Chimera (genetics)

This article is about genetic chimærism. For the cartilaginous fish, see Chimaera. For the mythological beast, see Chimera (mythology).
A chimeric mouse with its offspring

A genetic chimerism or chimera (also spelled chimaera) is a single organism composed of cells from different zygotes. This can result in male and female organs, two blood types, or subtle variations in form.[1] Animal chimeras are produced by the merger of multiple fertilized eggs. In plant chimeras, however, the distinct types of tissue may originate from the same zygote, and the difference is often due to mutation during ordinary cell division. Normally, genetic chimerism is not visible on casual inspection; however, it has been detected in the course of proving parentage.[2]

Another way that chimerism can occur in animals is by organ transplantation, giving one individual tissues that developed from two genomes. For example, a bone marrow transplant can change someone's blood type.

Animals

An animal chimera is a single organism that is composed of two or more different populations of genetically distinct cells that originated from different zygotes involved in sexual reproduction. If the different cells have emerged from the same zygote, the organism is called a mosaic. Chimeras are formed from at least four parent cells (two fertilised eggs or early embryos fused together). Each population of cells keeps its own character and the resulting organism is a mixture of tissues. There are some reports of human chimærism.[1]

This condition is either inherited or it is acquired through the infusion of allogeneic hematopoietic cells during transplantation or transfusion. In nonidentical twins, chimerism occurs by means of blood-vessel anastomoses. The likelihood of offspring being a chimera is increased if it is created via in vitro fertilisation.[3] Chimeras can often breed, but the fertility and type of offspring depends on which cell line gave rise to the ovaries or testes; varying degrees of intersex differences may result if one set of cells is genetically female and another genetically male.

Tetragametic chimærism

Tetragametic chimerism is a form of congenital chimærism. This condition occurs through the fertilisation of two separate ova by two sperm, followed by aggregation of the two at the blastocyst or zygote stages. This results in the development of an organism with intermingled cell lines. Put another way, the chimera is formed from the merging of two nonidentical twins (although a similar merging presumably occurs with identical twins, but as their DNA is almost identical, the presence would not be immediately detectable in a very early (zygote or blastocyst) phase). As such, they can be male, female, or have mixed intersex characteristics.

As the organism develops, it can come to possess organs that have different sets of chromosomes. For example, the chimera may have a liver composed of cells with one set of chromosomes and have a kidney composed of cells with a second set of chromosomes. This has occurred in humans, and at one time was thought to be extremely rare, though more recent evidence suggests that it is not as rare as previously believed.[1][4]

This is particularly true for the marmoset. Recent research shows most marmosets are chimeras, sharing DNA with their fraternal twins.[5] 95% of Marmoset fraternal twins trade blood through chorionic fusions, making them hematopoietic chimeras.[6][7]

Most chimeras will go through life without realizing they are chimeras. The difference in phenotypes may be subtle (e.g., having a hitchhiker's thumb and a straight thumb, eyes of slightly different colors, differential hair growth on opposite sides of the body, etc.) or completely undetectable. Chimeras may also show, under a certain spectrum of UV light, distinctive marks on the back resembling that of arrow points pointing downwards from the shoulders down to the lower back; this is one expression of pigment unevenness called Blaschko's lines.[8]

Affected persons may be identified by the finding of two populations of red cells or, if the zygotes are of opposite sex, ambiguous genitalia and intersex alone or in combination; such persons sometimes also have patchy skin, hair, or eye pigmentation (heterochromia). If the blastocysts are of opposite sex, genitals of both sexes may be formed: either ovary and testis, or combined ovotestes, in one rare form of intersex, a condition previously known as true hermaphroditism.

Note that the frequency of this condition does not indicate the true prevalence of chimerism. Most chimeras composed of both male and female cells probably do not have an intersex condition, as might be expected if the two cell populations were evenly blended throughout the body. Often, most or all of the cells of a single cell type will be composed of a single cell line, i.e. the blood may be composed predominantly of one cell line, and the internal organs of the other cell line. Genitalia produce the hormones responsible for other sex characteristics. If the sex organs are homogeneous, the individual will not be expected to exhibit any intersex traits.

