Your search keyword '"Ming-Ding Li"' showing total 2 results

1. Restricted Expression of New HERV-K Members in Human Teratocarcinoma Cells

Author

David L. Bronson, Ming Ding Li, Anthony J. Faras, and Todd D. Lemke

Subjects

clone (Java method), Teratocarcinoma, viruses, Molecular Sequence Data, Biology, Polymerase Chain Reaction, Complementary DNA, Sequence Homology, Nucleic Acid, Virology, Tumor Cells, Cultured, Humans, Northern blot, RNA, Messenger, RNA, Neoplasm, Cloning, Molecular, Genetics, Base Sequence, Hybridization probe, Nucleic acid sequence, Nuclease protection assay, RNA Probes, Sequence Analysis, DNA, Molecular biology, Genes, pol, Gene Expression Regulation, Neoplastic, genomic DNA, Retroviridae, embryonic structures, DNA Probes

Abstract

Northern hybridization with five HERV-K family members, previously cloned from human teratocarcinoma genomic DNA, indicated that two (HERV-(K)27 and -(K)67) of the five clones are expressed in these teratocarcinoma cells. These two clones are closely related (98.49%), however, and Northern blot hybridization lacks the specificity to distinguish between their respective mRNAs. Therefore, PCR analysis with mixed oligonucleotide primers homologous to conserved retroviral pol gene regions was employed to amplify cDNA synthesized from teratocarcinoma cell RNA. This amplification scheme yielded two novel HERV-K family members, HERV-(K)55 and HERV-(K)91. Clone HERV-(K)55 has approximately 98% nucleotide sequence identity to clones HERV-(K)27 and -(K)67. Subsequent RNase protection assays confirmed the expression of HERV-(K)55 and indicated that clones HERV-(K)27 and -(K)67 were not expressed in these cells. One interpretation is that the HERV-(K)27 and -(K)67 probes detected transcripts of clone HERV-(K)55 or other closely-related elements because of their high homologies. In addition, clone HERV-(K)91, which has approximately 81% nucleotide sequence identity to clones HERV-(K)27, -(K)67, and -(K)55, was obtained only from teratocarcinoma 2102E-Pr cells, but the RNase protection assay showed that this clone is also expressed in other human teratocarcinoma cell lines.

Published

1995

2. Synthesis and analysis of a 640-bp pol region of novel human endogenous retroviral sequences and their evolutionary relationships

Author

Ming Ding Li, Todd D. Lemke, David L. Bronson, and Anthony J. Faras

Subjects

viruses, Molecular Sequence Data, Genome, Viral, Biology, Polymerase Chain Reaction, Homology (biology), law.invention, Cell Line, Mice, Plasmid, Phylogenetics, law, Virology, Tumor Cells, Cultured, Animals, Humans, Amino Acid Sequence, Gene, Polymerase chain reaction, Phylogeny, DNA Primers, Genetics, Phylogenetic tree, Base Sequence, Nucleic acid sequence, Molecular biology, Genes, pol, Retroviridae, GenBank, DNA, Viral

Abstract

Nucleotide sequence comparisons of the pol gene among 47 retroelements identified two very conserved regions, separated by a span of approximately 640 bp, that have not been previously reported. A set of mixed oligonucleotide primers, 5'-MOP-2 and 3'-MOP-2, homologous to these two conserved pol regions was constructed for use in detection of retroelements. When MOPs-2 were employed in PCR amplification studies, products of about 0.64 kb in size were amplified from human and mouse genomic DNAs and from HIV-1 proviral DNA, but not from negative control plasmid DNAs. The PCR products amplified with MOPs-2 from human LuC-1 teratocarcinoma cell DNA were subcloned and sequenced. Five clones of approximately 0.64 kb in size were identified, and sequence comparisons with all entries in GenBank indicated that these five clones have highest homology, in a range of 64.31 to 98.65%, with the corresponding pol region of HERV-K10 and HM-16 of the human endogenous retrovirus-K (HERV-K) family. Southern hybridizations at high stringency demonstrated that these five clones are present in all human DNAs tested. The evolutionary relationships of these clones with the equivalent pol region of other retroelements were defined by phylogenetic analyses that placed three clones into the HERV-K family and two clones into a new family of human endogenous retroelements. In addition, clone HERV-(K)73 contains the smaller PV1b pol segment that was reported to be selectively expressed in blood leukocytes of patients with polycythemia vera.

Published

1996