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Hygiene hypothesis

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In medicine, the hygiene hypothesis states that early childhood exposure to particular microorganisms (such as the gut flora and helminth parasites) protects against allergies by properly tuning the immune system.[1][2] In particular, a lack of such exposure is thought to lead to poor immune tolerance.[1] The time period for exposure begins before birth and ends at school age.[3]

While early versions of the hypothesis referred to microorganism exposure in general, later versions apply to a specific set of microbes that have co-evolved with humans.[1][4][2] The updates have been given various names, including the microbiome depletion hypothesis, the microflora hypothesis, and the "old friends" hypothesis.[4][5] There is a significant amount of evidence supporting the idea that lack of exposure to these microbes is linked to allergies or other conditions,[2][6][7] although it is still rejected by many scientists.[4][8][9]

The term "hygiene hypothesis" has been described as a misnomer because people incorrectly interpret it as referring to their own cleanliness.[1][8][10][11] Having worse personal hygiene, such as not washing hands before eating, only increases the risk of infection without affecting the risk of allergies or immune disorders.[1][4][9] Hygiene is essential for protecting vulnerable populations such as the elderly from infections, preventing the spread of antibiotic resistance, and combating emerging infectious diseases such as Ebola or COVID-19.[12] The hygiene hypothesis does not suggest that having more infections during childhood would be an overall benefit.[1][8]

Overview

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The idea of a link between parasite infection and immune disorders was first suggested in 1968[13] before the advent of large scale DNA sequencing techniques. The original formulation of the hygiene hypothesis dates from 1989, when David Strachan proposed that lower incidence of infection in early childhood could be an explanation for the rise in allergic diseases such as asthma and hay fever during the 20th century.[14]

The hygiene hypothesis has also been expanded beyond allergies, and is also studied in the context of a broader range of conditions affected by the immune system, particularly inflammatory diseases.[15] These include type 1 diabetes,[16] multiple sclerosis,[17][10] and also some types of depression[17][18] and cancer.[19] For example, the global distribution of multiple sclerosis is negatively correlated with that of the helminth Trichuris trichiura and its incidence is negatively correlated with Helicobacter pylori infection.[10] Strachan's original hypothesis could not explain how various allergic conditions spiked or increased in prevalence at different times, such as why respiratory allergies began to increase much earlier than food allergies, which did not become more common until near the end of the 20th century.[12]

In 2003, Graham Rook proposed the "old friends" hypothesis which has been described as a more rational explanation for the link between microbial exposure and inflammatory disorders.[20] The hypothesis states that the vital microbial exposures are not colds, influenza, measles and other common childhood infections which have evolved relatively recently over the last 10,000 years, but rather the microbes already present during mammalian and human evolution, that could persist in small hunter-gatherer groups as microbiota, tolerated latent infections, or carrier states. He proposed that coevolution with these species has resulted in their gaining a role in immune system development.[citation needed]

Strachan's original formulation of the hygiene hypothesis also centred around the idea that smaller families provided insufficient microbial exposure partly because of less person-to-person spread of infections, but also because of "improved household amenities and higher standards of personal cleanliness".[14] It seems likely that this was the reason he named it the "hygiene hypothesis". Although the "hygiene revolution" of the nineteenth and twentieth centuries may have been a major factor, it now seems more likely that, while public health measures such as sanitation, potable water and garbage collection were instrumental in reducing our exposure to cholera, typhoid and so on, they also deprived people of their exposure to the "old friends" that occupy the same environmental habitats.[21]

The rise of autoimmune diseases and acute lymphoblastic leukemia in young people in the developed world was linked to the hygiene hypothesis.[22][23][24] Autism may be associated with changes in the gut microbiome and early infections.[25] The risk of chronic inflammatory diseases also depends on factors such as diet, pollution, physical activity, obesity, socio-economic factors, and stress. Genetic predisposition is also a factor.[26][27][28]

History

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Since allergies and other chronic inflammatory diseases are largely diseases of the last 100 years or so, the "hygiene revolution" of the last 200 years came under scrutiny as a possible cause. During the 1800s, radical improvements to sanitation and water quality occurred in Europe and North America. The introduction of toilets and sewer systems and the cleanup of city streets, and cleaner food were part of this program. This in turn led to a rapid decline in infectious diseases, particularly during the period 1900–1950, through reduced exposure to infectious agents.[21]

Although the idea that exposure to certain infections may decrease the risk of allergy is not new, Strachan was one of the first to formally propose it, in an article published in the British Medical Journal in 1989. This article proposed to explain the observation that hay fever and eczema, both allergic diseases, were less common in children from larger families, which were presumably exposed to more infectious agents through their siblings, than in children from families with only one child.[29] The increased occurrence of allergies had previously been thought to be a result of increasing pollution.[8] The hypothesis was extensively investigated by immunologists and epidemiologists and has become an important theoretical framework for the study of chronic inflammatory disorders.[citation needed]

