Gut flora

From Wikipedia, the free encyclopedia

Jump to: navigation, search
Escherichia coli, one of the many species of bacteria present in the human gut.

The gut flora consists of the microorganisms that normally live in the digestive tract of animals. Though widely known as the "intestinal microflora", this is technically a misnomer since the word root "flora" pertains to plants and biota refers to microbial life such as bacteria other than plants. Thus recently, the more appropriate term intestinal microbiota is applied, though its use has not eclipsed the entrenched use and recognition of "flora" with regard to intestinal bacteria, and for the time being, both terms are being used in different textbooks.

The average human body, consisting of about 1013 (10,000,000,000,000 or about ten trillion) cells, has about ten times that number of microorganisms in the gut.[1][2][3][4] The metabolic activity performed by these bacteria is equal to that of a virtual organ causing some to describe the gut bacteria as a "forgotten" organ.[5]

Bacteria make up most of the flora in the colon[6] and 60% of the dry mass of feces.[2] This fact makes feces an ideal source to test for gut flora for any tests and experiments by extracting the nucleic acid from fecal specimens, and bacterial 16S rRNA gene sequences are generated with bacterial primers. This form of testing is ideal when compared to more invasive techniques, such as biopsies. Somewhere between 300[2] and 1000 different species live in the gut,[3] with most estimates at about 500.[5][7][4] However, it is probable that 99% of the bacteria come from about 30 or 40 species.[8] Fungi and protozoa also make up a part of the gut flora, but little is known about their activities.

Research suggests that the relationship between gut flora and humans is not merely commensal (a non-harmful coexistence), but rather is a mutualistic, symbiotic relationship.[3] Though people can survive with no gut flora,[4] the microorganisms perform a host of useful functions, such as fermenting unused energy substrates, training the immune system, preventing growth of harmful species,[2] regulating the development of the gut, producing vitamins for the host (such as biotin and vitamin K), and producing hormones to direct the host to store fats. However, in certain conditions, some species are thought to be capable of causing disease by causing infection or increasing cancer risk for the host.[2][6]

Contents

[edit] Localization

The colon has the greatest numbers of bacteria and the most different species, and the activity of these bacteria make the colon the most metabolically active organ in the body.[7] The acid in the stomach, as well as bile and pancreatic secretions, hinder colonization of most bacteria in the stomach and proximal small intestine.[5] Most of the bacteria in the distal small intestine are Gram-positive, while those in the colon are mostly Gram-negative.[9] The first part of the colon is mostly responsible for fermenting carbohydrates,[8][7][2] while the latter part mostly breaks down proteins and amino acids.[7][2] Bacterial growth is rapid in the cecum and ascending colon, which has a low pH, and slow in the descending colon, which has an almost neutral pH.[2] The body maintains the proper balance and locations of species by altering pH, the activity of the immune system, and peristalsis.[6]

Over 99% of the bacteria in the gut are anaerobes,[8][2][6][3][10] but in the cecum, aerobic bacteria reach high densities.[2]

[edit] Types

Candida albicans, a dimorphic fungus which grows as a yeast in the gut.

Not all the species in the gut have been identified[2][3] because some cannot be cultured,[8][3][11] so DNA isolation and identification is difficult.[12] Populations of species vary widely among different individuals but stay fairly constant within an individual over time, even though some alterations may occur with changes in lifestyle, diet and age.[2][5] An effort to better describe the microflora of the gut and other body locations has been initiated; see Human microbiome project.

Most bacteria come from the genera Bacteroides, Clostridium, Fusobacterium,[8][2][10] Eubacterium, Ruminococcus, Peptococcus, Peptostreptococcus, and Bifidobacterium.[2][8] Other genera such as Escherichia and Lactobacillus are present to a lesser extent.[2] Species from the genus Bacteroides alone constitute about 30% of all bacteria in the gut, suggesting that that genus is especially important in the functioning of the host.[3]

The currently known genera of fungi of the gut flora include Candida, Saccharomyces, Aspergillus, and Penicillium.

