By 品璉 江 - originally posted to Flickr as [1]This file has been extracted from another file: Taipei panorama.jpg, CC BY 2.0, https://commons.wikimedia.org/w/index.php?curid=79310952
Taipei, home to Lactobacillus plantarum PS128, isolated from fu-tsai, which is a spontaneously fermented mustard product
Our reader Prada is a fan of the Biogaia Gastrus probiotic and did comment recently that her doctor does not believe in SIBO (Small Intestinal Bacterial Overgrowth). We know that many doctors, particularly in English-speaking countries, believe that probiotics have no serious medical value. Many autism parents think their child has SIBO and give them probiotics, among other therapies.
Unless there is a consistently reliable diagnostic test that is affordable and widely available, you inevitably get the situation where patients are convinced that they have a condition (SIBO, PANS/PANDAS, Fibromyalgia etc) while their local doctor thinks it is all in their imagination.
When it comes to probiotic bacteria as a therapy, Italian doctors take them entirely seriously, while many English-speaking doctors regard them as little more than a placebo. I discovered to my surprise 20 years ago that some really do work.
One reader of this blog in Italy was recommended the new Taiwanese-developed “Psychobiotic” Neuraxbio (Lactobacillus plantarum PS128) by her gastroenterologist and found it was beneficial for her child’s stereotypy. Anyway, her enthusiasm brought me back to Psychobiotics.
I did consider writing a post a while back on Psychobiotics, which are probiotic bacteria that can provide reliable modulation of something useful inside the brain and may have nothing to do with treating GI problems. It is a nice idea, but the problem is the “reliable” part. In this blog we have already seen that in some people certain commercially available probiotics can have a benefit on behaviour. The problem is that in most people there was either no effect, or actually a negative effect.
There is a small probiotic company in Taiwan, called Bened, that is developing products specifically targeting neurological conditions, including: -
· Depression
· Autism
· ADHD
· Parkinson’s disease
In 2016 they patented their first product, Lactobacillus plantarum PS128 (isolated from fu-tsai) and started selling it in Asia, where it is widely available and now it is sold in Europe and the US.
In Hong Kong it is sold as “Smart Kids Probiotics” (智樂益生素), under the brand Boost & Guard (補健).
In France it is sold as Neurobiotique, in Italy as Neuraxbio and in the US as Solace. The US vendor has an easy to read brochure
For readers in the Balkans, PS128 is also coming your way soon, Corona virus permitting.
In Bened’s view, the current opportunities are: -
· Psychobiotics, that regulate both serotonin and dopamine and can treat anxiety and depression. (Lactobacillus plantarum PS128)
“Chronic administration of Lactobacillus plantarum PS128 significantly ameliorates anxiety and depression-like behaviors, increases dopaminergic activity in the prefrontal cortex, and reduced stress-induced elevation of serum corticosterone and inflammatory cytokine levels in mice subjected to early maternal separation. Oral administration with Lactobacillus plantarum PS128 significantly decreases visceral hypersensitivity in a rat animal model. Lactobacillus plantarum PS128 shows potential for irritable bowel syndrome (IBS) treatment.”
· Immunobiotics, that rebalance the production of Th1/Th2 cytokines (Lactococcus lactis A17)
“In vitro experiment reveals cytokines IFN-γ production by human peripheral blood mononuclear cells stimulated with Lactococcus lactis A17 is higher compared with those with other 17 Lactic acid bacteria strains, including Lactobacillus rhamnosus GG and Lactobacillus casei strain Shirota. The Ovalbumin (OVA)-sensitized BALB/c mouse model was further conducted to further examine the Immunomodulatory activities of A17. Repression of NOD-1, NOD-2, TLR-4 production”
· Metabolicbiotics, that reduce weight, cholesterol and triglycerides in those with a high fat diet (Lactobacillus plantarum K21)
“Supplementation of Lactobacillus plantarum K21 appeared to alleviate body weight gain and epididymal fat mass accumulation, reduce plasma leptin levels, decrease cholesterol and triglyceride levels, and mitigate liver damage in diet-induced obese mice. In addition, Lactobacillus plantarum K21 supplementation strengthens intestinal permeability and modulates the amount of Lactobacillus spp., Bifidobacterium spp., and Clostridium perfringens in the cecal contents of diet-induced obese mice. Dietary intake of Lactobacillus plantarum K21 does protect against the onset of high-fat diet induced obesity through multiple mechanisms of action.”