The "old friends hypothesis" proposed in 2003[20] may offer a better explanation for the link between microbial exposure and inflammatory diseases.[18][20] This hypothesis argues that the vital exposures are not common cold and other recently evolved infections, which are no older than 10,000 years, but rather microbes already present in hunter-gatherer times when the human immune system was evolving. Conventional childhood infections are mostly "crowd infections" that kill or immunise and thus cannot persist in isolated hunter-gatherer groups. Crowd infections started to appear after the neolithic agricultural revolution, when human populations increased in size and proximity. The microbes that co-evolved with mammalian immune systems are much more ancient. According to this hypothesis, humans became so dependent on them that their immune systems can neither develop nor function properly without them.

Rook proposed that these microbes most likely include:

  • Ambient species that exist in the same environments as humans
  • Species that inhabit human skin, gut and respiratory tract, and that of the animals we live with
  • Organisms such as viruses and helminths (worms) that establish chronic infections or carrier states that humans can tolerate and so could co-evolve a specific immunoregulatory relationship with the immune system.

The modified hypothesis later expanded to include exposure to symbiotic bacteria and parasites.[30]

"Evolution turns the inevitable into a necessity." This means that the majority of mammalian evolution took place in mud and rotting vegetation and more than 90 percent of human evolution took place in isolated hunter-gatherer communities and farming communities. Therefore, the human immune systems have evolved to anticipate certain types of microbial input, making the inevitable exposure into a necessity. The organisms that are implicated in the hygiene hypothesis are not proven to cause the disease prevalence, however there are sufficient data on lactobacilli, saprophytic environment mycobacteria, and helminths and their association. These bacteria and parasites have commonly been found in vegetation, mud, and water throughout evolution.[18][20]

Multiple possible mechanisms have been proposed for how the 'Old Friends' microorganisms prevent autoimmune diseases and asthma. They include:

  1. Reciprocal inhibition between immune responses directed against distinct antigens of the Old Friends microbes which elicit stronger immune responses than the weaker autoantigens and allergens of autoimmune disease and allergy respectively.
  2. Competition for cytokines, MHC receptors and growth factors needed by the immune system to mount an immune response.
  3. Immunoregulatory interactions with host TLRs.[23]

The "microbial diversity" hypothesis, proposed by Paolo Matricardi and developed by von Hertzen,[31][32] holds that diversity of microbes in the gut and other sites is a key factor for priming the immune system, rather than stable colonization with a particular species. Exposure to diverse organisms in early development builds a "database" that allows the immune system to identify harmful agents and normalize once the danger is eliminated.[citation needed]

For allergic disease, the most important times for exposure are: early in development; later during pregnancy; and the first few days or months of infancy. Exposure needs to be maintained over a significant period. This fits with evidence that delivery by Caesarean section may be associated with increased allergies, whilst breastfeeding can be protective.[21]

Evolution of the adaptive immune system

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Humans and the microbes they harbor have co-evolved for thousands of centuries; however, it is thought that the human species has gone through numerous phases in history characterized by different pathogen exposures. For instance, in very early human societies, small interaction between its members has given particular selection to a relatively limited group of pathogens that had high transmission rates. It is considered that the human immune system is likely subjected to a selective pressure from pathogens that are responsible for down regulating certain alleles and therefore phenotypes in humans. The thalassemia genes that are shaped by the Plasmodium species expressing the selection pressure might be a model for this theory[33] but is not shown in-vivo.

Recent comparative genomic studies have shown that immune response genes (protein coding and non-coding regulatory genes) have less evolutionary constraint, and are rather more frequently targeted by positive selection from pathogens that coevolve with the human subject. Of all the various types of pathogens known to cause disease in humans, helminths warrant special attention, because of their ability to modify the prevalence or severity of certain immune-related responses in human and mouse models. In fact recent research has shown that parasitic worms have served as a stronger selective pressure on select human genes encoding interleukins and interleukin receptors when compared to viral and bacterial pathogens. Helminths are thought to have been as old as the adaptive immune system, suggesting that they may have co-evolved, also implying that our immune system has been strongly focused on fighting off helminthic infections, insofar as to potentially interact with them early in infancy. The host-pathogen interaction is a very important relationship that serves to shape the immune system development early on in life.[34][35][36][37]

Biological basis

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The primary proposed mechanism of the hygiene hypothesis is an imbalance between the TH1 and TH2 subtypes of T helper cells.[10][38] Insufficient activation of the TH1 arm would stimulate the cell defense of the immune system and lead to an overactive TH2 arm, stimulating the antibody-mediated immunity of the immune systems, which in turn led to allergic disease.[39]

