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--- home:pathogenesis:evidence_bacteria [08.29.2012] – [Other evidence] paulalbert
+++ home:pathogenesis:evidence_bacteria [01.13.2020] – [Other evidence] sallieq
@@ Line 38: / Line 38: @@
   * **Treatment response** –  Whatever the chronic inflammatory condition, patients on the Marshall Protocol invariably experience the tell-tale immunopathological reaction, which can only be described as a bacterial die-off reaction. Though a number of other antibacterial treatments are ultimately less effective than the MP, patients also respond to these. Even high-dose antibiotics, which has a well-deserved reputation for being ineffective over the long term, do cause fundamental changes in disease symptoms of supposedly non-infectious diseases.
   * <html><span id="microbepopulations"></span></html>**Microbe populations** – Bacteria populations in patients with a given chronic disease have been shown to be different compared to those found in controls. Patients with autism have different bacteria in their gastrointestinal tract(({{pubmed>long:16157555}})) (({{pubmed>long:15459553}})) than do healthy infants as do those babies who later in life become obese or overweight.(({{pubmed>long:18326589}})) A team at Washington University has shown that the types of microbes in obese humans and mice are different when compared to those of normal weight; obese humans and mice have a 50% relative reduction in the abundance of Bacteroidetes and a proportional increase in Firmicutes.(({{pubmed>long:16033867}})) The team further showed that when the chronic disease obesity is decreased in humans through a low-calorie diet, the relative proportion of microbes changes.(({{pubmed>long:17183309}})) Finally, the group showed that obesity is transmissible: Ley et al took germ-free mice of normal weight, colonized their guts with an "obese microbiota", and found a significantly greater increase in total body fat than those mice colonized with a "lean microbiota."(({{pubmed>long:17183312}}))
-  * **[[home:diseases:co-infections|Co-infections]]** - Persistent co-infections, including fungi and viruses, are generally a sign of disease driven by infection. According to the Marshall Pathogenesis, these co-infections are able to proliferate because such chronic infections are able to slow the innate immune response. The presence of co-infections able to persist because the host is immunocompromised is common across all chronic disease types.  For example, a wide range of pathogens - at least have been found in the granuloma of sarcoidosis patients. According to Nicolson: "A large subset of ASD [autism spectrum disorder] patients shows evidence of bacterial and/or viral infections." (({{pubmed>long:17265454}}))  He reports that his team found conclusive evidence of Mycoplasma ssp., Chlamydia pneumoniae, and human herpes virus-6 coinfections in ASD patients.
+  * **[[home:diseases:co-infections|Co-infections]]** - Persistent co-infections, including fungi and viruses, are generally a sign of disease driven by infection. According to the Marshall Pathogenesis, these co-infections are able to proliferate because such chronic infections are able to slow the innate immune response. The presence of co-infections able to persist because the host is immunocompromised is common across all chronic disease types.  For example, a wide range of pathogens - at least have been found in the granuloma of sarcoidosis patients. According to Nicolson: "A large subset of ASD [autism spectrum disorder] patients shows evidence of bacterial and/or viral infections." (({{pubmed>long:17265454}}))  He reports that his team found conclusive evidence of Mycoplasma ssp., Chlamydia pneumoniae, and human herpes virus-6 co-infections in ASD patients.
 [{{ :home:pathogenesis:microbiota:gestationalage.gif|**Newer cultivation techniques have associated bacterial count in a pregnant woman's amniotic fluid with age at delivery.** This data strongly suggests a causative role for pathogenic bacteria in premature delivery. Source: [[http://www.ncbi.nlm.nih.gov/pubmed/18725970|DiGulio et al.]]}}]
   * **Failure of lifestyle interventions** – It has been widely hypothesized that lifestyle factors, including a poor diet and a lack of exercise, are the primary driver behind increased rates of chronic disease. For example, the World Health Organization [[http://www.who.int/dietphysicalactivity/publications/facts/obesity/en/|has termed]] "an obesity epidemic," but even the most ambitious obesity intervention programs, which have gone to great lengths to increase rates of exercise and improve eating habits of a population, have been failures. One 1999 $200,000 NIH-funded intervention, known as the Pathways program, was performed on two groups of children. Pathways involved a substantial increase in physical education programs, classes about nutrition, significant reduction in fat and calorie content of all school meals, and several other health related measures - and all as part of a randomized controlled trial, the gold standard in studies. The primary goal of the study was to reduce the rate of body fat in the intervention group, but after the three-year intervention the percent of body fat in both groups was essentially identical. The researchers were unable to explain the failure of their intervention.(({{pubmed>long:14594792}})) Other such trials for obesity have been equally unsuccessful.(({{pubmed>long:17028105}}))
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 If the common inflammatory diseases (including autoimmune diseases) were genetic, the only way they would manage not to be weeded out of the population would be if they conferred some sort of beneficial survival trait not related to the disease.
-To date, no such benefits have been identified in any chronic disease, schizophrenia being a good example.(({{pubmed>long:12878806}})) Schizophrenics have a high suicide rate, few children, and a high rate of abnormality in their children.(({{pubmed>long:10978869}})) (({{pubmed>long:8885043}})) Schizophrenic mothers are more likely than non-schizophrenics to have stillborn babies and children with congenital malformations.(({{pubmed>long:11448375}})) On the contrary, incidence of the disease is only escalating suggesting that bacteria are passed from generation to generation. This would mean schizophrenic mothers and fathers would be less likely to pass on a theoretical schizophrenic gene to their offspring.
+To date, no such benefits have been identified in any chronic disease, schizophrenia being a good example.(({{pubmed>long:12878806}})) Schizophrenics have a high suicide rate, few children, and a high rate of abnormality in their children.(({{pubmed>long:10978869}})) (({{pubmed>long:8885043}})) Schizophrenic mothers are more likely than non-schizophrenics to have stillborn babies and children with congenital malformations.(({{pubmed>long:11448375}})) This would mean schizophrenic mothers and fathers would be less likely to pass on a theoretical schizophrenic gene to their offspring. On the contrary, incidence of the disease is only escalating suggesting that bacteria are passed from generation to generation.

home/pathogenesis/evidence_bacteria.txt · Last modified: 09.14.2022 by 127.0.0.1