% of the total transcripts sequenced in the P. argentipes salivary gland library.
Similarly, the most abundant transcripts found in the P. perniciosus salivary gland cDNA library coded for secretory proteins. From a total of 535 sequenced cDNA we found that 394 cDNA were potentially secreted and were grouped into 30 clusters (average of 14.36 sequences per cluster). The cDNA coding for secretory proteins represent 74% of the cDNA sequenced, while transcripts coding for housekeeping genes represent 13.4 % (72/535). An additional 13 % (69/535) of transcripts coded for unknown (non-secreted) proteins. Table 1 and Table 2 contain the results of the analysis of the transcripts coding for secreted proteins from the salivary glands of P. argentipes and P. perniciosus.
<p>Table 1</p>
Putative secreted proteins from the salivary glands of Phlebotomus argentipes.
Sequence name
NCBI accession number
Cluster
Signal P site
MW
pI
Best match to NR protein database
E value
Comments
Present in proteome
PagSP01
DQ136148
1
20–21
14.2
6.1
SL1 protein L. longipalpis
2e-018
Similar to PpSP15
Yes
PagSP02
DQ136149
2
20–21
13.6
9.4
SL1 protein L. longipalpis
7e-029
Similar to PpsP15
Yes
PagSP03
DQ136150
3
21–22
34.9
9.1
Apyrase Phlebotomus
4e-092
Salivary apyrase
Yes
PagSP04
DQ136151
4
18–19
43.2
8.8
44 kDa salivary protein
1e-120
Yellow protein
Yes
PagSP05
DQ136152
5
19–20
29.1
9.1
Antigen 5 L. longipalpis
1e-104
Antigen 5 protein
Yes
PagSP06
DQ136153
6
17–18
24.9
9.6
32 kDa salivary protein
9e-038
Similar to PpSP32
Yes
PagSP07
DQ136154
7
20–21
14.3
8.9
SL1 protein L. longipalpis
2e-019
Similar to PpSP15
Yes
PagSP09
DQ136155
9
22–23
33.1
8.9
32 kDa protein L. longipalpis
2e-64
Yes
PagSP10
DQ136156
10
19–20
26.7
5.5
28 kDa salivary protein
7e-078
D7 related protein
Yes
PagSP11
DQ136157
11
21–22
40.1
9.4
Endonuclease L. longipalpis
4e-039
Endonuclease
PagSP12
DQ136158
12
20–21
14.1
8.9
SL1 protein L. longipalpis
4e-023
Similar to PpSP15
PagSP13
DQ136159
13
20–21
13.9
8.9
14 kDa salivary protein
8e-031
Similar to PpSP15
PagSP14
DQ136160
14
24–25
43.9
8.8
ebiP3881 An gambiae
7e-099
Lipase-like
PagSP15
DQ136161
15
20–21
30.1
9.6
Novel protein
PagSP17
DQ136162
17
20–21
29.4
8.0
Novel protein
Yes
PagSP19
DQ136163
19
21–22
30.0
12
Novel protein
PagSP20
DQ136164
20
20–21
27.4
9.6
Novel protein
PagSP25
DQ136165
25
20–21
27.9
9.5
30 kDa salivary protein
6e-045
D7 protein
PagSP56
DQ136166
56
20–21
30.1
7.0
Novel protein
PagSP60
DQ136167
60
19–20
11.7
3.9
putative histone promoter
2e-005
PagSP73
DQ136168
73
20–21
16.1
5.5
A. gambiae unknown
0.002
Unknown
PagSP124
DQ136169
124
21–22
15.5
5.2
Novel protein
PagSP132
DQ136170
132
22–23
47.3
6.5
agCP4255 An. gambiae
2e-095
Pyrophosphatase
<p>Table 2</p>
Putative secreted proteins from the salivary glands of Phlebotomus perniciosus.
Sequence name
NCBI accession number
Cluster
Signal P site
MW
pI
Best match to NR protein database
E value
Comments
Present in proteome
PpeSP01
DQ192490
1
20–21
35.5
9.3
Salivary apyrase P. papatasi
4e-86
Apyrase
Yes
PpeSP01B
DQ192491
1B
Salivary apyrase P. papatasi
Apyrase
Yes
PpeSP02
DQ150620
2
20–21
14.8
8.7
SL1 protein L. longipalpis
2e-20
SP15 like protein
Yes
PpeSP03
DQ150621
3
18–19
41.8
6.0
42 kDa salivary prot. P. papatasi
1e-113
Yellow protein
Yes
PpeSP03B
DQ150622
3B
18–19
42.7
8.6
44 kDa salivary prot. P. papatasi
1e-117
Yellow protein
Yes
PpeSP04
DQ150623
4
19–20
24.5
8.5
28 kDa salivary prot. P. papatasi
6e-64
D7 protein
Yes
PpeSP04B
DQ150624
4B
19–20
26.9
8.7
28 kDa salivary prot. P. papatasi
3e-80
D7 protein
Yes
PpeSP05
DQ153099
5
17–18
27.8
10.4
29 kDa salivary prot. L. longipalpis
1e-23
PpeSP06
DQ153100
6
22–23
33.0
8.9
32 kDa salivary prot. L. longipalpis
6e69
Yes
PpeSP07
DQ153101
7
19–20
29.6
9.1
Antigen 5 prot. L. longipalpis
5e-84
Antigen 5 protein
Yes
PpeSP08
DQ153102
8
25–26
28.8
4.9
Salivary prot. C. sonorensis
0.016
PpeSP09
DQ153103
9
20–21
14.6
8.6
14 kDa salivary prot. P. papatasi
2e-28
SP15-like protein
Yes
PpeSP10
DQ153104
10
19–20
26.7
9.4
30 kDa salivary prot. P. papatasi
2e-47
D7 protein
Yes
PpeSP11
DQ153105
11
19–20
13.2
9.0
SL1 prot. L. longipalpis
1e-20
SP15 like protein
Yes
PpeSP12
DQ153106
12
20–21
7.1
11.0
Novel protein
PpeSP13
DQ153107
13
20–21
9.7
4.8
Novel protein
PpeSP15
DQ192489
15
25–26
2.7
10.6
Novel protein
PpeSP18
DQ154097
18
29–30
29.9
8.3
Phospholipase A2, Drosophila
1e-78
Phospholipase A2
PpeSP19
DQ154098
19
20–21
45.8
8.5
37 kDa prot.. L. longipalpis
2e-33
Yes
PpeSP32
DQ154099
32
23–24
41.4
9.5
L. longipalpis endonuclease
1e-121
Endonuclease