What does Lactobacillus PS128 do?
The research suggests that PS128 affects serotonin and dopamine while also being anti-inflammatory by reducing the expression of the inflammatory cytokine IL-6 and increasing the expression of the anti-inflammatory cytokine IL-10. In the jargon, it shifts the Th1/Th2 balance.
Psychotropic effects of Lactobacillus plantarum PS128 in early life-stressed and naïve adult mice.
Highlights
· We found a Lactobacillus plantarum strain PS128 changed emotional behaviors.
· PS128 reduced depression-like behavior in ELS mice.
· PS128 reduced anxiety-like behavior in normal adult mice.
· PS128 modulated prefrontal cortical serotonergic and dopaminergic systems.
Ingestion of specific probiotics, namely "psychobiotics", produces psychotropic effects on behavior and affects the hypothalamic-pituitary-adrenal axis and neurochemicals in the brain. We examined the psychotropic effects of a potential psychobiotic bacterium, Lactobacillus plantarum strain PS128 (PS128), on mice subjected to early life stress (ELS) and on naïve adult mice. Behavioral tests revealed that chronic ingestion of PS128 increased the locomotor activities in both ELS and naïve adult mice in the open field test. In the elevated plus maze, PS128 significantly reduced the anxiety-like behaviors in naïve adult mice but not in the ELS mice; whereas the depression-like behaviors were reduced in ELS mice but not in naïve mice in forced swimming test and sucrose preference test. PS128 administration also reduced ELS-induced elevation of serum corticosterone under both basal and stressed states but had no effect on naïve mice. In addition, PS128 reduced inflammatory cytokine levels and increased anti-inflammatory cytokine level in the serum of ELS mice. Furthermore, the dopamine level in the prefrontal cortex (PFC) was significantly increased in PS128 treated ELS and naïve adult mice whereas serotonin (5-HT) level was increased only in the naïve adult mice. These results suggest that chronic ingestion of PS128 could ameliorate anxiety- and depression-like behaviors and modulate neurochemicals related to affective disorders. Thus PS128 shows psychotropic properties and has great potential for improving stress-related symptoms.
Alteration of behavior and monoamine levels attributable to Lactobacillus plantarum PS128 in germ-free mice.
Probiotics, defined as live bacteria or bacterial products, confer a significant health benefit to the host, including amelioration of anxiety-like behavior and psychiatric illnesses. Here we administered Lactobacillus plantarum PS128 (PS128) to a germ-free (GF) mouse model to investigate the impact of the gut-brain axis on emotional behaviors. First, we demonstrated that chronic administration of live PS128 showed no adverse effects on physical health. Then, we found that administration of live PS128 significantly increased the total distance travelled in the open field test and decreased the time spent in the closed arm in the elevated plus maze test, whereas the administration of PS128 had no significant effects in the depression-like behaviors of GF mice. Also, chronic live PS128 ingestion significantly increased the levels of both serotonin and dopamine in the striatum, but not in the prefrontal cortex or hippocampus. These results suggest that the chronic administration of PS128 is safe and could induce changes in emotional behaviors. The behavioral changes are correlated with the increase in the monoamine neurotransmitters in the striatum. These findings suggest that daily intake of the L. plantarum strain PS128 could improve anxiety-like behaviors and may be helpful in ameliorating neuropsychiatric disorders.
New perspectives of Lactobacillus plantarum as a probiotic: The gut-heart-brain axis
Lactobacillus plantarum is a non-gas-producing lactic acid bacterium that is generally regarded as safe (GRAS) with Qualified Presumption of Safety (QPS) status. Although traditionally used for dairy, meat and vegetable fermentation, L. plantarum is gaining increasing significance as a probiotic. With the newly acclaimed gut-heart-brain axis, strains of L. plantarum have proven to be a valuable species for the development of probiotics, with various beneficial effects on gut health, metabolic disorders and brain health. In this review, the classification and taxonomy, and the relation of these with safety aspects are introduced. Characteristics of L. plantarum to fulfil the criteria as a probiotic are discussed. Emphasis are also given to the beneficial functions of L. plantarum in gut disorders such as inflammatory bowel diseases, metabolic syndromes, dyslipidemia, hypercholesteromia, obesity, and diabetes, and brain health aspects involving psychological disorders.
