Abstract

Systematic analyses of transcripts in early embryogenesis by the group of Dr. M. Ko (q.v. in these Annual Reports) have uncovered a relative dearth of X-linked genes. Nevertheless, 15 X-linked genes showed a high level of expression. Two of these have been chosen for special study.One, isolated as a cDNA from the ectoplacental cone (that is, the first tissue that gives rise to placenta) turns out to be a previously unisolated member of the Bex family, Bex-3. The transcribed sequence is 789 bp in length and encodes a protein of 124 residues with a CAAX motif at its C-terminal end. It appears in a single cDNA and Northern species of 1.1 kb. Expression declines after the fetal period, but adult mouse and human show sustained expression in several organs, including brain, testis and ovary. The putative Bex-3 amino acid sequence shows very high homology to a partially characterized human cDNA clone called pHGR74, which is associated with spontaneous ovarian granulosa cell carcinoma. In vitro-expressed Bex3 is attached to the plasma membrane, and we are examining the possibility that it may be involved in signal transduction during mouse development.The second gene is an ortholog of an X-linked human gene, ZNF127-Xp, which had been partially recovered in cDNA form and shown to escape X-inactivation. The mouse gene is expressed at increasingly high levels as development proceeds, with mRNA species of 3.4, 1.9 and 0.8 kb detected in several tissues; in adult mouse and human, the largest cDNA species shows especially marked expression in testis. Sequencing of the full-length 1.9 kb cDNA species recombinant GST-RING protein constructs revealed a putative protein of 515 amino acids, containing 4 C3H motifs, 1C2H2CH motif and near the carboxy terminus, a RING-finger motif(C3HC4). Cell expression of recombinant GST-RING protein constructs show that the C-terminal portion is associated with cytoskeletal or nuclear matrix fractions, and we are continuing to examine specific attachment partners as a start toward understanding its function.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Intramural Research (Z01)
Project #
1Z01AG000658-01
Application #
6413974
Study Section
National Institute on Aging Initial Review Group (NIA)
Project Start
Project End
Budget Start
Budget End
Support Year
1
Fiscal Year
2000
Total Cost
Indirect Cost

  Institution

Name
Aging
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Kim, Ae-Jung; Lee, Cheol-Soon; Schlessinger, David (2004) Bex3 associates with replicating mitochondria and is involved in possible growth control of F9 teratocarcinoma cells. Gene 343:79-89
Sharov, Alexei A; Piao, Yulan; Matoba, Ryo et al. (2003) Transcriptome analysis of mouse stem cells and early embryos. PLoS Biol 1:E74
Fant, Michael; Weisoly, David L; Cocchia, Massimo et al. (2002) PLAC1, a trophoblast-specific gene, is expressed throughout pregnancy in the human placenta and modulated by keratinocyte growth factor. Mol Reprod Dev 63:430-6
Chiao, Eric; Fisher, Peter; Crisponi, Laura et al. (2002) Overgrowth of a mouse model of the Simpson-Golabi-Behmel syndrome is independent of IGF signaling. Dev Biol 243:185-206
Toretsky, J A; Zitomersky, N L; Eskenazi, A E et al. (2001) Glypican-3 expression in Wilms tumor and hepatoblastoma. J Pediatr Hematol Oncol 23:496-9
Schlessinger, D; Van Zant, G (2001) Does functional depletion of stem cells drive aging? Mech Ageing Dev 122:1537-53
Khan, S; Blackburn, M; Mao, D L et al. (2001) Glypican-3 (GPC3) expression in human placenta: localization to the differentiated syncytiotrophoblast. Histol Histopathol 16:71-8
Mumm, S; Herrera, L; Waeltz, P W et al. (2001) X/autosomal translocations in the Xq critical region associated with premature ovarian failure fall within and outside genes. Genomics 76:30-6
Cocchia, M; Huber, R; Pantano, S et al. (2000) PLAC1, an Xq26 gene with placenta-specific expression. Genomics 68:305-12
Ciccodicola, A; D'Esposito, M; Esposito, T et al. (2000) Differentially regulated and evolved genes in the fully sequenced Xq/Yq pseudoautosomal region. Hum Mol Genet 9:395-401