[edit] Acquisition of gut flora in human infants

The gastrointestinal tract of a normal fetus is sterile. During birth and rapidly thereafter, bacteria from the mother and the surrounding environment colonize the infant's gut. Immediately after vaginal delivery, babies have bacterial strains in the upper gastrointestinal tract derived from the mothers’ feces.[13] Infants born by caesarean section may also be exposed to their mothers’ microflora, but the initial exposure is most likely to be from environmental microbes such as the air, other infants, and the nursing staff which serve as vectors for transfer.[14] The primary gut flora in infants born by cesarean delivery may be disturbed for up to 6 months after birth whereas vaginally born infants take up to 1 month for their intestinal micro flora to be well established. After birth, environmental, oral and cutaneous bacteria are readily transferred from the mother to the infant through suckling, kissing, and caressing. All infants are initially colonized by large numbers of E. coli and streptococci. Within a few days, bacterial numbers reach 108 to 1010 per gram of feces.[14][15] During the first week of life, these bacteria create a reducing environment favorable for the subsequent bacterial succession of strict anaerobic species mainly belonging to the genera Bifidobacterium, Bacteroides, Clostridium, and Ruminococcus.[16] Breast-fed babies become dominated by bifidobacteria, possibly due to the contents of bifidobacterial growth factors in breast milk.[17] In contrast, the microbiota of formula-fed infants is more diverse with high numbers of Enterobacteriaceae, enterococci, bifidobacteria, Bacteroides, and clostridia.[18][19] After the introduction of solid food and weaning, the microflora of breast-fed infants becomes similar to that of formula-fed infants. By the second year of life the fecal microflora resembles that of adults.

[edit] Functions

Bacteria in the gut fulfills a host of useful functions for humans, including digestion of unutilized energy substrates;[20] stimulating cell growth; repressing the growth of harmful microorganisms; training the immune system to respond only to pathogens; and defending against some diseases.[2][3][21]

[edit] Carbohydrate fermentation and absorption

Without gut flora, the human body would be unable to utilize some of the undigested carbohydrates it consumes, because some types of gut flora have enzymes that human cells lack for breaking down certain polysaccharides.[3] Rodents raised in a sterile environment and lacking in gut flora need to eat 30% more calories just to remain the same weight as their normal counterparts.[3] Carbohydrates that humans cannot digest without bacterial help include certain starches; fiber; oligosaccharides and sugars that the body failed to digest and absorb[7][2][8] like lactose in the case of lactose intolerance and sugar alcohols, mucus produced by the gut, and proteins.[7]

Bacteria turn carbohydrates they ferment into short chain fatty acids, or SCFAs.[7][6][8] These materials can be used by host cells, providing a major source of useful energy and nutrients for humans.[7] They increase the gut's absorption of water, reduce counts of damaging bacteria, increase growth of human gut cells,[6] and are also used for the growth of indigenous bacteria.[2] The SCFAs are produced by a form of fermentation called saccharolytic fermentation[7] and include acetic acid, propionic acid, and butyric acid.[7][6][8] Gases and organic acids like lactic acid are also produced by saccahrolytic fermentation.[8] Acetic acid is used by muscle, propionic acid helps the liver produce ATP, and butyric acid provides energy to gut cells and may prevent cancer.[7]

Another, less favorable type of fermentation, proteolytic fermentation, breaks down proteins like enzymes, dead host and bacterial cells, and collagen and elastin found in food, and can produce toxins and carcinogens in addition to SCFAs. Thus a diet lower in protein lowers exposure to toxins.[2][6]

Evidence also suggests that bacteria enhance the absorption and storage of lipids.[3] Bacteria also produce and help the body absorb needed vitamins like vitamin K. In addition, the SCFAs they produce help the body absorb nutrients such as calcium, magnesium, and iron.[2]

