Molecular cloning of a member of the gene family that encodes pMGA, a hemagglutinin of Mycoplasma gallisepticum.

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Infect Immun. 1993 March; 61(3): 903-909

Molecular cloning of a member of the gene family that encodes pMGA, a hemagglutinin of Mycoplasma gallisepticum.

P F Markham, M D Glew, K G Whithear and I D Walker

School of Veterinary Science, University of Melbourne, Victoria, Australia.

ABSTRACT

A hemagglutinin with an M(r) of 67,000 (pMGA) from Mycoplasmagallisepticum S6 was purified by using monoclonal antibody affinitychromatography. Purified pMGA was treated with a number of enzymes,the resultant peptides were purified, and their amino acid sequencewas determined by using an Applied Biosystems (model 471A) proteinsequencer. The DNA sequence encoding two peptides was used todictate the sequences of synthetic oligonucleotides which wereused to screen a library of EcoRI-cut M. gallisepticum DNA inpUC18. A clone reactive to both probes was isolated and foundto contain a recombinant insert of 10 kb. The clone was mappedby using restriction endonucleases and fragments subcloned intopUC18 for DNA sequencing. Analysis of part of the DNA sequencerevealed an open reading frame containing 1,941 nucleotideswhich encoded 647 amino acids. The amino terminus was precededby a putative leader sequence of 25 amino acids. A promoterregion preceding the putative start codon GUG was also located.This gene would encode a mature protein of 67,660 Da. Therewere a number of differences between the predicted amino acidsequence and that determined by direct peptide sequencing. Also,two tryptic peptides of pMGA were not found in the DNA sequence.This suggested that the cloned gene did not encode pMGA butdid encode a homolog (pMGA1.2). Furthermore, downstream of pMGA1.2was a region of DNA encoding a leader sequence followed by anamino acid sequence with high homology to that encoded by thepMGA1.2 gene. The presence within M. gallisepticum of a familyof pMGA genes is inferred from the DNA sequence and Southerntransfer data. A possible role for this gene family in immuneevasion is discussed.

Infect Immun. 1993 March; 61(3): 903-909

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