In addition to the identification of proteins previously reported from other sandflies, we found a number of transcripts coding for proteins not previously shown to be present in the salivary glands of sandflies. A protein homologous to lipases from Anopheles gambiae, Drosophila melanogaster and other organisms was found in the P. argentipes cDNA library. We also found in this library and in the P. perniciosus cDNA library, a transcript coding for a protein homologous to a pyrophosphatase. The predicted 47-kDa protein named PagSP132 contains a phosphodiesterase type I, phosphodiesterase/nucleotide pyrophosphatase motif. This type of enzymes cleaves the phosphodiester and phosphosulfate bonds in NAD, deoxynucleotides and nucleotide sugars 10. BLAST search of this protein identified protein orthologs found in mammals as well as in A. gambiae. To our knowledge, pyrophosphatases have not been described in the saliva of other sandflies.
We found one cluster in the P. perniciosus cDNA library coding for a phospholipase A2 (PLA2) protein (PpeSP18). This type of protein has never been reported from the saliva of a blood-feeding insect. PLA2 (Phosphatidylcholine-2-acylhydrolase, E.C. 3.1.1.4) are well known for their ability to cleave the arachidonic acid and lysophosphatidylcholine from the sn-2 position of membrane glycerol-3-phospholipids. Also PLA2 are known to work as toxins by blocking the release of neurotransmitters 11.
We identified transcripts coding for secreted proteins that did not match any reported proteins in accessible databases. P. argentipes contained six unknown proteins that ranged from 15 to 30 kDa, while only three were found in the P. perniciosus library and all were relatively small ranging from 10 to 27 kDa (Tables 1 and 2).
Proteome analysis of P. argentipes and P. perniciosus salivary proteins
Edman degradation of the salivary proteins separated by SDS-PAGE from P. argentipes resulted in the identification of 12 N-terminal sequences (Figure 1A). The identified proteins included three PpSP15-like protein (PagSP02, PagSP01 and PagSP07), D7-related protein (PagSP10), PpSP32-like salivary protein (PagSP06), antigen 5 related proteins (PagSP05), a novel protein (PagSP17), P. papatasi apyrase-like protein (PagSP03), L. longipalpis 32-kDa-like salivary protein (PagSP09), and a yellow-related protein (PagSP04). Three proteins with different mobility on the gel had the same N-terminal sequence (PagSP04), and were probably derived from the same transcript but with different post-translational modifications.
<p>Figure 1</p>
Amino-terminal sequence of salivary gland proteins
Amino-terminal sequence of salivary gland proteins. (A) Supernatant of salivary gland homogenate of Phlebotomus argentipes was separated in SDS-PAGE and transfer to PVDF membrane as described in Methods. N-terminal sequence obtained was searched in the sandfly database and the clone containing the sequence is shown at the right. (B) N-terminal sequence and matched clones of salivary gland proteins from Phlebotomus perniciosus.
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From P. perniciosus salivary gland protein analysis we found 13 N-terminus sequences (Figure 1B). The identified proteins included: three PpSP15-like proteins (PpeSP11, PpeSP02 and PpeSP09), three D7-related proteins (PpeSP04, PpeSP04B, PpeSP10), a 37-kDa-like protein described previously in the saliva of L. longipalpis (PpeSP19), an antigen-5 related protein (PpeSP07), two apyrase-like proteins (PpeSP01, PpeSP01B), a 32-kDa-like salivary protein described on L. longipalpis (PpeSP06) and two yellow-related proteins (PpeSP03, PpeSP03B). Not all attempted Edman degradation experiments resulted in a sequence, either because of insufficient protein amount or because N-terminal ends were blocked.
Comparative analysis of salivary transcripts from vectors of visceral leishmaniasis: P. argentipes, P. perniciosus, P. ariasi and L. longipalpis
In an attempt to understand the relationship of salivary proteins among different sandflies and to gain insights into the evolution of sandfly salivary proteins, we compared cDNA libraries from four different sandflies. We selected the sandflies based on their availability and their significance for this study. First, we selected sandflies from the two different genera, Phlebotomus and Lutzomyia. Secondly, from the Phlebotomus genus we selected two different subgenus, Euphlebotomus (P. argentipes) and Larroussius (P. ariasi and P. perniciosus). The phylogenetic relationship among these sandflies was previously studied using the small subunit nuclear ribosomal DNA 12.
