Journal article
Cellular survival in rat vein-to-artery grafts
Cell and Tissue Research, Vol.306(2), pp.251-256
2001
Abstract
Microsurgical models of vein-to-artery graft surgery have been developed in rats as a means of assessing vein graft adaptation and neo-intimal hyperplasia. Neo-intimal hyperplasia in these grafts is often attributed, at least in part, to an adaptive response by venous smooth muscle cells to the increased intraluminal pressure of the arterial pressure. However, considerable evidence suggests complete or near-complete cellular replacement in these grafts. A series of experiments were undertaken in which male vein or artery grafts were placed into either allogeneic female nude rat hosts or into syngeneic WKy female hosts as a means of determining donor cell survival. Grafts were removed at postsurgery week 2 or week 6 and the fate of the donor male cells assessed by PCR amplification of the testis-determining gene Sry. The Sry gene was undetectable in 2-week male to female vein grafts. When left for 6 weeks, donor cells were detectable in vein grafts only after multiple 50-cycle PCR analyses. Minimal donor cell survival was not due to an allograft response, as donor male cells were readily detectable in WKy male to female nude rat artery-to-artery grafts. These data were not nude rat specific, as poor donor cell survival was also evidenced in syngeneic male to female vein-to-artery grafts. In conclusion, we demonstrate only marginal survival of donor cells in rat vein-to-artery grafts. Neo-intimal hyperplasia in these grafts was not a consequence of donor venous smooth muscle cell proliferation.
Details
- Title
- Cellular survival in rat vein-to-artery grafts
- Authors/Creators
- A. Redwood (Author/Creator) - The University of Western AustraliaM. Tennant (Author/Creator) - The University of Western Australia
- Publication Details
- Cell and Tissue Research, Vol.306(2), pp.251-256
- Publisher
- Springer Verlag
- Identifiers
- 991005541167907891
- Murdoch Affiliation
- Murdoch University
- Language
- English
- Resource Type
- Journal article
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- 1 Clinical & Life Sciences
- 1.71 Cardiology - Circulation
- 1.71.242 Percutaneous Coronary Intervention
- Web Of Science research areas
- Cell Biology
- ESI research areas
- Molecular Biology & Genetics