However, this explanation cannot explain the rise in incidence (similar to the rise of allergic diseases) of several TH1-mediated autoimmune diseases, including inflammatory bowel disease, multiple sclerosis and type I diabetes. [Figure 1Bach] However, the North South Gradient seen in the prevalence of multiple sclerosis has been found to be inversely related to the global distribution of parasitic infection.[Figure 2Bach] Additionally, research has shown that MS patients infected with parasites displayed TH2 type immune responses as opposed to the proinflammatory TH1 immune phenotype seen in non-infected multiple sclerosis patients.[Fleming] Parasite infection has also been shown to improve inflammatory bowel disease and may act in a similar fashion as it does in multiple sclerosis.[Lee][citation needed]

Allergic conditions are caused by inappropriate immunological responses to harmless antigens driven by a TH2-mediated immune response, TH2 cells produce interleukin 4, interleukin 5, interleukin 6, interleukin 13 and predominantly stimulate immunoglobulin E production.[23] Many bacteria and viruses elicit a TH1-mediated immune response, which down-regulates TH2 responses. TH1 immune responses are characterized by the secretion of pro-inflammatory cytokines such as interleukin 2, IFNγ, and TNFα. Factors that favor a predominantly TH1 phenotype include: older siblings, large family size, early day care attendance, infection (TB, measles, or hepatitis), rural living, or contact with animals. A TH2-dominated phenotype is associated with high antibiotic use, western lifestyle, urban environment, diet, and sensitivity to dust mites and cockroaches. TH1 and TH2 responses are reciprocally inhibitory, so when one is active, the other is suppressed.[40][41][42]

An alternative explanation is that the developing immune system must receive stimuli (from infectious agents, symbiotic bacteria, or parasites) to adequately develop regulatory T cells. Without that stimuli it becomes more susceptible to autoimmune diseases and allergic diseases, because of insufficiently repressed TH1 and TH2 responses, respectively.[43] For example, all chronic inflammatory disorders show evidence of failed immunoregulation.[26] Secondly, helminths, non-pathogenic ambient pseudocommensal bacteria or certain gut commensals and probiotics, drive immunoregulation. They block or treat models of all chronic inflammatory conditions.[44]

Evidence

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There is a significant amount of evidence supporting the idea that microbial exposure is linked to allergies or other conditions,[2][6][7] although scientific disagreement still exists.[4][8][9] Since hygiene is difficult to define or measure directly, surrogate markers are used such as socioeconomic status, income, and diet.[38]

Studies have shown that various immunological and autoimmune diseases are much less common in the developing world than the industrialized world and that immigrants to the industrialized world from the developing world increasingly develop immunological disorders in relation to the length of time since arrival in the industrialized world.[23] This is true for asthma and other chronic inflammatory disorders.[18] The increase in allergy rates is primarily attributed to diet and reduced microbiome diversity, although the mechanistic reasons are unclear.[45]

The use of antibiotics in the first year of life has been linked to asthma and other allergic diseases,[46] and increased asthma rates are also associated with birth by Caesarean section.[47] However, at least one study suggests that personal hygienic practices may be unrelated to the incidence of asthma.[9] Antibiotic usage reduces the diversity of gut microbiota. Although several studies have shown associations between antibiotic use and later development of asthma or allergy, other studies suggest that the effect is due to more frequent antibiotic use in asthmatic children. Trends in vaccine use may also be relevant, but epidemiological studies provide no consistent support for a detrimental effect of vaccination/immunization on atopy rates.[21] In support of the old friends hypothesis, the intestinal microbiome was found to differ between allergic and non-allergic Estonian and Swedish children (although this finding was not replicated in a larger cohort), and the biodiversity of the intestinal flora in patients with Crohn's disease was diminished.[23]

Limitations

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The hygiene hypothesis does not apply to all populations.[9][38] For example, in the case of inflammatory bowel disease, it is primarily relevant when a person's level of affluence increases, either due to changes in society or by moving to a more affluent country, but not when affluence remains constant at a high level.[38]

The hygiene hypothesis has difficulty explaining why allergic diseases also occur in less affluent regions.[9] Additionally, exposure to some microbial species actually increases future susceptibility to disease instead, as in the case of infection with rhinovirus (the main source of the common cold) which increases the risk of asthma.[4][48]

Treatment

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Current research suggests that manipulating the intestinal microbiota may be able to treat or prevent allergies and other immune-related conditions.[2] Various approaches are under investigation. Probiotics (drinks or foods) have never been shown to reintroduce microbes to the gut. As yet, therapeutically relevant microbes have not been specifically identified.[49] However, probiotic bacteria have been found to reduce allergic symptoms in some studies.[15] Other approaches being researched include prebiotics, which promote the growth of gut flora, and synbiotics, the use of prebiotics and probiotics at the same time.[2]