Full-length secreted proteins from each sandfly library were compared using a stand alone version of BLAST. We found 10 families of proteins that are common among all four cDNA libraries: 1) PpSP15 like protein, 2) apyrase-like, 3) yellow related protein, 4) antigen-5 related protein, 5) PpSP32 like protein, 6) 32 kDa-like protein, 7) D7 related protein and 8) an endonuclease-like protein, 9) a 39-kDa-like protein, and a 16.1 kDa-like protein (Table 3). The level of similarities according to BLAST values was highly significant (2E-18 to 1E-169). The protein families listed above may be common to both Lutzomyia and Phlebotomus species, and may be present in other species from both genera.
<p>Table 3</p>
Salivary transcripts shared by Phlebotomus and Lutzomyia sandflies.
Family of proteins
P. argentipes
P. ariasi
P. perniciosus
L. longipalpis
PpSP15-like protein
PagSP01, 02, 07, 12, 13
ParSP03, 08
PpeSP02, 09, 11
LJM04
Apyrase
PagSP03
ParSP01
PpeSP01, 01B
LJL23
Yellow protein
PagSP04
ParSP04, 04B
PpeSP03, 03B
LJM17, LJM11, LJM111
Antigen 5-related protein
PagSP05
ParSP05
PpeSP07
LJL34
PpSP32-like protein
PagSP06
ParSP02
PpeSp05
LJL04
33 kDa, unknown function
PagSP09
ParSP09
PpeSP06
LJL143
D7-related protein
PagSP10, 25
ParSP07, 12, 16
PpeSP04, 04B, 10
LJL13
Endonuclease-like
PagSP11
ParSP10
PpeSP32
LJL138
39 kDa, unknown function
ParSp17
PpeSP19
LJM78
16.1 kDa, unknown function.
ParSP80
LJS138
It is interesting to note the amount of variation that exists in the number of members of the different protein families found in the four sandflies (Table 3). The PpSP15-like family has five members identified in P. argentipes (PagSP01, PagSP02, PagSP07, PagSP12 and PagSP13), two in P. ariasi (ParSP03, ParSP08), three in P. perniciosus (PpeSP02, PpeSP09 and PpeSP11), yet only one (LloSP05) in L. longipalpis (Table 3). On the other hand, only one member of the apyrase family of proteins has been found in each sandfly except for P. perniciosus, which has two members (Table 3). Other families of salivary proteins, such as antigen 5, PpSP32, 32 kDa and endonuclease-like protein were represented by only one member from each of the different sandflies. The yellow-related protein has one member found in P. argentipes, two members in the P. perniciosus and P. ariasi and three members in the Lutzomyia longipalpis sandfly. The D7-related protein was represented by three members in Phlebotomus sandflies, while only one member is present in the L. longipalpis sandfly.
Through comparative analysis we found at least one unique transcript from each of the four cDNA libraries. Nine unique transcripts were identified in P. argentipes, five in P. ariasi, one in P. perniciosus and twenty-four in L. longipalpis. The large difference in L. longipalpis may be due to genus differences (Phlebotomus vs. Lutzomyia); therefore, we would expect to find similar transcripts in other Lutzomyia species. Only four families of proteins were unique to Phlebotomus: a 32-kDa protein of unknown function, a 2-kDa peptide, a 5-kDa peptide and a phospholipase A2-like protein (Table 4).
<p>Table 4</p>
Salivary transcripts shared by Phlebotomus sandflies.
Protein
P. argentipes
P. ariasi
P. perniciosus
32 kDa, unknown function
PagSP19
ParSP25
PpeSP08
2 kDa, unknown function
ParSP23
PpeSP15
5 kDa, unknown function
ParSP15
PpeSP12
Phospholipase A2-like
PagSP18
ParSP11
PpeSP18
Molecular characteristics of salivary proteins shared among the analysed sandflies
In order to understand the relationship among salivary proteins from different sandflies, we performed multiple sequence alignment followed by phylogenetic analysis of the salivary transcripts shared by the vectors of visceral leishmaniasis studied (Table 3). Following is a description of the shared proteins:
SL1/PpSP15 related proteins
The SL1/PpSP15 group of proteins is similar to the SL1 salivary protein from L. longipalpis, which has no known function 13, and to PpSP15, a 15- kDa salivary protein from Phlebotomus papatasi that was previously shown to confer protection against L. major infection 14. The predicted molecular weight of these transcripts is approximately 14 kDa and is in agreement with the observed MW found through the proteome analysis (Figure 1). This group represents the most abundant transcripts in the salivary gland cDNA library of P. argentipes (Table 1). The fact that only one PpSP15 member was found in L. longipalpis, suggests that a number of lineage-specific gene expansions (gene duplication events) occurred in the Phlebotomus lineage at various periods in the evolution of these sandflies.
The PpSP15 family of proteins has only been found in species of sandflies suggesting that this family was a specific invention that occurred during sandfly evolution, most likely during their adaptation to a blood-feeding environment. Although PSI-BLAST analysis using PpSP15 proteins retrieved only members of the PpSP15 family, the PHYRE prediction servers indicated that members of the PpSP15 family possess an EF-hand fold most closely related to members of the odorant-binding protein (OBP) family to which the D7-proteins belong. It is thus likely that PpSP15 members were derived from an OBP ancestral protein. Characteristically, the OBP family in Drosophila has a low degree of sequence similarity among its members with only six conserved cysteines among the thirty-four members of this family 15.