Natural chimeras are almost never detected unless they exhibit abnormalities such as male/female or hermaphrodite characteristics or uneven skin pigmentation. The most noticeable are some male tortoiseshell cats or animals with ambiguous sex organs.

The existence of chimerism is problematic for DNA testing, a fact with implications for family and criminal law. The Lydia Fairchild case, for example, was brought to court after DNA testing apparently showed that her children could not be hers. Fraud charges were filed against her and her custody of her children was challenged. The charge against her was dismissed when it became clear that Lydia was a chimera, with the matching DNA being found in her cervical tissue. Another case was that of Karen Keegan, who was also suspected (initially) of not being her children's biological mother, after DNA tests on her adult sons for a kidney transplant she needed seemed to show she wasn't their mother.[1][9]

The tetragametic state has important implications for organ or stem-cell transplantation. Chimeras typically have immunologic tolerance to both cell lines.

Microchimerism

Main article: Microchimerism

Microchimerism is the presence of a small number of cells that are genetically distinct from those of the host individual. Most people are born with a few cells genetically identical to their mothers' and the proportion of these cells goes down in healthy individuals as they get older. People who retain higher numbers of cells genetically identical to their mothers' have been observed to have higher rates of some autoimmune diseases, presumably because the immune system is responsible for destroying these cells and a common immune defect prevents it from doing so and also causes autoimmune problems. The higher rates of autoimmune diseases due to the presence of maternally-derived cells is why in a 2010 study of a 40 year old man with scleroderma-like disease (an autoimmune rheumatic disease), the female cells detected in his blood stream via FISH (fluorescence in situ hybridization) were thought to be maternally-derived. However, his form of microchimerism was found to be due to a vanished twin, and whether or not microchimerism from a vanished twin might predispose individuals to autoimmune diseases as well is unknown.[10] Women often also have a few cells genetically identical to that of their children, and some people also have some cells genetically identical to that of their siblings (maternal siblings only, since these cells are passed to them because their mother retained them).

Symbiotic chimerism in anglerfish

Chimerism occurs naturally in adult Ceratioid anglerfish and is in fact a natural and essential part of their life cycle. Once the male achieves adulthood, it begins its search for a female. Using strong olfactory receptors (i.e. smell receptors), the male searches until it locates a female anglerfish. The male, less than an inch in length, bites into her skin and releases an enzyme that digests the skin of his mouth and her body, fusing the pair down to the blood-vessel level. While this attachment has become necessary for the male's survival, it will eventually consume him, as both anglerfish fuse into a single hermaphroditic individual. Sometimes in this odd ritual, more than one male will attach to a single female as a symbiote. They will all be consumed into the body of the larger female angler. Once fused to a female, the males will reach sexual maturity, developing large testicles as their other organs atrophy. This process allows for sperm to be in constant supply when the female produces an egg, so that the chimeric fish is able to have a greater number of offspring.[11]

Germline chimerism

Germline chimerism occurs when the germ cells (for example, sperm and egg cells) of an organism are not genetically identical to its own. It has recently been discovered that marmosets can carry the reproductive cells of their (fraternal) twin siblings, because of placental fusion during development. (Marmosets almost always give birth to fraternal twins.)[5][12][13]

Humans

Research

In biological research, chimeras are artificially produced by selectively transplanting embryonic cells from one organism onto the embryo of another, and allowing the resultant blastocyst to develop. Chimeras are not hybrids, which form from the fusion of gametes from two species that form a single zygote with a combined genetic makeup, or Hybridomas which, as with hybrids, result from fusion of two species' cells into a single cell and artificial propagation of this cell in the laboratory. Essentially, in a chimera, each cell is from either of the parent species, whereas in a hybrid and hybridoma, each cell is derived from both parent species. "Chimera" is a broad term and is often applied to many different mechanisms of the mixing of cells from two different species.

As with cloning, the process of creating and implanting a chimera is imprecise, with the majority of embryos spontaneously terminating. Successes, however, have led to major advancements in the field of embryology, as creating chimeras of one species with different physical traits, such as colour, has allowed researchers to trace the differentiation of embryonic cells through the formation of organ systems in the adult individual.