[edit] Trophic effects

Another benefit of SCFAs is that they increase growth of intestinal epithelial cells and control their proliferation and differentiation.[2] They may also cause lymphoid tissue near the gut to grow. Bacterial cells also alter intestinal growth by changing the expression of cell surface proteins such as sodium/glucose transporters.[3] In addition, changes they make to cells may prevent injury to the gut mucosa from occurring.[21]

[edit] Repression of pathogenic microbial growth

C. difficile colonies on a blood agar plate. The overgrowth of C. difficile in the gut can be harmful to the host.

Another important role of helpful gut flora is that they prevent species that would harm the host from colonizing the gut; an activity termed the "barrier effect". Yeasts and harmful bacterial species such as Clostridium difficile (the overgrowth of which can cause pseudomembranous colitis) are unable to grow too much due to competition from helpful gut flora species to adhere to the mucosal lining of the intestine, thus animals without gut flora are infected very easily. The barrier effect protects humans from both invading species and species normally present in the gut at low numbers, whose growth is usually inhibited by the gut flora.[2]

Helpful bacteria prevent the growth of pathogenic species by competing for nutrition and attachment sites to the epithelium of the colon. Symbiotic bacteria are more at home in this ecological niche and are thus more successful in the competition. The indigenous bacteria send chemical signals to the host about the amount of nutrients they need, and the host provides only that much, so harmful bacteria are starved out. Indigenous gut floras also produce bacteriocins which are proteinacious toxins that inhibit growth of similar bacterial strains, substances which kill harmful microbes and the levels of which can be regulated by enzymes produced by the host.[2]

The process of fermentation, since it produces fatty acids, also serves to lower the pH in the colon, preventing the proliferation of harmful species of bacteria and facilitating that of helpful species. The pH may also enhance the excretion of carcinogens.[7] Lactic bacteria such as Acidophilus and Bifidiobacterium, have a specific property of transforming sugars into lactic acid and acetic acid which will carry out the same job as fermentation; decrease the pH of the intestine and produce substances that suppress harmful bacteria.

[edit] Immunity

Gut flora have a continuous and dynamic effect on the host's gut and systemic immune systems. The bacteria are key in promoting the early development of the gut's mucosal immune system both in terms of its physical components and function and continue to play a role later in life in its operation. The bacteria stimulate the lymphoid tissue associated with the gut mucosa to produce antibodies to pathogens. The immune system recognizes and fights harmful bacteria, but leaves the helpful species alone, a tolerance developed in infancy.[2][11][4][6]

As soon as an infant is born, bacteria begin colonizing its digestive tract. The first bacteria to settle in are able to affect the immune response, making it more favorable to their own survival and less so to competing species; thus the first bacteria to colonize the gut are important in determining the person's lifelong gut flora makeup. However, there is a shift at the time of weaning from predominantly facultative aerobic species such as Streptococci and Escherichia coli to mostly obligate anaerobic species.[2][3]

Recent findings have shown that gut bacteria play a role in the expression of Toll-like receptors (TLRs) in the intestines, molecules that help the host repair damage due to injury. TLRs cause parts of the immune system to repair injury caused for example by radiation.[3][21] TLRs are one of the two pattern recognition receptors (PRR) that provide the intestine the ability to discriminate between the pathogenic and commensal bacteria. These PRRs identify the pathogens that have crossed the mucosal barriers and trigger a set of responses that take action against the pathogen which involve 3 main immunosensory cells; surface enterocytes, M cells and dendritic cells. [5]

The other PRR is the nucleotide-binding oligomerization domain/caspase recruitment domain isoforms (NOD/CARD) which is a cytoplasmic protein that recognizes endogenous or microbial molecules or stress responses and forms oligomers that activate inflammatory caspases. This would result in the cleavage and activation of important inflammatory cytokines and/or activate NF-kB signaling pathway to induce the production of inflammatory molecules.[5]