The multiple pair-wise alignment analysis of sandfly PpSP15 shows a high degree of divergence among the sequences, 7.5% identity and 23.10% similarity (Figure 2A). The number of amino acids between the second and third cysteine (three) and between the fifth and the sixth cysteine (eight) were shown to be conserved among all the Drosophila OBP members 15. All of the sandflies sequences analysed from the PpSP15 protein family contained identical cysteine positioning. This data suggests that this family of proteins may be closely related to the short form of D7 because of the similarities to OBP and its small size of 15 kDa, which is similar to the MW found in the mosquitoes short D7 16.
<p>Figure 2</p>
Analysis of PpSP15 family of sandfly salivary proteins
Analysis of PpSP15 family of sandfly salivary proteins. (A) Multiple sequence alignment of PpSP15 salivary proteins from Phlebotomus argentipes (Pag), Phlebotomus ariasi (Par), Phlebotomus perniciosus (Ppe) and Lutzomyia longipalpis (LJ). Sequences were aligned using ClustalX and manually refined using BioEdit sequence-editing software. (B) Phylogenetic tree analysis of PpSP15 salivary proteins from these four sandflies. Phylogenetic analysis was conducted on protein alignments using Tree Puzzle version 5.2 by maximum likelihood using quartet puzzling, automatically estimating internal branch node support (1000 replications).
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Phylogenetic analysis of PpSP15 transcripts from the different sandflies including P. papatasi resulted in the formation of 5 distinct clades (Figure 2B). As such, three major clusters of orthologous groups of proteins (COGs), and hence gene duplication events, can be identified that possibly occurred in the ancestor to the Phlebotomus lineage. COG1 includes members from P. perniciosus, P. argentipes and P. papatasi with a second related clade that includes a lineage-specific expansion (LSE) in P. papatasi. COG2 includes members from P. perniciosus and P. argentipes. COG3 includes members from P. perniciosus, P. argentipes and P. ariasi. Another clade composed solely of members of P. argentipes indicates another LSE. Evolutionarily, the P. papatasi group was basal to the other Phlebotomus members analysed in this study, followed by P. argentipes, with P. perniciosus and P. ariasi forming the terminal clade. Given this, the topology of the cladogram obtained for the PpSP15 family suggests that COG2 resulted from gene duplication event that occurred in the ancestor to P. perniciosus and P. ariasi. COG1 follows the expected phylogenetic grouping but suggests that this gene was lost in P. ariasi or we failed to detect the ortholog in our library. COG3 again suggests that this specific gene duplication event occurred after divergence from the shared ancestor with P. papatasi. The PpSP15 family found in sandflies is thus characterised by both gene duplication and possibly gene loss events, both restricting an accurate reconstruction of its phylogeny. It is currently impossible to say which proteins share a conserved function with the PpSP15 from L. longipalpis as the major clades create a polytomy. As such, this family might bind related or similar pharmacologic components so that they all have, in fact, a similar function. This might explain the seemingly haphazard acquisition and loss of genes.
D7 family of proteins
D7-related proteins are found in the saliva of different diptera, including Anopheles 17, Aedes 18 and Culex 19 mosquitoes as well as in the sandflies P. papatasi 19, L. longipalpis 13 and P. ariasi 21 and does not appear to occur in non-dipteran species. Two forms of the protein have been described; a long and short form 19; and appear to be distantly related to an odorant binding super family of proteins. Interestingly, the OBP family seems to be the ancestral molecule of the PpSP15 family (see above). Therefore, it may be possible that both D7 and PpSP15 related proteins have a common ancestor.
The D7 protein named hamadarin from Anopheles stephensi acts as an anticoagulant affecting the plasma contact system by inhibiting the activation of Factor XII and kallikrein 23. Recently, a biological function of four short members of the D7 family from A. gambiae and a long D7 from Aedes aegypti was described 16. These salivary proteins were shown to bind biogenic amines such as serotonin, histamine and norepinephrine. This function is relevant for blood-feeding because of the inhibition of the vasoconstrictor, platelet aggregating, and pain inducing properties of these biogenic amines 16. The exact function of D7 proteins in sandflies is largely unknown, but it may be related to the function observed in mosquito D7 proteins, either as an anticoagulant or binding biogenic amines.
The D7 family is represented in the P. argentipes cDNA library by two members, PagSP10 and PagSP25, and in the P. perniciosus cDNA library by three members, PpeSP04, PpeSP04B and PpeSP10. Only one member of this family is present in L. longipalpis sandfly, suggesting a case of gene duplication of this protein that probably occurred more recently in the Phlebotomus genus.
Comparative analysis of the D7 family of proteins from different sandflies reveals few conserved regions of identity, with only 16% identity and 23% similarity between the sandfly D7 proteins. There are 10 conserved cysteines throughout the molecule. The size of the sandfly D7 proteins is slightly smaller than the long D7 forms found in mosquitoes. Additionally, sandfly D7 is missing the last cysteine that is present at the carboxy terminal region of the mosquito long- and short-form D7 and, instead, have a cysteine present between conserved cysteines 8 and 19 19. Based on PHYRE prediction results, the long-form D7 proteins have 16 alpha helix domains, the short form have 8 alpha helix domains, while the sandfly form have 13 domains. All three forms are associated to OBP, as mentioned above. Interestingly, the sandfly D7 proteins are predicted to contain a beta-strand domain starting at the 7th cysteine and characterised by a repeat of tyrosines at amino acid 188 (Figure 3A), replacing the alpha helix domain found in the mosquito D7 proteins at the same position. Due to these differences we are categorising the sandfly D7 as the medium form (Figure 3B).