The first known primate chimeras are the rhesus monkey twins Roku and Hex; each having 6 genomes. They were created by mixing cells from totipotent 4 cell blastocysts; although the cells never fused they worked together to form organs. It was discovered that one of these primates, Roku, was a sexual chimera; as four percent of Roku's blood cells contained two x chromosomes.[6]

A major milestone in chimera experimentation occurred in 1984, when a chimeric geep was produced by combining embryos from a goat and a sheep, and survived to adulthood.[18] The creation of the "geep" revealed several complexities to chimera development. In implanting a goat embryo for gestation in a sheep, the sheep's immune system would reject the developing goat embryo, whereas a "geep" embryo, sharing markers of immunity with both sheep and goats, was able to survive implantation in either of its parent species.

In August 2003, researchers at the Shanghai Second Medical University in China reported that they had successfully fused human skin cells and rabbit ova to create the first human chimeric embryos. The embryos were allowed to develop for several days in a laboratory setting, then destroyed to harvest the resulting stem cells.[19] In 2007, scientists at the University of Nevada School of Medicine created a sheep whose blood contained 15% human cells and 85% sheep cells.[20]

Mice

Chimeric mice are important tools in biological research, as they allow the investigation of a variety of biological questions in an animal that has two distinct genetic pools within it. These include insights into such problems as the tissue specific requirements of a gene, cell lineage, and cell potential. The general methods for creating chimeric mice can be summarized either by injection or aggregation of embryonic cells from different origins. The first chimeric mouse was made by Beatrice Mintz in the 1960s through the aggregation of eight cell stage embryos.[21] Injection on the other hand was pioneered by Richard Gardner and Ralph Brinster who injected cells into blastocysts to create chimeric mice with germ lines fully derived from injected ES Cells.[22] Chimeras can be derived from mouse embryos that have not yet implanted in the uterus as well as from implanted embryos. ES cells from the inner cell mass of an implanted blastocyst can contribute to all cell lineages of a mouse including the germ line. ES cells are also a useful tool in chimeras because genes can be mutated in them through the use of homologous recombination, thus allowing gene targeting. Since this discovery occurred in 1999, ES cells have become a key tool in the generation of specific chimeric mice.[23]

Underlying biology

The ability to make mouse chimeras comes from an understanding of early mouse development. Between the stages of fertilization of the egg and the implantation of a blastocyst into the uterus, different parts of the mouse embryo retain the ability to give rise to a variety of cell lineages. Once the embryo has reached the blastocyst stage, it is composed of several parts, mainly the trophectoderm, the inner cell mass, and the primitive endoderm. Each of these parts of the blastocyst gives rise to different parts of the embryo; the inner cell mass gives rise to the embryo proper, while the trophectoderm and primitive endoderm give rise to extra embryonic structures that support growth of the embryo.[24] Two- to eight-cell-stage embryos are competent for making chimeras, since at these stages of development, the cells in the embryos are not yet committed to give rise to any particular cell lineage, and could give rise to the inner cell mass or the trophectoderm. In the case where two diploid eight-cell-stage embryos are used to make a chimera, chimerism can be later found in the epiblast, primitive, endoderm and trophectoderm of the mouse blastocyst.[25][26] It is possible to dissect the embryo at other stages so as to accordingly give rise to one lineage of cells from an embryo selectively and not the other. For example, subsets of blastomeres can be used to give rise to chimera with specified cell lineage from one embryo. The Inner Cell Mass of a diploid blastocyst for example can be used to make a chimera with another blastocyst of eight-cell diploid embryo; the cells taken from the inner cell mass will give rise to the primitive endoderm and to the epiblast in the chimera mouse.[27] From this knowledge, ES cell contributions to chimeras have been developed. ES cells can be used in combination with eight-cell-and two-cell-stage embryos to make chimeras and exclusively give rise to the embryo proper. Embryos that are to be used in chimeras can further be genetically altered in order to specifically contribute to only one part of chimera. An example is the chimera built off of ES cells and tetraploid embryos, tetraploid embryos which are artificially made by electrofusion of two two-cell diploid embryos. The tetraploid embryo will exclusively give rise to the trophectoderm and primitive endoderm in the chimera[28][29]