Bacteria can influence the phenomenon known as oral tolerance, in which the immune system is less sensitive to an antigen (including those produced by gut bacteria) once it has been ingested. This tolerance, mediated in part by the gastrointestinal immune system and in part by the liver, can reduce an overreactive immune response like those found in allergies and auto-immune disease.[22]

Some species of gut flora, such as some of those in the Bacteroides genus, are able to change their surface receptors to mimic those of host cells in order to evade immune response. Bacteria with neutral and harmful effects on the host can also use these types of strategies. The host immune system has also adapted to this activity, preventing overgrowth of harmful species.[2][4]

[edit] Metabolic Function

The resident gut microflora positively control the intestinal epithelial cell differentiation and proliferation through the production of short-chain fatty acids. They also mediate other metabolic effects such as the syntheses of vitamins like biotin and folate as well as absorption of ions including Magnesium, Calcium and Iron.[5]

The gut flora plays a major role in metabolizing dietary carcinogens[5]; the microcomponents and the macrocomponents. The microcomponents are genotoxic and the major focus is on recent advances in heterocyclic amines (HCAs) which are produced by cooking proteinaceous food such as meat and fish which can then induce tumors in organs like breast, colon and prostate. HCAs are naturally occurring therefore the complete avoidance of them is impractical which is why the metabolic function of gut flora of such components is of great importance to our body as this would help in prevention of such tumors that are difficult to avoid. The macrocomponents consists of the excessive intake of fat and sodium chloride which can later promote tumors such as in breasts and colons from fat and gastric carcinogenesis from sodium chloride.[23]

[edit] Preventing allergy

Bacteria are also implicated in preventing allergies,[1] an overreaction of the immune system to non-harmful antigens. Studies on the gut flora of infants and young children have shown that those who have or later develop allergies have different compositions of gut flora from those without allergies, with higher chances of having the harmful species C difficile and S aureus and lower prevalence of Bacteroides and Bifidobacteria.[1] One explanation is that since helpful gut flora stimulate the immune system and "train" it to respond properly to antigens, a lack of these bacteria in early life leads to an inadequately trained immune system which overreacts to antigens.[1] On the other hand, the differences in flora could be a result, not a cause, of the allergies.[1]

[edit] Preventing inflammatory bowel disease

Another indicator that bacteria help train the immune system is the epidemiology of Inflammatory Bowel Disease, or IBD, such as Crohn's Disease (CD). Some authors suggest that SCFAs prevent IBD. In addition, some forms of bacteria can prevent inflammation.[24] The incidence and prevalence of IBD is high in industrialized countries with a high standard of living and low in less economically developed countries, having increased in developed countries throughout the twentieth century. The disease is also linked to good hygiene in youth; lack of breastfeeding; and consumption of large amounts of sucrose and animal fat.[24] Its incidence is inversely linked with poor sanitation during the first years of life and consumption of fruits, vegetables, and unprocessed foods.[24] Also, the use of antibiotics, which kill native gut flora and harmful infectious pathogens alike, especially during childhood, is associated with inflammatory bowel disease.[20] On the other hand, using probiotics, bacteria consumed as part of the diet that impart health benefits (aside from just nutrition), helps treat IBD.

[edit] Alterations in balance

[edit] Effects of antibiotic use

Altering the numbers of gut bacteria, for example by taking broad-spectrum antibiotics, may affect the host's health and ability to digest food.[25] People may take the drugs to cure bacterial illnesses or may unintentionally consume significant amounts of antibiotics by eating the meat of animals to which they were fed.[25] Antibiotics can cause antibiotic-associated diarrhea (AAD) by irritating the bowel directly, changing the levels of gut flora, or allowing pathogenic bacteria to grow.[8] Another harmful effect of antibiotics is the increase in numbers of antibiotic-resistant bacteria found after their use, which, when they invade the host, cause illnesses that are difficult to treat with antibiotics.[25]