<p>Figure 3</p>
Analysis of D7-related proteins
Analysis of D7-related proteins. A) Multiple sequence analysis of D7 proteins from the salivary glands of Phlebotomus argentipes (Pag), Phlebotomus ariasi (Par), Phlebotomus perniciosus (Ppe) and Lutzomyia longipalpis (LJ). Sequences were aligned using ClustalX and manually refined using BioEdit sequence-editing software. (B) Phylogenetic tree analysis of D7 salivary proteins from P. argentipes (Pag), P. ariasi (Par), P. perniciosus (Ppe), L. longipalpis (LJ), P. papatasi, Aedes aegypti, Ae. albopictus, Anopheles gambiae, An. Arabiensis, An. Darlingi, An. Stephensi and Culex quinquefasciatus. Phylogenetic analysis was conducted on protein alignments using Tree Puzzle version 5.2 by maximum likelihood using quartet puzzling, automatically estimating internal branch node support (1000 replications).
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Phylogenetic analysis of D7 proteins from different organisms shows 2 distinct clades with the sandfly proteins branching from the long form (Figure 3B). All of the sandfly D7 members are clustered within one clade, distinct from the long form members. The clade containing the mosquito D7 short-form proteins contains two clusters, one containing the Anopheles mosquitoes and the other containing the Culex and Aedes species. The sandfly clade subdivides into two distinct clades. The lower clade shows 5 distinct groups, two of these groups represent COGs of P. perniciosus and P. ariasi, and the group of P. papatasi seems to be a case of lineage expansion. The lower clade shows a COG that includes P. argentipes, P. ariasi and P. perniciosus proteins, PagSP25, ParSP07 and PpeSP10.
Apyrase family of proteins
Both the P. perniciosus and P. argentipes libraries contained transcripts homologous to the Cimex family of apyrases 24, a protein also present in the saliva of P. papatasi 7 and L. longipalpis 13. Apyrases are enzymes that function as potent anti-platelet factors by destroying or hydrolysing the platelet activator ADP. An orthologue was found in humans and the recombinant protein was shown to hydrolyse a variety of nucleoside di- and triphosphates, preferentially UDP, followed by GDP, UTP, GTP, ADP, and ATP 2526.
Sequence alignment of the P. argentipes,P. perniciosus and P. ariasi apyrases show a 47% identity and 81% similarity at the amino acid level (Figure 4A). When L. longipalpis is included in the analysis, there is a considerable decrease in the identity (29%) as well as in the similarity (67%) (data not shown).
<p>Figure 4</p>
Analysis of apyrase protein family
Analysis of apyrase protein family. (A) Multiple sequence analysis of apyrases from the salivary glands of Phlebotomus argentipes (Pag), Phlebotomus ariasi (Par) and Phlebotomus perniciosus (Ppe). Sequences were aligned using ClustalX and manually refined using BioEdit sequence-editing software. (B) Phylogenetic tree analysis of apyrase protein family from P. argentipes (Pag), P. ariasi (Par), P. perniciosus (Ppe), L. longipalpis (LJ), P. papatasi, Cimex lectularius, and transcripts coding from this protein family (identified at GenBank) from Drosophila melanogaster, An. Gambiae, A. mellifera, C. elegans, M. musculus, R. ratus, B. Taurus, H. sapiens, P. troglodytes, G. galus, D. rerio and X. leavis. Phylogenetic analysis was conducted on protein alignments using Tree Puzzle version 5.2 by maximum likelihood using quartet puzzling, automatically estimating internal branch node support (1000 replications).
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Phylogenetic analysis of apyrases from different organisms indicates three main clades with the sandfly apyrases in a distinct clade, apart from vertebrates, yet closely related to other insects (Figure 4B). Interestingly sandfly apyrases share a common ancestor with Cimex lectularius apyrase. The two insects appear to have evolved to the blood feeding mode independently 27. Within the clade containing the sandflies, one of the P. perniciosus apyrases, PpeSP01, is more closely related to the P. ariasi apyrase (ParSP01) than the second apyrase from P. perniciosus (PpSP01B). This may be the result of a gene duplication event in P. perniciosus and subsequent loss in P. ariasi. When searching databases we found a transcript from A. gambiae similar to sandfly apyrases. This is interesting because the known mosquito apyrases belong to the 5'-nucleotidase family of proteins. The known mosquito apyrase is very distinct, in size and sequence, from the Cimex family of apyrases also present in sandflies 28247, thus it is possible that mosquitoes in addition to a functional 5'-nucleotidase type apyrase, may have a non-functional sandfly/bedbug-like apyrase gene or it may have a house keeping function such as hydrolysing UDP formed after transglycosylation reactions in the Golgi 29. Alternatively, the mosquito may have a similar apyrase but with different substrate specificity or this protein is not present in their salivary gland.
Interestingly, the mosquito apyrase gene seems to be ancestral to the sandfly apyrase based on phylogenetic association (Figure 4B). Then it may be possible that mosquitoes have lost the function of this gene and kept the active form of the 5'-nucleotidase gene, which is the active apyrase in these insects.
