Abstract

The Laboratory mouse is one of the more commonly used animal models in retinitis pigmentosa research. Small size, rapid breeding and short generation time make this species - the E. coli of mammalian genetics - ideal for experimental research into the genetic mechanisms related to visual cell development, function and decay. These are phenomena which are basic to the understanding of cause, pathogenesis and eventually remedial measures of the human disease. Of the various genes known to affect the retina in mice, two - rd (retinal degeneration) and rds (retinal degeneration slow) - affect the photoreceptor cell specifically; and thus simulate some of the clinical features of the human disease. It has been often felt that availability of these mutant genes in characterized and uniform genetic background will vastly increase the resolving power of any analysis undertaken into these systems, especially analysis at the cellular and molecular level. Accordingly, a program was initiated and as a result of sustained effort over the last fifteen years, four lines of congenic mice which carry rd, rds, both rd and rds, and their normal alleles had been produced in normal agouti coloured C3H and albino BALB/c strains of mice. This research proposal has four main objectives - (1) To propagate by programmed breeding the eight different congenic lines of mice with different allelic combination at the rd and rds loci, (2) To produce by extension breeding adequate and appropriate animal resources to provide tissue samples with different but specific genotypic combination which will be made available to other investigators interested to use the mouse model, (3) To undertake new breeding programmes to examine the effects of other gene loci on the expression of the rd and the rds genes; thus expanding the genetic repertoire of the available materials, and (4) To study the degeneration process in retinal explants in tissue and organ culture set-ups with the eventual aim of developing genetically defined in vitro systems. 70% of the grant support will be used in the fulfilment of objectives 1 and 2, the rest for the objectives 3 and 4. Since this proposal is believed to be a modest one, and furthermore, since Bramus University Rotterdam will not charge overhead, the aims of this project can hoped to be realized in a very cost effective way.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Eye Institute (NEI)
Type
Research Project--Cooperative Agreements (U01)
Project #
5U01EY006841-03
Application #
3551932
Study Section
Vision Research and Training Committee (VSN)
Project Start
1986-12-19
Project End
1989-09-29
Budget Start
1988-09-30
Budget End
1989-09-29
Support Year
3
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
Erasmus University of Rotterdam
Department
Type
DUNS #
City
Rotterdam
State
Country
Netherlands
Zip Code

  Publications

Caffe, A R; Soderpalm, A; van Veen, T (1993) Photoreceptor-specific protein expression of mouse retina in organ culture and retardation of rd degeneration in vitro by a combination of basic fibroblast and nerve growth factors. Curr Eye Res 12:719-26
Viczian, A; Sanyal, S; Toffenetti, J et al. (1992) Photoreceptor-specific mRNAs in mice carrying different allelic combinations at the rd and rds loci. Exp Eye Res 54:853-60
Jansen, H G; Sanyal, S (1992) Synaptic plasticity in the rod terminals after partial photoreceptor cell loss in the heterozygous rds mutant mouse. J Comp Neurol 316:117-25
Sanyal, S; Hawkins, R K; Jansen, H G et al. (1992) Compensatory synaptic growth in the rod terminals as a sequel to partial photoreceptor cell loss in the retina of chimaeric mice. Development 114:797-803
Schalken, J J; Janssen, J J; Sanyal, S et al. (1990) Development and degeneration of retina in rds mutant mice: immunoassay of the rod visual pigment rhodopsin. Biochim Biophys Acta 1033:103-9
Tawara, A; Hollyfield, J G (1990) Proteoglycans in the mouse interphotoreceptor matrix. III. Changes during photoreceptor development and degeneration in the rds mutant. Exp Eye Res 51:301-15
Cantera, R; von Schantz, M; Chader, G J et al. (1990) Postnatal development of photoreceptor-specific proteins in mice with hereditary retinal degeneration. An immunocytochemical study. Exp Biol 48:305-12
Jansen, H G; Aguirre, G D; van Veen, T et al. (1990) Development and degeneration of retina in rds mutant mice: ultraimmunohistochemical localization of S-antigen. Curr Eye Res 9:903-11
Sanyal, S; Hawkins, R K (1989) Development and degeneration of retina in rds mutant mice: altered disc shedding pattern in the heterozygotes and its relation to ocular pigmentation. Curr Eye Res 8:1093-101
Caffe, A R; Visser, H; Jansen, H G et al. (1989) Histotypic differentiation of neonatal mouse retina in organ culture. Curr Eye Res 8:1083-92

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