MOSAICISM OF TYROSINASE-LOCUS TRANSCRIPTION AND CHROMATIN STRUCTURE IN DARK VS LIGHT MELANOCYTE CLONES OF HOMOZYGOUS CHINCHILLA-MOTTLED MICE

被引:54
作者
PORTER, S [1 ]
LARUE, L [1 ]
MINTZ, B [1 ]
机构
[1] FOX CHASE CANC INST, INST CANC RES, 7701 BURHOLME AVE, PHILADELPHIA, PA 19111 USA
来源
DEVELOPMENTAL GENETICS | 1991年 / 12卷 / 06期
关键词
CLONAL VARIATION; GENE EXPRESSION; DNASE-I HYPERSENSITIVE SITES; MATRIX-ASSOCIATED REGIONS;
D O I
10.1002/dvg.1020120604
中图分类号
Q [生物科学];
学科分类号
07 ; 0710 ; 09 ;
摘要
The chinchilla-mottled (c(m)) mutation at the mouse tyrosinase-encoding locus leads to a transversely striped pattern of dark- and light-grey coat colors in homozygotes. The same basic pattern occurs in various other genotypes and has previously been found to represent the clonal developmental history of melanocytes. In a homozygote such as c(m)/c(m), cis-acting mechanisms would be expected to account for the color differences. To search for these mechanisms, the genomic structure of the mutation was examined and compared with the wild-type, and its function was compared in cultured melanocyte clones of the respective colors. Evidence from restriction mapping indicated that the coding region of the mutant gene resembles that of the fully and uniformly pigmented wild-type. However, the upstream sequences are rearranged in the mutation. The rearrangement begins 5 kb 5' of the transcription initiation site and is estimated to encompass at least 30 kb of distal upstream sequence. At least two stable functional states of the c(m) gene were detectable: Light-cell clones have low levels of tyrosinase-specific transcription, reduced DNAase I sensitivity of tyrosinase chromatin, and no detectable hypersensitive sites near the gene; dark-cell clones have higher (but subnormal) levels of transcription, greater sensitivity of chromatin to DNAase I, and a hypersensitive site in the promoter region. The changed relation between the structural gene and its upstream region may separate it from cis-acting control elements, resulting in reduced and variable ability to achieve the appropriate chromatin configuration near the time of melanocyte determination; differences in expression among clonal initiator cells are then mitotically perpetuated.
引用
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页码:393 / 402
页数:10
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