The crystal structure of the Cimex family of apyrases was elucidated from the human counterpart and the amino acids relevant for calcium- and nucleotide-binding sites were determined 30. Several differences were noted among the amino acids relevant for nucleotide- or calcium-binding between sandflies, bedbugs and humans 30. Figure 5 shows the alignment of the different apyrases with amino acids relevant for calcium- and nucleotide-binding highlighted. We observed clear differences in some of these amino acids when sandflies were compared with other organisms including mosquitoes. The amino acids at position 124 are Ser (S), Thr (T) or Ala (A), in sandflies and Met (M) or Leu (L) in other organisms (Figure 5). Amino acids at position 126 is Met (M), Ile (I) or Leu (L) in sandflies and Lys (K) in other organisms; at position 129, sandflies have either Lys (K), Tyr (Y) or Leu (L) and other organisms have only Thr (T). At position 178, sandflies and bedbugs have a Trp (W) while other organisms have Ile (I). Amino acid substitutions may produce the specificity of the sandfly apyrases to ADP, a molecule that these insects must hydrolyse to overcome the hemostatic system and take a successful blood meal. In fact, Dai et al 30 showed that amino acid substitutions at some positions changed the substrate (GDP to ADP) in human apyrase. Human apyrases have more affinity for GDP substrate while sandfly apyrases have affinity for ADP 30.
<p>Figure 5</p>
Multiple sequence analysis of the apyrase family of proteins
Multiple sequence analysis of the apyrase family of proteins. Multiple sequence alignment of different organisms showing the amino acids highlighted in grey that are relevant for calcium and nucleotide binding as predicted from the structure of the human apyrase. Sequences were aligned using ClustalX and manually refined using BioEdit sequence-editing software.
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Yellow-related protein
The gene coding for the yellow protein was first described in Drosophila melanogaster 31. The proteins in this family appear to be derived from a common ancestor of the major royal jelly proteins (MRJPs) from honeybees and the yellow protein from Drosophila spp.
Drosophila yellow protein is related to pigmentation and male sexual behavior. In the family Culicidae a yellow protein was identified in Ae. aegypti whole-larvae extract and was associated to a dopachrome converting enzyme activity found in this insect 32. The function of this protein in the saliva of sandflies and its importance for blood feeding remains to be elucidated. The yellow protein family is one of the most abundant proteins found in the sandfly saliva.
We identified transcripts coding for secreted proteins of approximately 45 kDa, previously described in the saliva of L. longipalpis, P. papatasi and P. ariasi as yellow-related proteins 131421. In the P. argentipes cDNA library we found only one cluster (PagSP04) coding for this protein, yet in P. papatasi and L. longipalpis salivary glands there are multiple members of this family of proteins 33. Proteomic analysis (Figure 1A) revealed that the PagSP04 transcript (YHVEREYAWRNVTFEGVN) was one of the most abundant proteins found in the salivary glands of P. argentipes. Interestingly, three proteins with different mobilities coded for the same N-terminus sequence (Figure 1A) suggesting they may represent the same protein with different post-translational modifications.
Based on comparative analysis, we identified ten different sandfly salivary proteins that are members of the yellow family. Alignment of yellow proteins from Phlebotomus sandflies (P. argentipes, P. perniciosus, and P. ariasi), revealed a 43% identity and 79% similarity among the members of this protein family (Figure 6A). When the three yellow proteins from L. longipalpis were added, the identity was 21% identity and similarity was 57% among these proteins (Figure 6B). The phylogenetic analysis based on maximum likelihood using amino acid data of several MRJP/yellow proteins resulted in the formation of various clades (Figure 7), one clade containing yellow proteins from honeybees, a second clade containing mosquitoes and Drosophila, and a third clade containing the yellow proteins from sandflies. The sandfly clade was subdivided into three sub-clades, one containing the two yellow proteins from P. papatasi, the second clade containing the yellow proteins from P. ariasi and P. pernicious, and the third clade containing the L. longipalpis yellow proteins.
<p>Figure 6</p>
Multiple sequence analysis of yellow-related proteins from the salivary glands of different sandflies
Multiple sequence analysis of yellow-related proteins from the salivary glands of different sandflies. (A) Only Phlebotomus species were compared. (B) A combination of Phlebotomus and Lutzomyia sandfly salivary yellow-related proteins is shown on this alignment. Sequences were aligned using ClustalX and manually refined using BioEdit sequence-editing software.
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<p>Figure 7</p>
Phylogenetic tree analysis of yellow-related salivary proteins
Phylogenetic tree analysis of yellow-related salivary proteins. Yellow-related proteins from other organisms including S. invicta, An. Gambiae, A. mellifera, D. melanogaster and Ae. Aegypti. Phylogenetic analysis was conducted on protein alignments using Tree Puzzle version 5.2 by maximum likelihood using quartet puzzling, automatically estimating internal branch node support (1000 replications).
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Based on their MW, the yellow proteins from L. longipalpis appear to be the most recognised proteins from the sera of individuals living in endemic areas of visceral leishmaniasis and from individuals that have anti-Leishmania immunity 34. The antibody response against these salivary proteins appears to correlate with protection against leishmaniasis.
Antigen-5 family of proteins
This cluster codes for a secreted protein of 29 kDa similar to antigen 5-related protein found in wasp venom 35. Similar proteins have been isolated from the salivary glands of Aedes aegypti 20, An. gambiae 36 and from the salivary glands of L. longipalpis 13. We found only one cluster coding for this protein in the cDNA library of P. argentipes (PagSP05) and in the cDNA library of P. perniciosus (PpeSP07). The N-terminal sequence corresponding to these transcripts was identified in the salivary glands of P. argentipes (Figure 1A) and P. perniciosus (Figure 1B).