Should these therapies become accepted, public policy implications include providing green spaces in urban areas or even providing access to agricultural environments for children.[50]

Helminthic therapy is the treatment of autoimmune diseases and immune disorders by means of deliberate infestation with a helminth larva or ova. Helminthic therapy emerged from the search for reasons why the incidence of immunological disorders and autoimmune diseases correlates with the level of industrial development.[51][52] The exact relationship between helminths and allergies is unclear, in part because studies tend to use different definitions and outcomes, and because of the wide variety among both helminth species and the populations they infect.[53] The infections induce a type 2 immune response, which likely evolved in mammals as a result of such infections; chronic helminth infection has been linked with a reduced sensitivity in peripheral T cells, and several studies have found deworming to lead to an increase in allergic sensitivity.[54][13] However, in some cases helminths and other parasites are a cause of developing allergies instead.[4] In addition, such infections are not themselves a treatment as they are a major disease burden and in fact they are one of the most important neglected diseases.[54][13] The development of drugs that mimic the effects without causing disease is in progress.[4]

Public health

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The reduction of public confidence in hygiene has significant possible consequences for public health.[12] Hygiene is essential for protecting vulnerable populations such as the elderly from infections, preventing the spread of antibiotic resistance, and for combating emerging infectious diseases such as SARS and Ebola.[12]

The misunderstanding of the term "hygiene hypothesis" has resulted in unwarranted opposition to vaccination as well as other important public health measures.[8] It has been suggested that public awareness of the initial form of the hygiene hypothesis has led to an increased disregard for hygiene in the home.[55] The effective communication of science to the public has been hindered by the presentation of the hygiene hypothesis and other health-related information in the media.[12]

Cleanliness

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No evidence supports the idea that reducing modern practices of cleanliness and hygiene would have any impact on rates of chronic inflammatory and allergic disorders, but a significant amount of evidence indicates that reducing hygiene would increase the risks of infectious diseases.[21] The phrase "targeted hygiene" has been used in order to recognize the importance of hygiene in avoiding pathogens.[1]

If home and personal cleanliness contributes to reduced exposure to vital microbes, its role is likely to be small. The idea that homes can be made “sterile” through excessive cleanliness is implausible, and the evidence shows that after cleaning, microbes are quickly replaced by dust and air from outdoors, by shedding from the body and other living things, as well as from food.[21][56][57][58] The key point may be that the microbial content of urban housing has altered, not because of home and personal hygiene habits, but because they are part of urban environments. Diet and lifestyle changes also affects the gut, skin and respiratory microbiota.[citation needed]

At the same time that concerns about allergies and other chronic inflammatory diseases have been increasing, so also have concerns about infectious disease.[21][59][60] Infectious diseases continue to exert a heavy health toll. Preventing pandemics and reducing antibiotic resistance are global priorities, and hygiene is a cornerstone of containing these threats.[citation needed]

Infection risk management

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The International Scientific Forum on Home Hygiene has developed a risk management approach to reducing home infection risks. This approach uses microbiological and epidemiological evidence to identify the key routes of infection transmission in the home. These data indicate that the critical routes involve the hands, hand and food contact surfaces and cleaning utensils. Clothing and household linens involve somewhat lower risks. Surfaces that contact the body, such as baths and hand basins, can act as infection vehicles, as can surfaces associated with toilets. Airborne transmission can be important for some pathogens. A key aspect of this approach is that it maximises protection against pathogens and infection, but is more relaxed about visible cleanliness in order to sustain normal exposure to other human, animal and environmental microbes.[56]

