Paramecium aurelia[1] are unicellular organisms belonging to the genus Paramecium of the phylum Ciliophora.[2] They are covered in cilia which help in movement and feeding.[2]Paramecium can reproduce sexually, asexually, or by the process of endomixis.[3] Paramecium aurelia demonstrate a strong "sex reaction" whereby groups of individuals will cluster together, and emerge in conjugant pairs. This pairing can last up to 12 hours, during which the micronucleus of each organism will be exchanged.[3] In Paramecium aurelia, a cryptic species complex was discovered by observation.[4] Since then, some have tried to decode this complex using genetic data.[5]

Paramecium aurelia
Scientific classification Edit this classification
Domain: Eukaryota
Clade: Diaphoretickes
Clade: SAR
Clade: Alveolata
Phylum: Ciliophora
Class: Oligohymenophorea
Order: Peniculida
Family: Parameciidae
Genus: Paramecium
Species:
P. aurelia
Binomial name
Paramecium aurelia

Physical characteristics

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The hair-like cilia that cover the outer body of the paramecium are in constant motion, helping the organism move along at a speed of four times its own length per second. As it moves forward, it rotates on its axis, which aids in pushing food into the gullet. It can move backwards by reversing the motion of the cilia.

Food enters the food vacuoles, which cilia push into the gullet in a process known as phagocytosis, and is digested with the aid of hydrochloric acid and enzymes (Raven and Johnson 1996).[full citation needed] When digestion is complete, the remaining food content is emptied into pellicles, known as cytoproct. Osmoregulation is carried out by a pair of contractile vacuoles on either end of the cell, which actively expel water absorbed by osmosis from the surroundings.

 
Drawing of Paramecium aurelia and its parasites

Taxonomy

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Paramecium aurelia is a species complex composed of 15 known species (syngens), which are[5][6]

Ecology

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Scum of algae and cyanobacteria on water surface

Paramecia are found in freshwater environments, and are especially in scums. Paramecia are attracted by acidic conditions, since they eat bacteria, which often acidify their surroundings. They are an important link in the detrital food web in aquatic ecosystems, eating bacteria and dead organic matter often associated with these bacteria, and being preyed on by protists and small animals.

Aging

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Clonal aging, associated with a gradual loss of vitality, occurs in the asexual fission phase of growth of P. tetraurelia, during which cell divisions occur by mitosis rather than meiosis. In P. tetraurelia, the asexual line loses vitality and expires after about 200 fissions if the cells fail to undergo autogamy or conjugation. The basis for this loss of vitality (clonal aging) was clarified by transplantation experiments of Aufderheide in 1986.[7] When macronuclei of clonally young P. tetraurelia were injected into P. tetraurelia of standard clonal age, the lifespan (clonal fissions) of the recipient was prolonged. In contrast, transfer of cytoplasm from clonally young P. tetraurelia did not prolong the lifespan of the recipient. These transplantation experiments indicated that the macronucleus, rather than the cytoplasm, is responsible for clonal aging. Additional experiments by Smith-Sonneborn,[8] Holmes and Holmes,[9] and Gilley and Blackburn[10] showed that, during clonal aging, DNA damage increases dramatically.[11] Thus, DNA damage in the macronucleus appears to be the cause of clonal aging in P. tetraurelia.

Meiosis and rejuvenation

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When clonally aged P. tetraurelia are stimulated to undergo meiosis in association with either conjugation or automixis, the genetic descendants are rejuvenated, and are able to have many more mitotic binary fission divisions. During conjugation or automixis, the micronuclei of the cell(s) undergo meiosis, the old macronucleus disintegrates, and a new macronucleus is formed by replication of the micronuclear DNA that had recently undergone meiosis. There is apparently little, if any, DNA damage in the new macronucleus. These findings further support the idea that clonal aging is due, in large part, to a progressive accumulation of DNA damage; and that rejuvenation is due to the repair of this damage in the micronucleus during meiosis. Meiosis appears to be an adaptation for DNA repair and rejuvenation in P. tetraurelia.[12] In P. tetraurelia, CtlP protein is a key factor needed for the completion of meiosis during sexual reproduction and recovery of viable sexual progeny.[12] The CtlP and Mre11 nuclease complex are essential for accurate processing and repair of double-strand breaks during homologous recombination.[12]