Changing the numbers and species of gut flora can reduce the body's ability to ferment carbohydrates and metabolize bile acids and may cause diarrhea. Carbohydrates that are not broken down may absorb too much water and cause runny stools, or lack of SCFAs produced by gut flora could cause the diarrhea.[8]

A reduction in levels of native bacterial species also disrupts their ability to inhibit the growth of harmful species such as C. difficile and Salmonella kedougou, and these species can get out of hand, though their overgrowth may be incidental and not be the true cause of diarrhea.[8][25][2]

Gut flora composition also changes in severe illnesses, due not only to antibiotic use but also to such factors as ischemia of the gut, failure to eat, and immune compromise. Negative effects from this have led to interest in selective digestive tract decontamination (SDD), a treatment to kill only pathogenic bacteria and allow the reestablishment of healthy ones.[26]

[edit] Pharmabiotics

Pharmabiotics is a generic term to encompass any form of therapeutic exploitation of the commensal flora, including the use of live probiotic bacteria, probiotic-derived biologically active metabolites, prebiotics, synbiotics or genetically modified commensal bacteria.[5] Since the lack of gut flora can have such harmful health effects, the use of probiotics has anti-inflammatory effects in the gut and may be useful for improving health. Prebiotics are dietary components that can help foster the growth of microorganisms in the gut, which may lead to better health.[24] There is evidence supporting a therapeutic role for probiotic strategies for treating mucosal inflammatory disorders such as IBD, atopy, infection, diarrhoea, cancer and arthritis.[5]

[edit] Role in disease

Bacteria in the digestive tract have pathogenic properties in addition to their health-inducing ones: they can produce toxins and carcinogens[6] and have been implicated in such conditions as multisystem organ failure, sepsis, colon cancer, and IBD.[2] A major factor in health is the balance of bacterial numbers; if the numbers grow too high or low, it will result in harm to the host. The host has enzymes to regulate this balance.[6]

[edit] Cancer

Some genera of bacteria, such as Bacteroides and Clostridium, have been associated with an increase in tumor growth rate, while other genera like Lactobacillus and Bifidobacteria are known to prevent tumor formation.[2]

[edit] Translocation

Helpful bacteria can be very harmful to the host if they get outside of the intestinal tract.[3][6][10] Translocation, which occurs when bacteria leave the gut through its mucosal lining, the border between the lumen of the gut and the inside of the body,[4][27] can occur in a number of different diseases.[10][24] It can be caused by too much growth of bacteria in the small intestine, reduced immunity of the human, or increased gut lining permeability.[24] The gut can become more permeable in diseases like cirrhosis, which is damaging due in part to the activity of gut flora.[28]

If the gut is perforated, bacteria can invade the body, causing a potentially fatal infection. Aerobic bacteria can make infection by anaerobes worse by using up all available oxygen and creating an environment favorable to anaerobes.[10]

[edit] Inflammatory bowel disease

Some suspect that IBD is due to a reduction in immune tolerance and subsequent overreaction of the host's immune system to harmful or non-harmful bacteria. IBD may be caused by the entire gut flora together or some specific types.[20][29]

It has been noted that though Ulcerative Colitis and Crohn's disease (two types of IBD) probably have genetic components, they are not inherited in a Mendelian fashion and are thus probably due to a complex set of factors rather than solely to a gene.[29] Though neither bacterial colonization nor genetics is sufficient to cause the disease, bacteria probably play a role in these disorders.[29]