Psychobiotics
According to the definition by WHO, mental health is an integral and essential component of health, a state of complete physical, mental and social well-being and not merely the absence of disease or infirmity. Furthermore, mental health is more than just the absence of mental disorders or disabilities (WHO, 2016). Major depressive disorder and anxiety disorders are debilitating illnesses that are rising as a global burden of disease (Whiteford et al., 2015; Logan et al., 2016). Dr. Dinan and colleagues defined a new group of bacteria, termed psychobiotics, as ‘live organisms that produce health benefits in patients suffering from psychiatric illness when ingested in adequate amounts’ and the ingestion of psychobiotics may induce psychotropic effects on behavior and additional neurochemicals in the brain (Dinan et al., 2013). This concept has shed light on microbe-based psychopharmacology. The human intestine has a large surface area, ranging from 30 to 400 cubic meters (Perez-Lopez et al., 2016), and is inhabited by 1013 to 1014 microorganisms. The number of microorganisms is 10 times greater than that of human cells, and the encapsulated genetic material exceeds the human genome content by 150-fold (de Vos and de Vos, 2012; Lozupone et al., 2012; Dinan et al., 2013). Because the large number of microorganisms live with human, it is logical to infer that associated microorganisms may play roles in human health and even in mental health. Considering that the gut-brain axis is a new concept and the applications of probiotics to enhance mental health is at its infancy, only few strains of L. plantarum have been investigated for this purpose. One of the more prominent strains of L. plantarum investigated as a psychobiotic is L. plantarum PS128 (Liu et al., 2016a, 2016b). The psychotropic effects of L. plantarum PS128 were investigated in an early life stress (ELS) mouse model. ELS negatively impacts brain development and results in behavioral changes in adulthood (Lupien et al., 2009). Maternal separation triggers ELS in rodents (O’Mahony et al., 2011). Mice that experience maternal separation exhibit lasting behavioral abnormalities, enhanced stress responses, increased anxiety-like and depression-like behaviors, elevated HPA reactivity, and altered neurochemical expression (Cryan and Holmes, 2005). Several behavior tests were employed to evaluate the effects of L. plantarum PS128 on abnormal behaviors, namely the sucrose preference test (SPT) and forced swimming test (FST). L. plantarum PS128 at a daily dose of 109 CFU/mouse reduced ELS-induced depression-like behaviors (Liu et al., 2016b). Maternal separation-triggered stress responses are evidenced by elevated levels of corticosterone before and after FST stress treatment. L. plantarum PS128 significantly reduced corticosterone levels at baseline and after FST, indicating that PS128 normalizes the HPA axis. Elevated serum levels of IL-6 are often observed in people experiencing childhood stress (Coelho et al., 2014). Modulation of IL-6 expression also potentiates the beneficial effects of L. plantarum PS128 on depression. Reduced levels of dopamine (DA) and serotonin (5-HT) and increased turnover rates of DA and 5-HT have been observed in the prefrontal cortex (PFC) of ELS mice. L. plantarum PS128 reversed these changes to a status similar to normal control mice, demonstrating the potential of PS128 as a psychobiotic to improve mental health. L. plantarum C29 was reported to protect memory deficit induced by scopolamine (Jung et al., 2012), D-galactose (Woo et al., 2014), aging (Jeong et al., 2015), and IBD (Lee et al., 2018). Increased expression of derived neurotrophic factor (BNDF) was observed in the above studies. BDNF protein is widely distributed throughout the adult brain in almost all cortical areas and was believed to be necessary for the continued survival and phenotypic maintenance of mature, fully developed neurons. In review of Zuccato and Cattaneo (2009), the levels of BDNF in brain were decreased in neurodegenerative diseases, Alzheimer disease, Parkinson disease, and Huntington disease (Zuccato and Cattaneo, 2009). The protective effects of L. plantarum C29 on memory deficit may attribute to the ability to elevate BDNF in brain
Does Lactobacillus PS128 work for “autism”?
People understandably assume a product should do what it says. Probiotics to treat GI problems from diarrhea to IBS to IBD are pretty well researched and though some are expensive (e.g. VSL#3, Vivomixx) they do work for many people.
