CAARD:Pepsins A1a d2

Ancestral ML reconstructions were performed using FastML 2.02 (Pupko et al. 2000). The tool generates six outputs:

• Pin; reconstructed ancestral NJ tree in newick format.
• Fin; parental relationship among reconstructed nodes and contemporary sequences.
• Jrof; multiple alignment of contemporary sequences and nodes reconstructed with the Joint method.
• Jpf; joint probability per position and total log likelihood.
• Mrof; multiple alignment of contemporary sequences and nodes reconstructed with the marginal method
• Mpf; marginal probability and total log likelihood

There are two methods of ancestral reconstruction - Joint and Marginal. In this section, we provide a multiple alignment including both input peptidases and ancestral ML sequences reconstructed using the Joint method.The alignment is available in several formats clicking below the option "Set 1". To build HMM profiles and MRC sequences we removed non-informative amino acid stretches and gaps from several ancestral ML reconstruction analyses You can also retrieve the processed Jrof output, clicking below the option "Set 2". Note however that should you cannot select option 2 is because the output was not processed. <align id="pepsins_a1a_d2" folder="jrof"></align>

There are two methods of ancestral reconstruction - Joint and Marginal. In this section, we provide a multiple alignment including both input peptidases and ancestral ML sequences reconstructed using the Joint method.The alignment is available in several formats clicking below the option "Set 1". To build HMM profiles and MRC sequences we removed non-informative amino acid stretches and gaps from several ancestral ML reconstruction analyses You can also retrieve the processed Jrof output, clicking below the option "Set 2". Note however that should you cannot select option 2 is because the output was not processed. <align id="pepsins_a1a_d2" folder="mrof"></align>

Sequence logo constructed from the input of the processed Jrof alignment. In every position, each residue is a letter whose height is proportional to its frequency multiplied by the information content of each position measured in bits. Letters are placed such that the most common is at the top.

• Basic residues are represented in red
• Hydrophobic residues in black
• Amino acids frequent in β-turns (G and P) in dark grey
• Small nucleophiles in violet
• Acidic residues in orange
• Acidic-relative amides in green

The logo was constructed using ChekAlign server with the Shannon's algorithm (Shannon 1997) and options "include gaps" and "Correction factor". Gaps are not represented by any symbol but occupy a blank also proportional to its frequency and, for aesthetic reasons, always at the top. Maximum entropy is log₂21. The alignment gap is considered to be another state or amino acid species.

>AP_pepsins_a1a_d2 profile HMM generated consensus sequence
vDTGTSLitgPssvvqalqkaiGAtessdgeYvvnCskintLPtitFtlgGkqytLpps
dYvlqvsGiClsGfggmDipplwILGDvFlrkyYtVFDrdnnrVGF

         Domain 1 of 1, from 1 to 98: score 40.9, E = 4.8e-13

DTG_ILG template *->vDTGAsvlsviskecklaqklgltrkkafdp..SS...Y.v.C..iv
                    vDTG+s+++ +s  + +a++++      +++++SS+++Y v+C++i+
AP_pepsins     1    VDTGTSLITGPSSVV-QALQKA------IGAteSSdgeYvVnCskIN 40   

                 tllsysqPssktsttaqdtirgagGqskiyvSklktsgqirknllslvti
                      ++P+  ++      + + gG  k+y    + +++       ++ +
AP_pepsins    41 -----TLPT--IT------F-TLGG--KQY----TLPPS-------DYVL 63   

                 kitkGnvTevenrslpsdgvflvv.tdpedqksrydvILGrldfLrqlns
                 ++  G       +  +    f    ++p      + +ILG+  fLr++++
AP_pepsins    64 QVS-G------ICLSG----F-GGmDIP------PLWILGD-VFLRKYYT 94   

                 vhidl<-*
                 v +d+   
AP_pepsins    95 V-FDR    98