We thank Dr. Clark Riley, Ms. Carol Davenport, and Ms. Jani ne Ptak for synthetic oligonucleotides; Dr. Keith Fry for the gift of mAb ABS; Ms. Cathy Blizzard for cat eyes; Dr. Mark Molliver for donating fixed monkey eyes; Drs. Masafumi Tanaka and Wi nshi p Herr for Oct.1 cDNA; Mr. Hao Zhou for the GST-Ott-1 POU domain protein; Dr. Y.-W. Peng for rabbit retinas and Dr. Hua-Shun Li for chicken retinas; Dr. Elio Ravi ol a for advice on histologic techniques; and Drs. Robert Rodieck, Jen-Chi h Hsieh, and King-wai Yau for hel pful comments on the manuscript.
The hypothesis that red-green "color blindness" is caused by alterations in the genes encoding red and green visual pigments has been tested and shown to be correct. Genomic DNA's from 25 males with various red-green color vision deficiencies were analyzed by Southern blot hybridization with the cloned red and green pigment genes as probes. The observed genotypes appear to result from unequal recombination or gene conversion (or both). Together with chromosome mapping experiments, these data identify each of the cloned human visual pigment genes.
The amino-acid sequence of the precursor of the human tumour cell line-derived platelet-derived growth factor (PDGF) A-chain has been deduced from complementary DNA clones and the gene localized to chromosome 7. The protein shows extensive homology to the PDGF B-chain precursor. Expression of the PDGF A-chain gene is independent of that of the PDGF B-chain in a number of human tumour cell lines, and secretion of a PDGF-like growth factor of relative molecular mass 31,000 correlates with expression of A- but not B-chain messenger RNA.
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