Abstract
Collectins are pattern recognition molecules of the innate immune system showing binding to carbohydrate structures on microorganisms in a calcium-dependent manner. Recently, three novel collectins, collectin liver 1 (CL-L1), collectin kidney 1 (CL-K1 and CL-11), and collectin placenta 1 (CL-P1), were discovered. The roles of these three collectins remain largely unknown. Here, we present a time-resolved immunofluorometric assay for quantification of CL-L1. The concentration of CL-L1 in donor plasma (n = 210) was distributed log-normally with a median value of 3.0 μg/ml (range 1.5-5.5 μg/ml). We observed on average 30% higher concentrations of CL-L1 in plasma as compared with serum. Size analysis by gel-permeation chromatography showed CL-L1 in serum to elute as large 700-800-kDa complexes and smaller 200-300-kDa complexes. CL-L1 showed specific binding to mannose-TSK beads in a Ca(2+)-dependent manner. This binding could be inhibited by mannose and glucose, but not galactose, indicating that CL-L1 binds via its carbohydrate-recognition domain and has ligand specificity similar to that of mannan-binding lectin. Western blot analysis of CL-L1 showed the presence of several oligomeric forms in serum. Ontogeny studies showed CL-L1 to be present at birth at near adult levels. CL-L1 levels exhibit low variation in healthy adults over a 1-year period. During acute-phase responses, the CL-L1 levels display only minor variations. In serum, CL-L1 was found in complexes with mannan-binding lectin-associated serine proteases, suggesting a role in the lectin pathway of complement activation. The presented data establish a basis for future studies on the biological role of CL-L1.
Highlights
The collectin collectin liver 1 (CL-L1) is a pattern recognition molecule of the innate immune system
Both Monoclonal Antibodies (mAb) and Polyclonal Antibodies (pAb) were raised against two different synthetic peptides representing the N-terminal cross-linking region (CLR) and carbohydrate recognition domain (CRD) of CL-L1 (Fig. 1A)
CL-L1, known as collectin 10 or COLEC-10, was described as a C-type lectin some years ago [6], but it has since escaped the attention of the scientific community
Summary
The collectin CL-L1 is a pattern recognition molecule of the innate immune system. Results: Several biological parameters are established and furnish a basis for continued investigations. Collectins are pattern recognition molecules of the innate immune system showing binding to carbohydrate structures on microorganisms in a calcium-dependent manner. CL-L1 showed specific binding to mannose-TSK beads in a Ca2؉-dependent manner This binding could be inhibited by mannose and glucose, but not galactose, indicating that CL-L1 binds via its carbohydrate-recognition domain and has ligand specificity similar to that of mannan-binding lectin. C-type lectins bind, in a calcium-dependent manner, to targets presenting ligands with adequately spaced terminal carbohydrate groups [1]. We present an assay for the measurement of CL-L1, and we use this assay to establish the levels of the protein in serum, size, and composition of the complexes, ontogeny, and acute phase reaction, and we analyze the lectin activity of CL-L1
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