Some suspect that inflammation in IBD is due to increased permeability of the inner lining of the colon, which may allow bacteria to invade the tissues and cause an immune reaction that leads prolonged inflammation.[4][27] Tissue damage in IBD results from the immunological misperception of danger within the naturally occurring flora or due to failure of normal tolerance to pathogenic bacteria. It is still unclear whether the inflammation that occurs is due to a specific subset of intestinal microbes or due to a problem with the tolerance of commensal gut flora.[5] Abnormal tight junctions, which are supposed to prevent permeability, have been found in cells of patients with IBD.[27] Because of the potentially harmful role of these bacteria, antibiotics are frequently prescribed to treat Crohn’s disease.[21] However, inflammation could occur first and cause the increased intestinal permeability found in diseases such as Crohn's, so the causative role of bacteria is not clear.[27] Conventional therapies for IBD primarily target the mucosal inflammatory responses by using pharmabiotics.[5]

[edit] Colitis

It has been suggested that commensal bacteria are responsible for the development of colitis, since mice raised in a sterile environment do not get the disease.[30] However, while some bacterial strains such as C. difficile[24] and even normal gut bacteria cause colitis,[30] others prevent the disease in mice.[24]

[edit] Obesity

It is known from experiments on mice that obese mice lacking leptin, a lipid metabolism regulator (ob/ob mice), have a distinct gut flora compared to (normal) lean mice, reflected in a change in the ratio between bacteria from the divisions Bacteroidetes and Firmicutes, which is shifted towards less Bacteroidetes and more Firmicutes in obese mice.

The microbes occupying the human gut are also in direct relation to obesity. A shift in the ratio between bacterial-divisions Firmicutes and Bacteroidetes can be observed in lean and obese individuals – in latter a shift towards Firmicutes can be observed. The ratio between Firmicutes and Bacteroidetes dynamically reflects the overall weight-condition of an individual, shifting towards Bacteroidetes if an obese individual loses weight.

The mutual influence of gut flora composition and weight-condition is connected to differences in the energy-reabsorbing potential of different ratios of Firmicutes and Bacteroidetes, especially in the digestion of fatty acids and dietary polysaccharides, as shown by experiments wherein the (caecum) gut flora of obese mice was transplanted into germ free recipient mice, leading to an increase in weight despite a decrease in food consumption.[31][32][33][34]