Some people use Biogaia Gastrus as a Pyschobiotic with success and our reader Prada has joined that group. The only way to find out is to try it, but in the case of Biogaia Gastrus it actually makes some people much worse.
There actually is a published study investigating the effect of Lactobacillus plantarum PS128 on Children with Autism.
The study suggests that our reader in Italy and the people with the testimonials in US version of PS128 are not just exceptions.
Effects of Lactobacillus plantarum PS128 on Children with Autism Spectrum Disorder in Taiwan: A Randomized,Double-Blind, Placebo-Controlled Trial
This four-week, randomized, double-blind, placebo-controlled study investigated the effects of Lactobacillus plantarum PS128 (PS128) on boys with autism spectrum disorder (ASD) aged 7–15 in Taiwan. All subjects fulfilled the criteria for ASD diagnosis of DSM-V and the Autism Diagnostic Interview-Revised (ADI-R). Questionnaires used for the primary outcome measure include the Autism Behavior Checklist-Taiwan version (ABC-T), the Social Responsiveness Scale (SRS) and the Child Behavior Checklist (CBCL). The Swanson, Nolan, and Pelham-IV-Taiwan version (SNAP-IV) and the Clinical Global Impression-improvement (CGI-I) were used for the secondary outcome measure. The results showed that PS128 ameliorated opposition/defiance behaviors, and that the total score of SNAP-IV for younger children (aged 7−12) improved significantly compared with the placebo group. Additionally, several elements were also notably improved in the PS128 group after 28-day consumption of PS128. Further studies are needed to better clarify the effects of PS128 for younger children with ASD on broader symptoms.
I think the following study is relevant to our Italian reader, for whom NAC did not benefit stereotypy, but PS128 did.
I did mention to her the Tourette’s type autism, that was studied in Siena. In these people a dopamine disorder causes the repetitive behavior, so the behaviors are really better described as tics than stereotypy. Note that a serotonin agonist can cause a dopamine driven tic.
Inflammatory Response to GAS (Group A Strep) and Dysmaturational Syndrome (Tourette’s Syndrome with Autism “Recovery” by 6 Years Old)
Lactobacillus plantarum PS128 ameliorates2,5-Dimethoxy-4-iodoamphetamine-induced tic-like behaviors via its influenceson the microbiota–gut-brain-axis
Highlights
Serotonin receptor agonist DOI causes tic-like behaviors and gut dysbiosis in rat.
DOI triggers hyperactive signaling in mesocortical and nigrostriatal pathways.
PS128 alleviates DOI-induced behavior and hyperactive signaling.
PS128 modulates enteric serotonergic system and stabilizes gut microbiota.
PS128 strengthens the microbiota–gut–brain axis function of the host.
Abstract
We previously reported a novel psychobiotic strain of Lactobacillus plantarum PS128 (PS128) which could ameliorate anxiety-like& depression-like behaviors and modulate cerebral dopamine (DA) and serotonin (5-HT) in mice. Here, we examine the possibility of using PS128 administration to improve tic-like behaviors by using a 5-HT2A and 5-HT2C receptor agonist 2,5-Dimethoxy-4-iodoamphetamine (DOI). PS128 was orally administered to male Wistar rat for 2 weeks before two daily DOI injections. We recorded the behaviors immediately after the second DOI injection and compared the results with control and haloperidol treatment groups. PS128 significantly reduced tic-like behaviors and pre-pulse inhibition deficit in a threshold-dose of 109 CFU per day. Brain tissue analysis showed that DOI induced abnormal DA efflux in the striatum and prefrontal cortex, while PS128 ingestion improved DA metabolism and increased norepinephrine (NE) levels in these two regions. In addition, PS128 ingestion increased DA transporter and β-arrestin expressions and decreased DOI-induced phosphorylation of DA and cAMP regulated phosphoprotein of molecular weight 32 kDa (DARPP-32) at Thr34 and extracellular regulated protein kinases (ERK). PS128 ingestion also modulated peripheral 5-HT levels and shaped the cecal microbiota composition, which helps to alleviate DOI-induced dysbiosis. These results suggested that PS128 ameliorated DOI-induced tic-like hyper-active behaviors via stabilizing cerebral dopaminergic pathways through its modulation of host’s microbiota–gut–brain axis. Thus, we believe there are potentials for utilizing psychobiotics to improve syndromes caused by DA dysregulation in DA-related neurological disorders and movement disorders such as Tourette syndrome.