See also

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References

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  1. ^ a b c d e f g Scudellari, Megan (2017). "News Feature: Cleaning up the hygiene hypothesis". Proceedings of the National Academy of Sciences. 114 (7): 1433–1436. Bibcode:2017PNAS..114.1433S. doi:10.1073/pnas.1700688114. PMC 5320962. PMID 28196925.
  2. ^ a b c d e f Stiemsma, Leah; Reynolds, Lisa; Turvey, Stuart; Finlay, Brett (July 2015). "The hygiene hypothesis: Current perspectives and future therapies". ImmunoTargets and Therapy. 4: 143–157. doi:10.2147/ITT.S61528. PMC 4918254. PMID 27471720.
  3. ^ Roduit, Caroline; Frei, Remo; von Mutius, Erika; Lauener, Roger (2016). "The Hygiene Hypothesis". Environmental Influences on the Immune System. pp. 77–96. doi:10.1007/978-3-7091-1890-0_4. ISBN 978-3-7091-1888-7.
  4. ^ a b c d e f g h Alexandre-Silva, Gabriel M.; Brito-Souza, Pablo A.; Oliveira, Ana C.S.; Cerni, Felipe A.; Zottich, Umberto; Pucca, Manuela B. (December 2018). "The hygiene hypothesis at a glance: Early exposures, immune mechanism and novel therapies". Acta Tropica. 188: 16–26. doi:10.1016/j.actatropica.2018.08.032. PMID 30165069. S2CID 52131098.
  5. ^ "Reconstituting the depleted biome to prevent immune disorders". The Evolution and Medicine Review. 13 October 2010.
  6. ^ a b Daley, Denise (October 2014). "The evolution of the hygiene hypothesis". Current Opinion in Allergy and Clinical Immunology. 14 (5): 390–396. doi:10.1097/ACI.0000000000000101. PMID 25102107. S2CID 45420527.
  7. ^ a b Versini, Mathilde; Jeandel, Pierre-Yves; Bashi, Tomer; Bizzaro, Giorgia; Blank, Miri; Shoenfeld, Yehuda (13 April 2015). "Unraveling the Hygiene Hypothesis of helminthes and autoimmunity: origins, pathophysiology, and clinical applications". BMC Medicine. 13 (1): 81. doi:10.1186/s12916-015-0306-7. PMC 4396177. PMID 25879741.
  8. ^ a b c d e f Björkstén, Bengt (2009). "The Hygiene Hypothesis: Do we still believe in it?". Microbial Host-Interaction: Tolerance versus allergy. Nestlé Nutrition Institute Workshop Series: Pediatric Program. Vol. 64. pp. 11–22. doi:10.1159/000235780. ISBN 978-3-8055-9167-6. PMID 19710512.
  9. ^ a b c d e f van Tilburg Bernardes, Erik; Arrieta, Marie-Claire (November 2017). "Hygiene Hypothesis in Asthma Development: Is Hygiene to Blame?". Archives of Medical Research. 48 (8): 717–726. doi:10.1016/j.arcmed.2017.11.009. PMID 29224909.
  10. ^ a b c d Wendel-Haga, M.; Celius, E.G. (November 2017). "Is the hygiene hypothesis relevant for the risk of multiple sclerosis?". Acta Neurologica Scandinavica. 136: 26–30. doi:10.1111/ane.12844. PMID 29068485.
  11. ^ Parker, W. (26 August 2014). "The 'hygiene hypothesis' for allergic disease is a misnomer". BMJ. 349 (aug26 2): g5267. doi:10.1136/bmj.g5267. PMID 25161287. S2CID 33624127.
  12. ^ a b c d e Bloomfield, Sally F; Rook, Graham AW; Scott, Elizabeth A; Shanahan, Fergus; Stanwell-Smith, Rosalind; Turner, Paul (27 June 2016). "Time to abandon the hygiene hypothesis: new perspectives on allergic disease, the human microbiome, infectious disease prevention and the role of targeted hygiene". Perspectives in Public Health. 136 (4): 213–224. doi:10.1177/1757913916650225. PMC 4966430. PMID 27354505.
  13. ^ a b c Maizels, R. M.; McSorley, H. J.; Smyth, D. J. (July 2014). "Helminths in the hygiene hypothesis: sooner or later?". Clinical & Experimental Immunology. 177 (1): 38–46. doi:10.1111/cei.12353. PMC 4089153. PMID 24749722.
  14. ^ a b Strachan, D. (1 August 2000). "Family size, infection and atopy: the first decade of the 'hygiene hypothesis'". Thorax. 55 (90001): 2S–10. doi:10.1136/thorax.55.suppl_1.s2. PMC 1765943. PMID 10943631.
  15. ^ a b Shu, Shang-An; Yuen, Agatha W. T.; Woo, Elena; Chu, Ka-Hou; Kwan, Hoi-Shan; Yang, Guo-Xiang; Yang, Yao; Leung, Patrick S. C. (18 December 2018). "Microbiota and Food Allergy". Clinical Reviews in Allergy & Immunology. 57 (1): 83–97. doi:10.1007/s12016-018-8723-y. PMID 30564985. S2CID 56476417.