[edit] See also

[edit] Sources and notes

  1. ^ a b c d e Björkstén B, Sepp E, Julge K, Voor T, and Mikelsaar and M. 2001. Allergy development and the intestinal microflora during the first year of life. Journal of Allergy and Clinical Immunology, Volume 108, Issue 4, Pages 516-520. PMID 11590374.
  2. ^ a b c d e f g h i j k l m n o p q r s t u v w x y z aa ab ac Guarner F and Malagelada JR. 2003. Gut flora in health and disease. The Lancet, Volume 361, Issue 9356, 8 February 2003, Pages 512-519. PMID 12583961.
  3. ^ a b c d e f g h i j k l m n o Sears CL. 2005. A dynamic partnership: Celebrating our gut flora. Anaerobe, Volume 11, Issue 5, Pages 247-251. PMID 16701579.
  4. ^ a b c d e f g Steinhoff U. 2005. Who controls the crowd? New findings and old questions about the intestinal microflora. Immunology Letters, Volume 99, Issue 1, June , Pages 12-16. PMID 15894105. doi:10.1016/j.imlet.2004.12.013
  5. ^ a b c d e f g h i j k l Ann M O'Hara, Fergus Shanahan The gut flora as a forgotten organ. EMBO reports 7, 688 - 693 (01 Jul 2006)
  6. ^ a b c d e f g h i j k l University of Glasgow. 2005. The normal gut flora. Available through web archive. Accessed May 22, 2008
  7. ^ a b c d e f g h i j k l Gibson RG. 2004. Fibre and effects on probiotics (the prebiotic concept). Clinical Nutrition Supplements, Volume 1, Issue 2, Pages 25-31.
  8. ^ a b c d e f g h i j k l m Beaugerie L and Petit JC. 2004. Microbial-gut interactions in health and disease. Antibiotic-associated diarrhoea. Best Practice & Research Clinical Gastroenterology, Volume 18, Issue 2, Pages 337-352. PMID 15123074.
  9. ^ Riordan SM, McIver CJ, Wakefield D, Duncombe VM, Thomas MC, and Bolin TD. 2001. Small intestinal mucosal immunity and morphometry in luminal overgrowth of indigenous gut flora. The American Journal of Gastroenterology, Volume 96, Issue 2, Pages 494-500. PMID 11232696. Accessed September 15, 2007
  10. ^ a b c d e Vedantam G and Hecht DW. 2003. Antibiotics and anaerobes of gut origin. Current Opinion in Microbiology, Volume 6, Issue 5, Pages 457-461. PMID 14572537. Accessed September 15, 2007
  11. ^ a b Shanahan F. 2002. The host–microbe interface within the gut. Best Practice & Research Clinical Gastroenterology, Volume 16, Issue 6, Pages 915-931. PMID 12473298. Accessed September 15, 2007
  12. ^ Nordgård L, Traavik T, and Nielsen KM. 2005. Nucleic acid isolation from ecological samples—vertebrate gut flora. Methods in Enzymology, Volume 395, Pages 38-48. PMID 15865959. Accessed September 7, 2007
  13. ^ Bettelheim KA, Breadon A, Faiers MC, O'Farrell SM, Shooter RA. 1974. The origin of O serotypes of Escherichia coli in babies after normal delivery. Journal of Hygiene, Volume 72, Issue 1, Pages 67-70. PMID 4593741. Accessed September 3, 2007
  14. ^ a b Schwiertz A, Gruhl B, Lobnitz M, Michel P, Radke M, Blaut M. 2003. Development of the intestinal bacterial composition in hospitalized preterm infants in comparison with breast-fed, full-term infants. Pediatric Research, Volume 54, Issue 3, Pages 393-399. PMID 12788986. Accessed September 3, 2007
  15. ^ Mackie RI, Sghir A, Gaskins HR. 1999.Developmental microbial ecology of the neonatal gastrointestinal tract. American Journal of Clinical Nutrition, Volume 69, Issue 5, Pages 1035S-1045S. PMID 10232646. Accessed September 7, 2007
  16. ^ Favier CF, Vaughan EE, De Vos WM, Akkermans AD. 2002. Molecular monitoring of succession of bacterial communities in human neonates. Applied and Environmental Microbiology, Volume 68, Issue 1, Pages 219-226. PMID 11772630.
  17. ^ Coppa GV, Bruni S, Morelli L, Soldi S, Gabrielli O. 2004. The first prebiotics in humans: human milk oligosaccharides. Journal of Clinical Gastroenterology, Volume 38, Supplement 6, Pages S80-S83. PMID 15220665. Accessed September 3, 2007
  18. ^ Harmsen HJ, Wildeboer-Veloo AC, Raangs GC, Wagendorp AA, Klijn N, Bindels JG, Welling GW. 2000. Analysis of intestinal flora development in breast-fed and formula-fed infants by using molecular identification and detection methods. Journal of Pediatric Gastroenterology and Nutrition, Volume 30, Issue 1, Pages 61-67. PMID 10630441. Accessed September 7, 2007