Lactobacillus PS128 clearly does benefit some people. It does have an effect on GI problems, but it may well benefit some people who have no GI problems. It is specifically targeted at the brain, not the gut.
If available locally it is worth a trial.
Is it going to make some people “worse”? It affects serotonin and dopamine and it is “anti-inflammatory” (raises IL-10 and lowers 1L-6), so some people undoubtedly will not be compatible.
It is not a cheap product, but is sold to be refrigerated and contains 30 billion colony forming units (CFU). It looks like a serious probiotic like VSL#3, Vivomixx and Biogaia.
People are making home-made yogurt with Biogaia Protectis and Biogaia Gastrus, so if Lactobacillus PS128 is effective but looks pricey, you can make your own. Lactobacillus bacteria grow well in milk
Some yoghurts have Lactobacillus rhamnosus added.
Making fermented milk products is actually very easy, this how you can grow your own Lactobacillus PS128.
I can envisage adding Lactobacillus PS128 fermented in milk to Monty’s breakfast yoghurt.
The other possible reason that Lactobacillus PS128 helped our Italian reader’s daughter is its effect on serotonin.
Some people find that SSRI drugs like Prozac reduce stereotypy along with anxiety. SSRI drugs can have side effects and may not be an ideal therapy for stereotypy.
Research in apes supports the fact that some people find inositol reduces stereotypy. Inositol is a naturally occurring sugar found in the brain that acts both as a messenger and a precursor to other neurotransmitters. The inositol trisphosphate receptor (IP3R) is a Ca2+ channel activated by inositol trisphosphate (IP3). IP3R appears to be a downstream nexus where many different types of autism converge.
Inositol is used to treat PCOS due to its metabolic effects.
Inositol appears to indirectly have an effect on serotonin, but it gets very complicated.
As you would expect, the serotine-type stereotypy is the result of one specific receptor. It appears to be 5-HT7 or 5-HT1A.
An Orally Active Phenylaminotetralin-Chemotype Serotonin 5-HT7 and 5-HT1A Receptor Partial Agonist That Corrects Motor Stereotypy in Mouse Models
Stereotypy (e.g., repetitive hand waving) is a key phenotype of autism spectrum disorder, Fragile X and Rett syndromes, and other neuropsychiatric disorders, and its severity correlates with cognitive and attention deficits. There are no effective treatments, however, for stereotypy. Perturbation of serotonin (5-HT) neurotransmission contributes to stereotypy, suggesting that distinct 5-HT receptors may be pharmacotherapeutic targets to treat stereotypy and related neuropsychiatric symptoms. For example, preclinical studies indicate that 5-HT7 receptor activation corrects deficits in mouse models of Fragile X and Rett syndromes, and clinical trials for autism are underway with buspirone, a 5-HT1A partial agonist with relevant affinity at 5-HT7 receptors. Herein, we report the synthesis, in vitro molecular pharmacology, behavioral pharmacology, and pharmacokinetic parameters in mice after subcutaneous and oral administration of (+)-5-(2′-fluorophenyl)-N,N-dimethyl-1,2,3,4-tetrahydronaphthalen-2-amine ((+)-5-FPT), a new, dual partial agonist targeting both 5-HT7 (Ki = 5.8 nM, EC50 = 34 nM) and 5-HT1A (Ki = 22 nM, EC50 = 40 nM) receptors. Three unique, heterogeneous mouse models were used to assess the efficacy of (+)-5-FPT to reduce stereotypy: idiopathic jumping in C58/J mice, repetitive body rotations in C57BL/6J mice treated with the NMDA antagonist, MK-801, and repetitive head twitching in C57BL/6J mice treated with the 5-HT2 agonist, DOI. Systemic (+)-5-FPT potently and efficaciously reduced or eliminated stereotypy in each of the mouse models without altering locomotor behavior on its own, and additional tests showed that (+)-5-FPT, at the highest behaviorally active dose tested, enhanced social interaction and did not cause behaviors indicative of serotonin syndrome. These data suggest that (+)-5-FPT is a promising medication for treating stereotypy in psychiatric disorders
Efficacy of Low-Dose Buspirone for Restricted and Repetitive Behavior in Young Children with Autism Spectrum Disorder: A Randomized Trial
Children 2-6 years of age with ASD (N = 166) were randomized to receive placebo or 2.5 or 5.0 mg of buspirone twice daily. The primary objective was to evaluate the effects of 24 weeks of buspirone on the Autism Diagnostic Observation Schedule (ADOS) Composite Total Score. Secondary objectives included evaluating the effects of buspirone on social competence, repetitive behaviors, language, sensory dysfunction, and anxiety and to assess side effects. Positron emission tomography measures of tryptophan metabolism and blood serotonin concentrations were assessed as predictors of buspirone efficacy.