Methods of production

There are a variety of combinations that can give rise to a successful chimera mouse and — according to the goal of the experiment — an appropriate cell and embryo combination can be picked; they are generally but not limited to diploid embryo and ES cells, diploid embryo and diploid embryo, ES cell and tetraploid embryo, diploid embryo and tetraploid embryo, ES cells and ES cells. The combination of embryonic stem cell and diploid embryo is a common technique used for the making of chimeric mice, since gene targeting can be done in the embryonic stem cell. These kinds of chimeras can be made through either aggregation of stem cells and the diploid embryo or injection of the stem cells into the diploid embryo. If embryonic stem cells are to be used for gene targeting to make a chimera, the following procedure is common: a construct for homologous recombination for the gene targeted will be introduced into cultured mouse embryonic stem cells from the donor mouse, by way of electroporation; cells positive for the recombination event will have antibiotic resistance, provided by the insertion cassette used in the gene targeting; and be able to be positively selected for.[30][31] ES cells with the correct targeted gene are then injected into a diploid host mouse blastocyst. These injected blastocysts are then implanted into a pseudo pregnant female surrogate mouse which will bring the embryos to term and give birth to a mouse whose germline is derived from the donor mouse's ES cells.[32] This same procedure can be achieved through aggregation of ES cells and diploid embryos, diploid embryos are cultured in aggregation plates in wells where single embryos can fit, to these wells ES cells are added the aggregates are cultured until a single embryo is formed and has progressed to the blastocyst stage, and can then be transferred to the surrogate mouse.[33]

Plants

Structure

The distinction between sectorial, mericlinal and periclinal chimeras are widely used.[34][35]

Graft chimeras

Main article: Graft-chimaera
Taxus mosaic.

These are produced by grafting genetically different parents, different cultivars or different species (which may belong to different genera). The tissues may be partially fused together following grafting to form a single growing organism that preserves both types of tissue in a single shoot.[36] Just as the constituent species are likely to differ in a wide range of features, so the behavior of their periclinal chimeras is like to be highly variable.[37] The first such known chimera was probably the Bizzaria which is a confusion of the Florentine citron and the sour orange. Well-known examples of a graft-chimera are Laburnocytisus 'Adamii', caused by a fusion of a Laburnum and a broom, and "Family" trees, where multiple varieties of apple or pear are grafted onto the same tree. Many fruit trees are cultivated by grafting the body of a sapling onto a rootstock.

Chromosomal chimeras

These are chimeras in which the layers differ in their chromosome constitution. Occasionally chimeras arise from loss or gain of individual chromosomes or chromosome fragments owing to misdivision.[38] More commonly cytochimeras have simple multiple of the normal chromosome complement in the changed layer. There are various effects on cell size and growth characteristics.

Nuclear gene-differential chimeras

These chimeras arise by spontaneous or induced mutation of a nuclear gene to a dominant or recessive allele. As a rule one character is affected at a time in the leaf, flower, fruit, or other parts.

Plastid gene-differential chimeras

These chimeras arise by spontaneous or induced mutation of a plastid gene, followed by the sorting-out of two kinds of plastid during vegetative growth. Alternatively, after selfing or nucleic acid thermodynamics, plastids may sort-out from a mixed egg or mixed zygote respectively. This type of chimera is recognized at the time of origin by the sorting-out pattern in the leaves. After sorting-out is complete, periclinal chimeras are distinguished from similar looking nuclear gene-differential chimeras by their non-mendelian inheritance. The majority of variegated-leaf chimeras are of this kind.

All plastid gene- and some nuclear gene-differential chimeras affect the color of the plasmids within the leaves, and these are grouped together as chlorophyll chimeras, or preferably as variegated leaf chimeras. For most variegation, the mutation involved is the loss of the chloroplasts in the mutated tissue, so that part of the plant tissue has no green pigment and no photosynthetic ability. This mutated tissue is unable to survive on its own but is kept alive by its partnership with normal photosynthetic tissue. Sometimes chimeras are also found with layers differing in respect of both their nuclear and their plastid genes.

