analysis and prediction of cancerlectins using evolutionary and domain information分析和预测cancerlectins使用进化和域信息.pdfVIP
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analysis and prediction of cancerlectins using evolutionary and domain information分析和预测cancerlectins使用进化和域信息
Kumar et al. BMC Research Notes 2011, 4:237
/1756-0500/4/237
RESEARCH ARTICLE Open Access
Analysis and prediction of cancerlectins using
evolutionary and domain information
*
Ravi Kumar, Bharat Panwar, Jagat S Chauhan and Gajendra PS Raghava
Abstract
Background: Predicting the function of a protein is one of the major challenges in the post-genomic era where a large
number of protein sequences of unknown function are accumulating rapidly. Lectins are the proteins that specifically
recognize and bind to carbohydrate moieties present on either proteins or lipids. Cancerlectins are those lectins that play
various important roles in tumor cell differentiation and metastasis. Although the two types of proteins are linked, still
there is no computational method available that can distinguish cancerlectins from the large pool of non-cancerlectins.
Hence, it is imperative to develop a method that can distinguish between cancer and non-cancerlectins.
Results: All the models developed in this study are based on a non-redundant dataset containing 178
cancerlectins and 226 non-cancerlectins in which no two sequences have more than 50% sequence similarity. We
have applied the similarity search based technique, i.e. BLAST, and achieved a maximum accuracy of 43.25%. The
amino acids compositional analysis have shown that certain residues (e.g. Leucine, Proline) were preferred in
cancerlectins whereas some other (e.g. Asparatic acid, Asparagine) were preferred in non-cancerlectins. It has been
found that the PROSITE domain “Crystalline beta gamma” was abundant in cancerlectins whereas domains like
“SUEL-type lectin domain” were found mainly in non-cancerlectins. An SVM-based model has been developed to
differentiate between the cancer and non-ca
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