The adaptive benefit of meiosis and self-fertilization in response to starvation appears to be independent of the generation of any new genetic variation in P. tetraurelia.[13] This observation suggests that the underlying molecular mechanism of meiosis provides a fitness advantage regardless of any concomitant effect of sex on genetic diversity.[13][14]

References

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  1. ^ "Paramecium aurelia". Integrated Taxonomic Information System.
  2. ^ a b "Paramecium". 101 Science.com. Retrieved 27 September 2016.
  3. ^ a b Sonneborn, T. M. (1937). "Sex, sex inheritance and sex determination in Paramecium Aurelia" (PDF). Proceedings of the National Academy of Sciences of the United States of America. 23 (7): 378–385. Bibcode:1937PNAS...23..378S. doi:10.1073/pnas.23.7.378. PMC 1076944. PMID 16588168. Retrieved 27 September 2016.
  4. ^ Sonneborn, T. M. (1975) The Paramecium-aurelia complex of 14 sibling species. Transactions of American Microscope Society, 94: 155–178.
  5. ^ a b Catania F, Wurmser F, Potekhin AA, Przybos E, Lynch M (2009). "Genetic Diversity in the Paramecium aurelia Species Complex". Molecular Biology and Evolution. 26 (2): 421–431. doi:10.1093/molbev/msn266. PMC 3888249. PMID 19023087.
  6. ^ Aufderheide, Karl J.; Daggett, Pierre-Marc; Nerad, Thomas A. (1983). "Paramecium sonneborni n. sp., a New Member of the Paramecium aurelia Species-Complex". The Journal of Eukaryotic Microbiology. 30 (1): 128–131. doi:10.1111/j.1550-7408.1983.tb01046.x. ISSN 1066-5234.
  7. ^ Aufderheide, Karl J. (1986). "Clonal aging in Paramecium tetraurelia. II. Evidence of functional changes in the macronucleus with age". Mechanisms of Ageing and Development. 37 (3): 265–279. doi:10.1016/0047-6374(86)90044-8. PMID 3553762. S2CID 28320562.
  8. ^ Smith-Sonneborn, J. (1979). "DNA repair and longevity assurance in Paramecium tetraurelia". Science. 203 (4385): 1115–1117. Bibcode:1979Sci...203.1115S. doi:10.1126/science.424739. PMID 424739.
  9. ^ Holmes, George E.; Holmes, Norreen R. (July 1986). "Accumulation of DNA damages in aging Paramecium tetraurelia". Molecular and General Genetics. 204 (1): 108–114. doi:10.1007/bf00330196. PMID 3091993. S2CID 11992591.
  10. ^ Gilley, David; Blackburn, Elizabeth H. (1994). "Lack of telomere shortening during senescence in Paramecium" (PDF). Proceedings of the National Academy of Sciences of the United States of America. 91 (5): 1955–1958. Bibcode:1994PNAS...91.1955G. doi:10.1073/pnas.91.5.1955. PMC 43283. PMID 8127914.
  11. ^ Bernstein, H; Bernstein, C (1991). Aging, Sex, and DNA Repair. San Diego: Academic Press. pp. 153–156. ISBN 978-0120928606.
  12. ^ a b c Godau, Julia; Ferretti, Lorenza P.; Trenner, Anika; Dubois, Emeline; von Aesch, Christine; Marmignon, Antoine; Simon, Lauriane; Kapusta, Aurélie; Guérois, Raphaël; Bétermier, Mireille; Sartori, Alessandro A. (2019). "Identification of a miniature Sae2/Ctp1/CtIP ortholog from Paramecium tetraurelia required for sexual reproduction and DNA double-strand break repair" (PDF). DNA Repair. 77: 96–108. doi:10.1016/j.dnarep.2019.03.011. PMID 30928893. S2CID 89619084.
  13. ^ a b Thind AS, Vitali V, Guarracino MR, Catania F (May 2020). "What's Genetic Variation Got to Do with It? Starvation-Induced Self-Fertilization Enhances Survival in Paramecium". Genome Biol Evol. 12 (5): 626–638. doi:10.1093/gbe/evaa052. PMC 7239694. PMID 32163147.
  14. ^ Bernstein H, Byerly HC, Hopf FA, Michod RE (September 1985). "Genetic damage, mutation, and the evolution of sex". Science. 229 (4719): 1277–81. doi:10.1126/science.3898363. PMID 3898363.