Origins

There are multiple reasons to explain the occurrence of plant chimera during plant recovery stage:

(1) The process of shoot organogenesis starts form the multicellular origin.[39]

(2) The endogenous tolerance leads to the ineffectiveness of the weak selective agents.

(3) A self-protection mechanism (cross protection). Transformed cells serve as guards to protect the untransformed ones.[40]

(4) The observable characteristic of transgenic cells may be a transient expression of the marker gene. Or it may due to the presence of agrobacterium cells.

Detection

Untransformed cells should be easy to detect and remove to avoid chimeras. Because it’s extremely important to maintain the stable ability of the transgenic plants across different generations. Reporter genes such as GUS and Green Fluorescent Protein[41](GFP) are utilized in combination with plant selective markers (herbicide, antibody etc.) However, GUS expression depends on the plant development stage and GFP may be influenced by the green tissue autofluorescence. Quantitative PCR could be an alternative method for chimera detection.[42]

Ethics and Legislation

Ethics

The US and Western Europe have strict codes of ethics and regulations in place that expressly forbid certain subsets of experimentation using human cells, though there is a vast difference in the regulatory framework.[43] Through the creation of human-chimera comes the question: where does society now draw the line of humanity? This question poses serious legal and moral issues, along with creating controversy. Chimpanzees, for example, are not offered any legal standing and if they pose a threat to humans are put down. Once a chimpanzee is genetically altered to be more similar to a human, it may blur the ethical line between animal and man. Legal debate would be the next step in the process to determine whether certain chimera should be granted legal rights.[44] Along with issues regarding the rights of chimera, individuals have expressed concern whether or not creating human-chimera diminishes the dignity of being human.[45]

Legislation

On May 2008, a robust debate in the House of Commons of the United Kingdom on the ethics of creating chimeras with human stem cells led to the decision that embryos would be allowed to be made in laboratories, given that they would be destroyed within the first 14 days.

On 11 July 2005 a bill, The Human Chimera Prohibition Act, was introduced into the United States Congress by Senator Samuel Brownback, however it died in Congress sometime in the next year. The bill was introduced based on the findings that science has progressed to the point where the human and nonhuman species can be merged to create new forms of life. Because of this serious ethical issues arise as this blurs the line between man and animal, and according to the bill with this blurring of the lines comes a show of disrespect for human dignity. The final claim brought up in The Human Chimera Prohibition Act was that there is an increasing amount of zoonotic diseases and the creation of human-animal chimeras can allow these diseases to reach humans.[45] Since the bill's death in congress there has not been another attempt at setting regulations on chimera research in the United States.

