Abstract

We will address the fundamental role of bilateral symmetry in normal and abnormal cardiogenesis by anatomic, biochemical and genetic investigations of the autosomal recessive iv/iv mouse mutant. The iv/iv mouse is a recognized model of human situs inversus and polysplenia-asplenia syndrome, demonstrating random sidedness of the heart and other viscera, as well as a high frequency of cardiac malformations such as complete AV canal, transposition of the great arteries, and double outlet right ventricle. We will also utilize an experimental avian model. These models will permit us to make baseline studies of normal development as well as begin to discern the mechanisms that can cause human malformations, arteries, and double outlet right ventricle. Extrapolation to human congenital heart defects will utilize the availability of human autosomal recessive mutations whose phenotype parallels the mouse mutant. This work will have four main thrusts: 1. To determine paterns of inheritance of situs inversus and heterotaxia in selected inbred strains homozygous for iv. Particular attention will be paid to SWV-iv where the gene occasionally shows a dominant effect. 2. To identify polypeptides uniquely synthesized during determination of embryonic laterality and use them in an attempt to clone the gene. We will determine if the iv gene is linked to any homeo box cluster. We will construct a genic (cDNA) library from 8 day mouse embryos and attempt to isolate the iv gene from this library. 3. To discern the relation between gene action and cardiovascular morphogenesis. We will study the laterality of myocardial cytodifferentiation in d and l rotated (both genetic and experimental) hearts to see if the genetic program for myosin expression is reversed in l loop. Since these mice have a high incidence of CAVC (an endocardial cushion defect), the morphological consequences of expression of this gene will be examined in cushion development both morphologically and experimentally. 4. To test models of heart looping utilizing both the genetic defect and an experimental avian system.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
1R01HL037703-01
Application #
3353619
Study Section
(SRC)
Project Start
1986-09-30
Project End
1991-09-29
Budget Start
1986-09-30
Budget End
1987-09-29
Support Year
1
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
Dartmouth College
Department
Type
Schools of Medicine
DUNS #
041027822
City
Hanover
State
NH
Country
United States
Zip Code
03755

  Publications

Layton, W M; Layton, M W; Binder, M et al. (1993) Expression of the IV (reversed and/or heterotaxic) phenotype in SWV mice. Teratology 47:595-602
Van Keuren, M L; Iacob, R A; Kurnit, D M (1991) Analysis of proteins synthesized by 9.5 day mouse embryos: determination of cardiac and noncardiac proteins. Mol Reprod Dev 29:145-9
Van Keuren, M L; Iacob, R A; Kurnit, D M (1991) Analysis of proteins expressed at the time of murine organogenesis. Mol Reprod Dev 29:129-35
Van Keuren, M L; Layton, W M; Iacob, R A et al. (1991) Situs inversus in the developing mouse: proteins affected by the iv mutation (genocopy) and the teratogen retinoic acid (phenocopy). Mol Reprod Dev 29:136-44
Durbin, E J; Erickson, R P; Van Keuren, M L et al. (1991) Developmental appearance of proteins identified by two-dimensional gel electrophoresis in mouse gonadal tissue. Mol Reprod Dev 28:245-8
Hanzlik, A J; Binder, M; Layton, W M et al. (1990) The murine situs inversus viscerum (iv) gene responsible for visceral asymmetry is linked tightly to the Igh-C cluster on chromosome 12. Genomics 7:389-93
Stewart, G D; Van Keuren, M L; Galt, J et al. (1989) Molecular structure of human chromosome 21. Annu Rev Genet 23:409-23
Manasek, F J (1988) Retrospection and prognostication: ontogeny of a discipline. Experientia 44:971-4
Stewart, G D; Hassold, T J; Berg, A et al. (1988) Trisomy 21 (Down syndrome): studying nondisjunction and meiotic recombination by using cytogenetic and molecular polymorphisms that span chromosome 21. Am J Hum Genet 42:227-36
Stewart, G D; Hassold, T J; Kurnit, D M (1988) Trisomy 21. Molecular and cytogenetic studies of nondisjunction. Adv Hum Genet 17:99-140

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