This family of proteins belong to the CAP family (CRISP, Ag5,PR-1) of proteins 3735. A remarkable feature of this family is the large number of cysteine residues, particularly at the carboxy-terminal region. X-ray structure of Na-AS-2, a member of this family from the human hookworm Necator americanus, was recently reported 38 and showed structural similarities to chemokines. Thus, it is possible that this type of protein in sandflies or other insects may bind cytokines with potential effects on the host immune response.
Multiple alignments of the antigen-5 protein from the sandflies indicated a 49% identity and 80% similarity (Figure 8A) with fourteen conserved cysteines. Phylogenetic analysis identified unique clades containing Hymenoptera, Culicidae, sandflies and mammals (Figure 8B). The only other organism included in the sandfly clade was the biting midge Culicoides sonorensis.
<p>Figure 8</p>
Analysis of antigen 5-related proteins
Analysis of antigen 5-related proteins. (A) Multiple sequence alignment of antigen 5 related proteins from the salivary glands of Phlebotomus argentipes (Pag), Phlebotomus ariasi (Par), Phlebotomus perniciosus (Ppe) and Lutzomyia longipalpis (LJ). Sequences were aligned using ClustalX and manually refined using BioEdit sequence-editing software. (B) Phylogenetic tree analysis of antigen 5-related protein from sandflies and other organisms, including A. Aegypti, A. Albopictus, A. stephensi, A. darlingi, A. gambiae, C. sonorensis, D. melanogaster, S. calcitrans, G. morsitans, C. quinquefasciatus, V. vidua, D. maculata, S. invicta, H. sapiens, R. novergicus, C. familiaris and G. gallus. Phylogenetic analysis was conducted on protein alignments using Tree Puzzle version 5.2 by maximum likelihood using quartet puzzling, automatically estimating internal branch node support (1000 replications).
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33-kDa protein family
The 33-kDa protein family does not appear to be related to any other known proteins found in GenBank. Phlebotomus ariasi and P. perniciosus, 33-kDa proteins, are more closely related to each other than to P. argentipes, whereas the 33-kDa protein from L. longipalpis is distant to the three Phlebotomus species (data not shown). In general, all four sequences are somewhat similar with only 34% shared amino acids (Figure 9). Without further investigation, the function of this protein is unknown.
<p>Figure 9</p>
Multiple sequence analysis of the 33-kDa protein family found on the salivary glands of sandflies
Multiple sequence analysis of the 33-kDa protein family found on the salivary glands of sandflies. Phlebotomus and Lutzomyia salivary proteins were used for this comparison. Sequences were aligned using ClustalX and manually refined using BioEdit sequence-editing software.
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Endonuclease family of proteins
Transcripts coding for an endonuclease-like protein were found in P. argentipes (PagSP11) and P. perniciosus (PpeSP32) salivary gland cDNA libraries. These transcripts code for a protein of approximately 40 kDa with similarities to non-specific endonucleases from the sandfly L. longipalpis 33, tse tse fly Glossina morsitans 39, and the mosquito Culex pipiens quinquefasciatus 40. This transcript does not have a direct match with the NUC Smart motif, which is indicative DNA/RNA non-specific endonucleases and phosphodiesterases, but it does have a high homology with other known endonucleases from other arthropods such as D. melanogaster (AAL13973) as well as non-insect arthropods such as P. camtschaticus (king crab) (AAN86143) and M. japonicus (prawn) (ACB55635) (Figure 10B).
<p>Figure 10</p>
Analysis of the endonuclease family of proteins
Analysis of the endonuclease family of proteins. (A) Multiple sequence analysis of salivary endonucleases from Phlebotomus and Lutzomyia sandflies. Sequences were aligned using ClustalX and manually refined using BioEdit sequence-editing software. (B) Phylogenetic tree analysis of endonucleases from sandflies and other organisms, including S. thypimurium, Anabaena sp., F. tularensis, H. pylori, S. serevisiae, M. musculus, H. sapiens, P. phaeoclathratiform, X. oryzar, Polaromonas sp., R. solanacearum, R. metallidurans, C. pippiens, G. morsitans, D. melanogaster, P. cantschaticus and M. japonicus. Phylogenetic analysis was conducted on protein alignments using Tree Puzzle version 5.2 by maximum likelihood using quartet puzzling, automatically estimating internal branch node support (1000 replications).
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Endonuclease proteins were found in all sandflies studied. The multiple alignment of sandfly endonuclease showed various regions of identity among amino acids, and many regions of conserved amino acids, even when comparing endonucleases from different sandfly genera (Figure 10A). Phylogenetic analysis indicated that the sandfly endonucleases clustered (92% bootstrap support) with other arthropods, including two non-insect arthropods (Paralithode camtschaticus and Marsupenaeus japonicus) (Figure 10B), however, sandfly endonucleases formed a distinct clade within the arthropod cluster (90% bootstrap support). Additionally, these endonucleases were clearly distant from other endonucleases. This suggests that this endonuclease may represent a common antigen for different sandflies and that the distant relationship to other endonucleases may avoid potential cross reactivity with non-insect organisms. Since this type of enzyme can cleave double- and single-stranded DNA, the role of this protein in the saliva of sandflies should be investigated further.