See also

References

  1. 1 2 3 4 Norton, Aaron; Ozzie Zehner (2008). "Which Half Is Mommy?: Tetragametic Chimerism and Trans-Subjectivity". Women's Studies Quarterly. Fall/Winter: 106–127.
  2. Friedman, Lauren. "The Stranger-Than-Fiction Story Of A Woman Who Was Her Own Twin". Retrieved 4 August 2014.
  3. 1 2 Strain, Lisa; John C.S. Dean; Mark P. R. Hamilton; David T. Bonthron (1998). "A True Hermaphrodite Chimera Resulting from Embryo Amalgamation after in Vitro Fertilization". The New England Journal of Medicine 338 (3): 166–169. doi:10.1056/NEJM199801153380305. PMID 9428825.
  4. Boklage, C.E. How New Humans Are Made. Hackensack, NJ; London: World Scientific Publishing Co. Pte. Ltd; 2010
  5. 1 2 Ross, C. N.; J. A. French; G. Orti (2007). "Germ-line chimerism and paternal care in marmosets (Callithrix kuhlii)". Proceedings of the National Academy of Sciences 104 (15): 6278–6282. doi:10.1073/pnas.0607426104. ISSN 0027-8424. PMC 1851065. PMID 17389380.
  6. 1 2 Masahito Tachibana, Michelle Sparman and Shoukhrat Mitalipov (January 2012). "Generation of Chimeric Rhesus Monkeys". cell.
  7. Gengozian, N.; Batson, JS; Eide, P. (1964). "Hematologic and Cytogenetic Evidence for Hematopoietic Chimerism in the Marmoset, Tamarinus Nigricollis". Cytogenetics 10: 384–393.
  8. Dr. Barry Starr. "2 ) In the chimera episode, the fact that the guy was a chimera was first established through a camera flash on the skin illuminating skin anomalies...". Ask a Geneticist. Stanford School of Medicine. Archived from the original on 2011-07-24.
  9. "The Twin Inside Me: Extraordinary People". Channel 5 TV, UK. 9 March 2006. Archived from the original on May 26, 2006.
  10. Bellefon, L.; Heiman, P.; Kanaan, S.; Azzouz, D.; Rak, J.; Martin, M.; Roudier, J.; Roufosse, F.; Lambert, C. (2010). "Cells from a vanished twin as a source of microchimerism 40 years later". Chimerism 1: 56–60. doi:10.4161/chim.1.2.14294.
  11. Ceratiidae
  12. Zimmer, Carl (2007-03-27). "In the Marmoset Family, Things Really Do Appear to Be All Relative". The New York Times. Retrieved 2010-04-01.
  13. Hooper, Rowan (26 March 2007). "Marmosets may carry their sibling's sex cells". New Scientist.
  14. Ballantyne, KN; Kayser, M; Grootegoed, JA (2011). "'Sex and gender issues in competitive sports: investigation of a historical case leads to a new viewpoint'". British Journal of Sports Medicine 46: 614–7. doi:10.1136/bjsm.2010.082552. PMC 3375582. PMID 21540190.
  15. Bowley, C. C.; Ann M. Hutchison; Joan S. Thompson; Ruth Sanger (July 11, 1953). "A human blood-group chimera" (PDF). British Medical Journal: 81. Retrieved 2011-10-02.
  16. http://citeseerx.ist.psu.edu/viewdoc/download?doi=10.1.1.149.9001&rep=rep1&type=pdf
  17. "She's Her Own Twin - ABC News". Abcnews.go.com. August 15, 2006. Retrieved September 17, 2013.
  18. "It's a Geep". Time. 27 February 1984. Retrieved 4 January 2012.
  19. Mott, Maryann (January 25, 2005). "Animal-Human Hybrids Spark Controversy". National Geographic News.
  20. "Iranian scientist creates sheep with half-human organs". Press TV. 27 Mar 2007. Archived from the original on November 14, 2007.
  21. Mintz, B.; Silvers, W. K. (1967). ""Intrinsic" Immunological Tolerance in Allophenic Mice". Science 158 (3807): 1484–6. doi:10.1126/science.158.3807.1484. PMID 6058691.
  22. Robertson, EJ (1986). "Pluripotential stem cell lines as a route into the mouse germ line". Trends Genet 2: 9–13. doi:10.1016/0168-9525(86)90161-7.
  23. Doetschman, T.; Maeda, N.; Smithies, O. (1988). "Targeted mutation of the Hp gene in mouse embryonic stem cells". Proc. Natl. Acad. Sci. 85 (22): 8583–8587. doi:10.1073/pnas.85.22.8583. PMC 282503. PMID 3186749.
  24. Ralston, A; Rossant, J (2005). "Genetic regulation of stem cell origins in the mouse embryo". Clin Genet 68 (2): 106–102. doi:10.1111/j.1399-0004.2005.00478.x.
