Abstract
A procedure has been developed which is much more specific for the solubilization of the elastin-associated microfibrils from fetal bovine nuchal ligament using treatment with reductive saline in place of reductive guanidine hydrochloride buffer. When analyzed by sodium dodecyl sulfate-polyacrylamide gel electrophoresis, reductive saline extracts were shown to contain only five major protein bands with Mrs of 340,000, 78,000, 70,000, 31,000, and 25,000. The 31-kDa species was identified immunologically as the previously described macromolecule named microfibril-associated glycoprotein (MAGP) (Gibson, M. A., Hughes, J. L., Fanning, J. C., and Cleary, E. G. (1986) J. Biol. Chem. 261, 11429-11436). The proteins were purified by gel permeation, ion exchange, and affinity chromatography. Amino acid analyses showed that each protein had a profile which was distinct from that of MAGP although each was also high in acidic amino acids and cystine. The 340- and 78-kDa species were each demonstrated by immunoelectron microscopy with affinity-purified antibodies to be derived from the elastin-associated microfibris, and these were provisionally named microfibrillar protein 340 (MP340) and microfibrillar protein 78 (MP78), respectively. Each of the above antibodies gave a tissue distribution identical to that of anti-MAGP antibodies, and thus MP340 and MP78 also were identified with the 12-nm microfibrils of nonelastic tissues. MP340 was shown to absorb out completely the microfibrillar immunoreactivity of anti-(reductive guanidine hydrochloride extract) antibodies, indicating that MP340 was (a) the major microfibrillar constituent in these extracts and (b) the second unidentified microfibrillar antigen described previously. The relationship of the 70- and 25-kDa proteins to microfibrils is yet to be established. Immunoblot and immunoabsorption studies showed that MAGP and MP78 were immunologically related to MP340 but not to each other. Cyanogen bromide peptide mapping indicated that MAGP was structurally related to MP340. It is postulated that MAGP and MP78 are constituents of MP340 which in turn is the subunit of which the 12-nm microfibrils are composed.
Highlights
A procedure hasbeen developed which is much more lung, and skin [1, 2]
The results suggest that microfibrillar protein 340 (MP340) is immunologicallyrelated to MAGP and toMP78 and/or SD70
The results indicate that both MAGP and microfibrillar protein 78 (MP78) are related immunochemically to MP340 butnotto each other
Summary
Nuchal ligament tissue (approximately 50 g, wet weight) from 210250-day-old fetal calves was finely crushed as described previously [17]. MP340 was eluted as a single peak (10 ml) with the same buffer to which mannitol had been added to 100 mM This peak was concentrated over an Amicon YM30 ultrafiltration membrane to 3 ml and was applied directly to a Sepharose CL-4B gel filtration column (150 X 1.6 cm) equilibrated in 4 M GdnHCl column buffer [18].Flow rate was 4 ml/h, and 4-ml fractions were collected. Fractions containingpolypeptides MP78 and SD70 as eluted from DEAE-cellulose were concentrated over a YM-30 membrane to 1.25 ml and applied directly to a Sephacryl S-300 gel filtration column (120 X 1.0 cm) equilibrated in 4 M GdnHCl column buffer [18].Flow rate was 2 ml/h, and 1-ml fractions were collected.
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