  16. ^ Stene, Lars C; Nafstad, Per (February 2001). "Relation between occurrence of type 1 diabetes and asthma". The Lancet. 357 (9256): 607–608. doi:10.1016/S0140-6736(00)04067-8. PMID 11558491. S2CID 7457497.
  17. ^ a b Raison, Charles L.; Lowry, Christopher A.; Rook, Graham A. W. (December 2010). "Inflammation, Sanitation, and Consternation". Archives of General Psychiatry. 67 (12): 1211–1224. doi:10.1001/archgenpsychiatry.2010.161. PMC 3724429. PMID 21135322.
  18. ^ a b c d Rook, Graham A. W.; Lowry, Christopher A.; Raison, Charles L. (2013). "Microbial 'Old Friends', immunoregulation and stress resilience". Evolution, Medicine, and Public Health. 2013 (1): 46–64. doi:10.1093/emph/eot004. PMC 3868387. PMID 24481186.
  19. ^ Rook, Graham A. W.; Dalgleish, Angus (March 2011). "Infection, immunoregulation, and cancer". Immunological Reviews. 240 (1): 141–159. doi:10.1111/j.1600-065X.2010.00987.x. PMID 21349092. S2CID 39495585.
  20. ^ a b c d Rook, Graham A.W.; Martinelli, Roberta; Brunet, Laura Rosa (October 2003). "Innate immune responses to mycobacteria and the downregulation of atopic responses". Current Opinion in Allergy and Clinical Immunology. 3 (5): 337–342. doi:10.1097/00130832-200310000-00003. PMID 14501431. S2CID 45020780.
  21. ^ a b c d e f g Smith, Rosalind Stanwell; Bloomfield, Sally F.; Rook, Graham A. (September 2012). "The Hygiene Hypothesis and its implications for home hygiene, lifestyle and public health". Home Hygiene & Health.
  22. ^ Smith, Malcolm A.; Simon, Richard; Strickler, Howard D.; McQuillan, Geraldine; Gloeckler Ries, Lynn A.; Linet, Martha S. (1998). "Evidence that childhood acute lymphoblastic leukemia is associated with an infectious agent linked to hygiene conditions". Cancer Causes & Control. 9 (3): 285–298. doi:10.1023/A:1008873103921. PMID 9684709. S2CID 25397922.
  23. ^ a b c d e Okada, H.; Kuhn, C.; Feillet, H.; Bach, J.-F. (11 March 2010). "The 'hygiene hypothesis' for autoimmune and allergic diseases: an update". Clinical & Experimental Immunology. 160 (1): 1–9. doi:10.1111/j.1365-2249.2010.04139.x. PMC 2841828. PMID 20415844.
  24. ^ Greaves, Mel (August 2018). "A causal mechanism for childhood acute lymphoblastic leukaemia". Nature Reviews Cancer. 18 (8): 471–484. doi:10.1038/s41568-018-0015-6. PMC 6986894. PMID 29784935.
  25. ^ Vallès, Yvonne; Francino, M. Pilar (29 September 2018). "Air Pollution, Early Life Microbiome, and Development". Current Environmental Health Reports. 5 (4): 512–521. doi:10.1007/s40572-018-0215-y. PMC 6306492. PMID 30269309.
  26. ^ a b Rook, G. A. W. (11 March 2010). "99th Dahlem Conference on Infection, Inflammation and Chronic Inflammatory Disorders: Darwinian medicine and the 'hygiene' or 'old friends' hypothesis". Clinical & Experimental Immunology. 160 (1): 70–79. doi:10.1111/j.1365-2249.2010.04133.x. PMC 2841838. PMID 20415854.
  27. ^ Filippi, C. M.; von Herrath, M. G. (29 October 2008). "Viral Trigger for Type 1 Diabetes: Pros and Cons". Diabetes. 57 (11): 2863–2871. doi:10.2337/db07-1023. PMC 2570378. PMID 18971433.
  28. ^ Rook, Graham A. W. (17 November 2011). "Hygiene Hypothesis and Autoimmune Diseases". Clinical Reviews in Allergy & Immunology. 42 (1): 5–15. doi:10.1007/s12016-011-8285-8. PMID 22090147. S2CID 15302882.
  29. ^ Strachan, D. P. (18 November 1989). "Hay fever, hygiene, and household size". BMJ. 299 (6710): 1259–1260. doi:10.1136/bmj.299.6710.1259. PMC 1838109. PMID 2513902.
  30. ^ Grammatikos, Alexandros P. (8 July 2009). "The genetic and environmental basis of atopic diseases". Annals of Medicine. 40 (7): 482–495. doi:10.1080/07853890802082096. PMID 18608118. S2CID 188280.