PpSP32-like protein
The PpSP32-like family of proteins is similar to the 32.4-kDa protein first identified in P. papatasi salivary glands 14. We found only one cluster (PagSP06) coding for this protein in the P. argentipes cDNA library. BLAST analysis of PagSP06 identified significant homology to L. longipalpis and P. papatasi PpSP32-like proteins. The P. perniciosus cDNA library contained only one cluster (PpeSP05) sharing identity with the PpSP32-like protein. Interestingly, upon BLAST analysis the PpSP32-like protein from P. perniciosus was found to be highly homologous to a Type VII collagen protein from Canis familiaris (E = 10-5) as well as a collagen from Mus musculus, Rattus norvegicus, Chinese hamster, and Bos taurus. This homology was found along approximately 74 amino acids (36% identity) and was dominated by conserved glycines and prolines (Figure 11).
<p>Figure 11</p>
Analysis of the PpSP32 protein family
Analysis of the PpSP32 protein family. (A) Multiple sequence analysis of PpSP32 like proteins from the salivary glands of Phlebotomus and Lutzomyia sandflies. (B) Multiple sequence alignment of Lutzomyia longipalpis salivary protein LJL04 and collagen adhesion proteins from B. thruingiensis and B. cereus. (C) Multiple sequence alignment of Phlebotomus perniciosus PpeSP05 and type VII collagen proteins from Canis familiairis, Mus musculus, Rattus norvegicus, Chinese hamster, and Bos Taurus. Sequences were aligned using ClustalX and manually refined using BioEdit sequence-editing software.
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The role of a collagen-like protein in sandfly salivary glands is unknown, yet intriguing. Because this protein may bind matrix protein, it is possible that this type of protein may form strong associations with basal matrix proteins. Within the Phlebotomus genera the relationship to collagen appears to be limited to PpSP32 kDa-like proteins from P. pernicious. P. papatasi and P. ariasi share only weak (non-significant) homology with Type VII collagen (E = 2.8 and 4.5, respectively) and P. argentipes did not match any collagen proteins upon multiple BLAST searches.
One explanation for the apparent homology between the four sandflies studied, yet lack of identity between collagen-related proteins in all sandflies, was revealed in the comparative analysis of the four sandflies. The majority of the homology between the four sandflies was found at the N- and carboxy terminus whereas the middle section of the protein appeared to be less conserved. The N-terminal and carboxy terminus has 43% and 23% identity between the four flies, respectively, whereas the midsection of the protein contains only 4% identity (Figure 11A). The region of homology between P. perniciosus and Type VII collagen was found in the non-homologous region of the protein (Figure 11B).
Additionally, BLAST analysis of L. longipalpis LJL04 (AAS16906) revealed a significant homology to collagen adhesion proteins from B. thuringiensis (ZP_00739782) and B. cereus (NP_830673) (Figure 11C). Again, the region of homology was found in the divergent section of the PpSP32-kDa protein. The most perplexing aspect of this family of proteins is that, although highly conserved among the four sandflies studied here, the N-terminal and carboxy regions of the protein have no homology to proteins of known function.
Perspectives on the evolution of hematophagy in sandflies
The presence of a specific gene in distantly related species could indicate a true orthologous relationship (i.e., the presence of the gene in the ancestral species) or acquisition of the gene by one of the species by horizontal gene transfer. While horizontal gene transfer is a common event in prokaryotes its provenance in eukaryotes is not well established and the general consensus is that its occurrence is rare, if present at all. In the case of sandflies this would imply that proteins present in evolutionary distant species (insects or other metazoans) were present in the ancestral sandfly. As such, two general trends can be observed for the sandfly protein families found in their transcriptomes. Firstly, those proteins that occur throughout the metazoans or insecta tend to be found as single members in all sandfly genera with no extensive gene duplication events occurring in sandflies. These proteins are generally well conserved and possibly share the same or a very similar function to those found in the main family. These proteins include the apyrase, antigen 5 and endonuclease families and probably consist of the core repertoire of the ancestral sandfly proteins that develop during adaptation to hematophagous behavior. Although yellow-related proteins and D7 proteins are generally well conserved, we observed some gene expansion of these proteins in sandflies (Figures 3 and 7).
Alternatively, a number of protein families are limited to sandflies as a group or specific species and show low levels of similarity to family members found in other insects. Members of this group show high levels of divergence, more gene duplication events and were probably evolved specifically during adaptation to a blood-feeding lifestyle and specific host species. Proteins in this category include the PSP15 like, PSP32 like, 32 kDa, 39 kDa and 16.1 kDa protein families (Table 3) Within this group can also be placed the singletons, which are proteins limited exclusively to single species (Table 4). In the case of the 39 kDa and 16.1 kDa families (Table 3), it is possible that gene losses occurred among selected sandfly species or the sequences or transcripts were missed on this analysis due to low representation of these transcripts in the sandflies studied. In the case of the 2- and 5-kDa salivary proteins only found in P. ariasi and P. perniciosus (Table 4), these proteins may be specific for the subgenus Larroussius. We found many transcripts in the P. argentipes and L. longipalpis cDNA libraries coding for proteins of similar MW, however with no significant homology to these two proteins.
As expected, we found that salivary proteins from sand flies belonging to the same subgenus are more closely related to each other than proteins from different subgenus. We observed that proteins belonging to P. ariasi (subgenus Larroussius) in all phylogenetic tree analysis based on protein sequence were more closely related to P. perniciosus (subgenus Larroussius) than to P. argentipes salivary proteins (subgenus Euphlebotomus). These results are in agreement with previously studies using the small subunit nuclear ribosomal DNA 12.