The discovery, reported in the journal Nature Communications, challenges two centuries of dogma -- originating at around 1827, when early embryologists first observed mammal eggs -- claiming that only an egg cell is capable of reprogramming sperm to permit the development of a mammal embryo.
Ironically, the new research that could empower men builds on a phenomenon known as parthenogenesis, aka "virgin birth," which has been documented in a number of species, such as certain fish, reptiles, insects and amphibians, but not in mammals. When such births occur, an embryo develops from an unfertilized egg cell, allowing females to reproduce without males.
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| Komodo dragon, which can reproduce by parthenogenesis. |
For the recent study, scientists overcame this problem by developing a method of injecting mouse parthenogenotes (which consist of mitotic cells, meaning cells that divide to form two identical cells) with sperm (which is a differentiated, or specialized, cell). The outcome resulted in healthy baby mice, with a success rate of about 24 percent.
"This work shows for the first time that a mitotic cell can completely reprogram a differentiated cell, with the outcome being the birth of live young," senior author Anthony Perry, a molecular embryologist at the University of Bath, told Discovery News. "Yes, the cells are special -- a parthenogenote and a sperm -- but imagine if any mitotic cell could reprogram a sperm in the same way. Then there would be no need for eggs."
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| Sperm moving toward an egg. |
For now, mammal males -- including men -- still need females for reproduction and vice versa because, even for this research, the parthenogenetic mice embryos were produced from eggs contributed by females, and females carried the pregnancies to term.
Many unknowns still exist. It's not clear how sperm are able to be reprogrammed to allow for embryonic development with an egg cell, much less without one, as for the new process.
Read more at Discovery News
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