  31. ^ Matricardi, P. M. (11 March 2010). "99th Dahlem Conference on Infection, Inflammation and Chronic Inflammatory Disorders: Controversial aspects of the 'hygiene hypothesis'". Clinical & Experimental Immunology. 160 (1): 98–105. doi:10.1111/j.1365-2249.2010.04130.x. PMC 2841842. PMID 20415858.
  32. ^ von Hertzen, Leena; Hanski, Ilkka; Haahtela, Tari (7 October 2011). "Natural immunity". EMBO Reports. 12 (11): 1089–1093. doi:10.1038/embor.2011.195. PMC 3207110. PMID 21979814.
  33. ^ Vrushali, Pathak; Roshan, Roshan; Kanjaksha, Ghosh (February 2018). "Plasmodium falciparum malaria skews globin gene expression balance in in-vitro haematopoietic stem cell culture system: Its implications in malaria associated anemia". Exp. Parasitol. 185: 29–38. doi:10.1016/j.exppara.2018.01.003. PMID 29309785.
  34. ^ Sironi, Manuela; Clerici, Mario (June 2010). "The hygiene hypothesis: an evolutionary perspective". Microbes and Infection. 12 (6): 421–427. doi:10.1016/j.micinf.2010.02.002. PMID 20178858.
  35. ^ Wolfe, Nathan D.; Dunavan, Claire Panosian; Diamond, Jared (May 2007). "Origins of major human infectious diseases". Nature. 447 (7142): 279–283. Bibcode:2007Natur.447..279W. doi:10.1038/nature05775. PMC 7095142. PMID 17507975.
  36. ^ Kosiol, Carolin; Vinař, Tomáš; da Fonseca, Rute R.; Hubisz, Melissa J.; Bustamante, Carlos D.; Nielsen, Rasmus; Siepel, Adam; Schierup, Mikkel H. (1 August 2008). "Patterns of Positive Selection in Six Mammalian Genomes". PLOS Genetics. 4 (8): e1000144. doi:10.1371/journal.pgen.1000144. PMC 2483296. PMID 18670650.
  37. ^ Fumagalli, Matteo; Pozzoli, Uberto; Cagliani, Rachele; Comi, Giacomo P.; Riva, Stefania; Clerici, Mario; Bresolin, Nereo; Sironi, Manuela (8 June 2009). "Parasites represent a major selective force for interleukin genes and shape the genetic predisposition to autoimmune conditions". The Journal of Experimental Medicine. 206 (6): 1395–1408. doi:10.1084/jem.20082779. PMC 2715056. PMID 19468064.
  38. ^ a b c d Leong, Rupert W.; Mitrev, Nikola; Ko, Yanna (2016). "Hygiene Hypothesis: Is the Evidence the Same All Over the World?". Digestive Diseases. 34 (1–2): 35–42. doi:10.1159/000442922. PMID 26982573. S2CID 21373849.
  39. ^ Folkerts, Gert; Walzl, Gerhard; Openshaw, Peter J.M. (March 2000). "Do common childhood infections 'teach' the immune system not to be allergic?". Immunology Today. 21 (3): 118–120. doi:10.1016/s0167-5699(00)01582-6. PMID 10777250.
  40. ^ Kramer, A.; Bekeschus, S.; Bröker, B.M.; Schleibinger, H.; Razavi, B.; Assadian, O. (February 2013). "Maintaining health by balancing microbial exposure and prevention of infection: the hygiene hypothesis versus the hypothesis of early immune challenge". Journal of Hospital Infection. 83: S29–S34. doi:10.1016/S0195-6701(13)60007-9. PMID 23453173.
  41. ^ Lee, S. J.; Maizels, R. M. (18 April 2014). "Inflammatory Bowel Disease". Evolution, Medicine, and Public Health. 2014 (1): 95. doi:10.1093/emph/eou017. PMC 4204624. PMID 24747119.
  42. ^ Weinberg, Eugene G. (February 2000). "Urbanization and childhood asthma: An African perspective". Journal of Allergy and Clinical Immunology. 105 (2): 224–231. doi:10.1016/s0091-6749(00)90069-1. PMID 10669840.
  43. ^ Bufford, Jeremy D.; Gern, James E. (May 2005). "The Hygiene Hypothesis Revisited". Immunology and Allergy Clinics of North America. 25 (2): 247–262. doi:10.1016/j.iac.2005.03.005. PMID 15878454.
  44. ^ Osada, Yoshio; Kanazawa, Tamotsu (2010). "Parasitic Helminths: New Weapons against Immunological Disorders". Journal of Biomedicine and Biotechnology. 2010: 743758. doi:10.1155/2010/743758. PMC 2821776. PMID 20169100.
  45. ^ Lambrecht, Bart N; Hammad, Hamida (1 October 2017). "The immunology of the allergy epidemic and the hygiene hypothesis". Nature Immunology. 18 (10): 1076–1083. doi:10.1038/ni.3829. PMID 28926539. S2CID 6239349.