  19. ^ Fanaro S, Chierici R, Guerrini P, Vigi V. 2003. Intestinal microflora in early infancy: composition and development. Acta Paediatrica, Volume 91, Issue 441, Pages 48-55. PMID 14599042. Accessed September 3, 2007
  20. ^ a b c Wynne AG, McCartney AL, Brostoff J, Hudspith BN, Glenn GR and Gibson G. 2004. An in vitro assessment of the effects of broad-spectrum antibiotics on the human gut microflora and concomitant isolation of a Lactobacillus plantarum with anti-Candida activities. Anaerobe, Volume 10, Issue 3, Pages 165-169. PMID 16701514. Accessed September 3, 2007
  21. ^ a b c d Keeley J. 2004. Good bacteria trigger proteins to protect the gut. Howard Hughes Medical Institute. EurekAlert. Accessed January 9, 2007
  22. ^ Jewell AP. 2005. Is the liver an important site for the development of immune tolerance to tumours? Medical Hypotheses, Volume 64, Issue 4, Pages 751-754. PMID 15694692. Accessed September 7, 2007
  23. ^ Sugimura, Takashi."Nutrition and Dietary Carcinogenesis.Carcinogenesis.21 (2000): 387-395.
  24. ^ a b c d e f g h Guarner F and Malagelada JR. 2003. Role of bacteria in experimental colitis. Best Practice & Research Clinical Gastroenterology, Volume 17, Issue 5, October 2003, Pages 793-804. PMID 14507589. Accessed September 15, 2007
  25. ^ a b c d Carman RJ, Simon MA, Fernández H, Miller MA, and Bartholomew MJ. 2004. Ciprofloxacin at low levels disrupts colonization resistance of human fecal microflora growing in chemostats. Regulatory Toxicology and Pharmacology, Volume 40, Issue 3, December, Pages 319-326. PMID 15546686. Accessed September 7, 2007
  26. ^ Knight DJW and Girling KJ. 2003. Gut flora in health and disease. The Lancet, Volume 361, Issue 9371, Page 1831. Accessed January 7, 2007
  27. ^ a b c d Suenaert P, Bulteel V, Lemmens L, Noman M, Geypens B, Assche GV, Geboes K, Ceuppens JL and Rutgeert P. 2002. Anti-tumor necrosis factor treatment restores the gut barrier in Crohn’s disease. The American Journal of Gastroenterology, Volume 97, Issue 8, Pages 2000-2004. PMID 12190167. Accessed September 7, 2007
  28. ^ Garcia-Tsao G and Wiest R. 2004. Gut microflora in the pathogenesis of the complications of cirrhosis. Best Practice & Research Clinical Gastroenterology, Volume 18, Issue 2, Pages 353-372. PMID 15123075. Accessed September 7, 2007
  29. ^ a b c Hugot JP. 2004. Inflammatory bowel disease: a complex group of genetic disorders. Best Practice & Research Clinical Gastroenterology, Volume 18, Issue 3, Pages 451-462. PMID 15157820. Accessed September 7, 2007
  30. ^ a b Veltkamp C, Tonkonogy SL, De Jong YP, Albright C, Grenther WB, Balish E, Terhorst C, and Sartor RB. 2001. Continuous stimulation by normal luminal bacteria is essential for the development and perpetuation of colitis in Tg(epsilon26) mice. Gastroenterology, Volume 120, Issue 4, Pages 900-913. PMID 11231944. Accessed September 7, 2007
  31. ^ Ley RE, Turnbaugh PJ, Klein S, Gordon JI. Microbial ecology: human gut microbes associated with obesity. Nature, 2006 Volume 444, Issue 7122, Pages 1022-1023. PMID 17183309. Accessed September 7, 2007
  32. ^ Turnbaugh PJ, Ley RE, Mahowald MA, Magrini V, Mardis ER, Gordon JI. 2006. An obesity-associated gut microbiome with increased capacity for energy harvest. Nature, Volume 444, Issue 7122, Pages 1027-1031. PMID 17183312. Accessed September 7, 2007
  33. ^ Bäckhed F, Manchester JK, Semenkovich CF, Gordon JI. 2007. Mechanisms underlying the resistance to diet-induced obesity in germ-free mice. Proceedings of the National Academy of Sciences of the USA, Volume 104, Issue 3, Pages 979-984. PMID 17210919. Accessed September 7, 2007
  34. ^ Bäckhed F, Ding H, Wang T, Hooper LV, Koh GY, Nagy A, Semenkovich CF, Gordon JI. The gut microbiota as an environmental factor that regulates fat storage. Proceedings of the National Academy of Sciences of the USA, Volume 101, Issue 44, Pages 15718-15723. PMID 15505215. Accessed September 7, 2007
Personal tools