  25. Tam, P.L.; Rossant, J. (2003). "Mouse embryonic chimeras: tools for studying mammalian development". Development 130 (25): 6155–6163. doi:10.1242/dev.00893. PMID 14623817.
  26. Rossant, J. (1976). "Postimplantation development of blastomeres isolated from 4- and 8-cell mouse eggs". J. Embryol. Exp. Morphol 36 (2): 283–290. PMID 1033982.
  27. Pappaioannou, V., R. Johnson. (1993). Production of chimeras and genetically defined offspring from targeted ES cells. In Gene Targeting: A Practical Approach (ed. A.Joyner) IRL Press at Oxford University Press
  28. Kubiak, J; Tarkowski, A. (1985). "Electrofusion of mouse blastomeres. Exp". Cell Res. 157 (2): 561–566. doi:10.1016/0014-4827(85)90143-0. PMID 3884349.
  29. Nagy, A. and Rossant J. (1999) Production of Es-cell aggregation chimeras. Gene Targeting: A Practical Approach (Joyner, A, ed.) IRL Press at Oxford University, Oxford, UK
  30. Jasin, M; Moynahan, ME; Richardson, C (1996). "Targeted transgenesis". PNAS 93 (17): 8804–8808. doi:10.1073/pnas.93.17.8804. PMC 38547. PMID 8799106.
  31. Ledermann, B (2000). "Embryonic Stem Cell and Gene Targeting". Experimental Physiology 85 (6): 603–613. doi:10.1017/S0958067000021059. PMID 11187956.
  32. Chimera Mouse production by blastocyst injection, Wellcome trust Sanger Institute, http://www.eucomm.org/docs/protocols/mouse_protocol_1_Sanger.pdf
  33. Tanaka, M; Hadjantonakis, AK; Nagy, A (2001). "Aggregation chimeras. Combining ES cells, diploid and tetraploid embryos.". Methods in molecular biology (Clifton, N.J.) 158: 135–54. doi:10.1385/1-59259-220-1:135. PMID 11236654.
  34. The plastids: their chemistry, structure, growth and inheritance, 2nd edition,1978, Elsevier/ North-Holland, Amsterdam, ISBN 0-444-80022-0
  35. Mutation breeding techniques and behavior of irradiated shoot apices of potato, 1978, Pudoc, Wageingen
  36. Norris, R., Smith, R.H., and Vaughn, K.C. (1983). "Plant chimeras used to establish de novo origin of shoots". Science 220 (4592): 75–76. doi:10.1126/science.220.4592.75.
  37. Plant Chimeras, 1st edition, 1992, Cambridge University Press, ISBN 0-521-42787-8
  38. Thompson, J.D., Herre, E.A., Hamrick, J.L., and Stone, J.L. (1991). "Genetic mosaics in strangler fig trees: implication for tropical conservation". Science 254 (5035): 1214–1216. doi:10.1126/science.254.5035.1214. PMID 17776412.
  39. Zhu, X., Zhao, M., Ma, S., Ge, Y., Zhang, M., and Chen, L. (2007). "Induction and origin of adventitious shoots from chimeras of Brassica juncea and Brassica oleracea". Plant Cell Rep 26 (10): 1727–1732. doi:10.1007/s00299-007-0398-4.
  40. Park SH, Rose SC, Zapata C, Srivatanakul M. (1998). "Cross-protection and selectable marker genes in plant transformation.". In Vitro Cellular & Developmental Biology - Plant 34 (2): 117–121. doi:10.1007/BF02822775.
  41. Rakosy-Tican, E., Aurori, C.M., Dijkstra, C., Thieme, R., Aurori, A., and Davey, M.R. (2007). "The usefulness of the gfp reporter gene for monitoring Agrobacterium-mediated transformation of potato dihaploid and tetraploid genotypes". Plant Cell Rep 26 (5): 661–671. doi:10.1007/s00299-006-0273-8.
  42. Faize, M., Faize, L. and Burgos, L. (2010). "Using quantitative real-time PCR to detect chimeras in transgenic tobacco and apricot and to monitor their dissociation". BMC Biotechnology 10 (1): 53. doi:10.1186/1472-6750-10-53.
  43. Futehally, Ilmas, Beyond Biology, Strategic Foresight Group
  44. Bruch, Quinton. "Defining Humanity: The Ethics of Chimeric Animals and Organ Growing". The Triple Helix Online. Retrieved 21 May 2015.
  45. 1 2 Brownback, Samuel. "S.659 -- Human Chimera Prohibition Act of 2005 (Introduced in Senate - IS)". The Library of Congress THOMAS. Retrieved 20 May 2015.
This article is issued from Wikipedia - version of the Sunday, May 01, 2016. The text is available under the Creative Commons Attribution/Share Alike but additional terms may apply for the media files.