  46. ^ Marra, Fawziah; Lynd, Larry; Coombes, Megan; Richardson, Kathryn; Legal, Michael; FitzGerald, J. Mark; Marra, Carlo A. (March 2006). "Does Antibiotic Exposure During Infancy Lead to Development of Asthma?". Chest. 129 (3): 610–618. doi:10.1378/chest.129.3.610. PMID 16537858.
  47. ^ Thavagnanam, S.; Fleming, J.; Bromley, A.; Shields, M. D.; Cardwell, C. R. (April 2008). "A meta-analysis of the association between Caesarean section and childhood asthma". Clinical & Experimental Allergy. 38 (4): 629–633. doi:10.1111/j.1365-2222.2007.02780.x. PMID 18352976. S2CID 23077809.
  48. ^ Haspeslagh, Eline; Heyndrickx, Ines; Hammad, Hamida; Lambrecht, Bart N (October 2018). "The hygiene hypothesis: immunological mechanisms of airway tolerance". Current Opinion in Immunology. 54: 102–108. doi:10.1016/j.coi.2018.06.007. PMC 6202673. PMID 29986301.
  49. ^ Sanders, Mary Ellen; Guarner, Francisco; Guerrant, Richard; Holt, Peter R; Quigley, Eamonn MM; Sartor, R Balfour; Sherman, Philip M; Mayer, Emeran A (May 2013). "An update on the use and investigation of probiotics in health and disease". Gut. 62 (5): 787–796. doi:10.1136/gutjnl-2012-302504. PMC 4351195. PMID 23474420.
  50. ^ Rook, G. A. (23 October 2013). "Regulation of the immune system by biodiversity from the natural environment: An ecosystem service essential to health". Proceedings of the National Academy of Sciences. 110 (46): 18360–18367. Bibcode:2013PNAS..11018360R. doi:10.1073/pnas.1313731110. PMC 3831972. PMID 24154724.
  51. ^ Zaccone, P.; Fehervari, Z.; Phillips, J. M.; Dunne, D. W.; Cooke, A. (2006). "Parasitic worms and inflammatory diseases". Parasite Immunology. 28 (10): 515–23. doi:10.1111/j.1365-3024.2006.00879.x. PMC 1618732. PMID 16965287.
  52. ^ Weinstock, J V; Summers, R; Elliott, DE (2004). "Helminths and harmony". Gut. 53 (1): 7–9. doi:10.1136/gut.53.1.7. PMC 1773927. PMID 14684567.
  53. ^ Nutman, Thomas B.; Santiago, Helton C. (5 October 2016). "Human Helminths and Allergic Disease: The Hygiene Hypothesis and Beyond". The American Journal of Tropical Medicine and Hygiene. 95 (4): 746–753. doi:10.4269/ajtmh.16-0348. PMC 5062766. PMID 27573628.
  54. ^ a b Loke, P.; Lim, Y. A. L. (June 2015). "Helminths and the microbiota: parts of the hygiene hypothesis". Parasite Immunology. 37 (6): 314–323. doi:10.1111/pim.12193. PMC 4428757. PMID 25869420.
  55. ^ Taché, J.; Carpentier, B. (January 2014). "Hygiene in the home kitchen: Changes in behaviour and impact of key microbiological hazard control measures". Food Control. 35 (1): 392–400. doi:10.1016/j.foodcont.2013.07.026.
  56. ^ a b Bloomfield, Sally F.; Exner, Martin; Signorelli, Carlo; Nath, Kumar Jyoti; Scott, Elizabeth A (July 2012). "The Chain of Infection Transmission in the Home and Everyday Life Settings, and the Role of Hygiene in Reducing the Risk of Infection". Home Hygiene & Health. Archived from the original on 24 February 2021. Retrieved 27 April 2020.
  57. ^ Bloomfield, Sally F.; Exner, Martin; Fara, Gaetano M; Nath, Kumar Jyoti; Scott, Elizabeth A (October 2013). "Hygiene procedures in the home and their effectiveness: a review of the scientific evidence base". Home Hygiene & Health.
  58. ^ Ege, Markus J. (November 2017). "The Hygiene Hypothesis in the Age of the Microbiome". Annals of the American Thoracic Society. 14 (Supplement_5): S348–S353. doi:10.1513/AnnalsATS.201702-139AW. PMID 29161087.
  59. ^ Bloomfield, Sally F.; Exner, Martin; Fara, Gaetano M; Nath, Kumar Jyoti; Scott, Elizabeth A; Voorden, Carolien Van der (June 2009). "The global burden of hygiene-related diseases in relation to the home and community". Home Hygiene & Health.
  60. ^ Bloomfield, Sally F.; Scott, Elizabeth A. (May 2013). "A risk assessment approach to use of antimicrobials in the home to prevent spread of infection". American Journal of Infection Control. 41 (5): S87–S93. doi:10.1016/j.ajic.2013.01.001. PMID 23622757.

Further reading

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