Please use this identifier to cite or link to this item: http://hdl.handle.net/2440/17233
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Type: Journal article
Title: Understanding cellular disruptions during early embryo development that perturb viability and fetal development
Author: Lane, M.
Gardner, D.
Citation: Reproduction Fertility and Development, 2005; 17(3):371-378
Publisher: C S I R O Publishing
Issue Date: 2005
ISSN: 1031-3613
1448-5990
Abstract: An inability to regulate ionic and metabolic homeostasis is related to a reduction in the developmental capacity of the embryo. The early embryo soon after fertilisation and up until compaction appears to have a reduced capacity to regulate its homeostasis. The reduced ability to regulate homeostasis, such as intracellular pH and calcium levels, by the precompaction-stage embryo appears to impact on the ability to regulate mitochondrial function and maintain adequate levels of energy production. This reduction in ATP production causes a cascade of events leading to disrupted cellular function and, perhaps ultimately, disrupted epigenetic regulation and aberrant placental and fetal development. In contrast, after compaction the embryo takes on a more somatic cell-like physiology and is better able to regulate its physiology and therefore appears less vulnerable to stress. Therefore, for human IVF it would seem important for the establishment of healthy pregnancies that the embryos are maintained in systems that are designed to minimise homeostatic stress, particularly for the cleavage-stage embryos, as exposure to stress is likely to culminate in impaired embryo function.
Keywords: Mitochondria; Animals; Humans; Calcium; Adenosine Triphosphate; Fertilization in Vitro; Embryo Culture Techniques; Energy Metabolism; Embryonic Development; Fetal Viability; Homeostasis; Hydrogen-Ion Concentration; Stress, Physiological
RMID: 0020050104
DOI: 10.1071/RD04102
Published version: http://www.publish.csiro.au/nid/44/paper/RD04102.htm
Appears in Collections:Obstetrics and Gynaecology publications

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