Results
There was no difference in the ADOS Composite Total Score between baseline and 24 weeks among the 3 treatment groups (P = .400); however, the ADOS Restricted and Repetitive Behavior score showed a time-by-treatment effect (P = .006); the 2.5-mg buspirone group showed significant improvement (P = .003), whereas placebo and 5.0-mg buspirone groups showed no change. Children in the 2.5-mg buspirone group were more likely to improve if they had fewer foci of increased brain tryptophan metabolism on positron emission tomography (P = .018) or if they showed normal levels of blood serotonin (P = .044). Adverse events did not differ significantly among treatment groups.
Conclusions
Treatment with 2.5 mg of buspirone in young children with ASD might be a useful adjunct therapy to target restrictive and repetitive behaviors in conjunction with behavioral interventions.
Stereotypies in Captive Primates and the Use of Inositol: Lessons from Obsessive–Compulsive Disorder in Humans
Animal stereotypies have long been used in the study of obsessive–compulsive disorder (OCD) in humans. These studies have led to the understanding of some of the molecular pathways in the disorder and the use of selective serotonin reuptake inhibitors and myo-inositol in the treatment of these conditions. If animal models, especially nonhuman primate models, were used to study human disorders and if the resulting treatments were successful, then conversely one should be able to treat nonhuman primate stereotypies with similar methods. We here summarize animal models of OCD (including nonhuman primate models) and human OCD treatments, and using successful human treatment by myo-inositol as models, recommend the use of myo-inositol in good captive management practice and the treatment of nonhuman primate stereotypies. We believe that this would be particularly useful in the treatment of stereotypies in nonhuman primates because they are physiologically so similar to humans.
Inositol holds much promise in the treatment and prevention of stereotypic behavior, and although much research is required to understand the molecular mechanisms behind its mode of action and the reason for failure in 30 % of human cases, its use does mean the possibility of treatment and prevention in 60–70 % of cases that would otherwise be untreatable.
Back to SIBO
Many people think their child with autism has SIBO (Small intestinal bacterial overgrowth). Most likely some do and some do not.
To diagnose SIBO you need a breath test
Here is what Johns Hopkins have to say about SIBO: -
Our gastroenterologists (doctors who specialize in the digestive system) diagnose SIBO with a lactulose breath test. For the test, you will swallow a drink containing the sugar lactulose. Next, you will breathe into a balloon approximately every 15 minutes over the course of three hours. Each time, we remove the breath sample from the balloon and test it. SIBO may be present if your breath sample contains hydrogen or methane shortly after drinking the solution.
Treatment
· hydrogen-predominant SIBO: The primary treatment is the antibiotic rifaximin.
· methane-predominant SIBO This type of SIBO is harder to treat, and it may take longer to respond to treatment. We use rifaximin plus neomycin for these cases.
· recurrent SIBO: We closely monitor you for a recurrence of SIBO. If it happens, you will benefit from our experience treating the disease. We have experience with formulations of antimicrobial herbs, which can be used to treat recurrences and as an alternative for initial treatment of hydrogen- or methane-predominant SIBO.
As part of your treatment, we recommend following a FODMAP (low fermentable oligosaccharides, disaccharides, monosaccharides and polyols) diet and consulting with a nutritionist.
As part of your treatment, we recommend following a FODMAP (low fermentable oligosaccharides, disaccharides, monosaccharides and polyols) diet and consulting with a nutritionist.
The symptoms of SIBO are not unique to SIBO
SIBO is an abnormal number of bacteria in the small intestine that can lead to:
· bloating and increased passing of gas (flatulence)
· diarrhea or constipation
· abdominal pain
· nausea
· fatigue
What are SIBO risk factors?
Structural or anatomic abnormalities may affect normal movement of the small intestine (motility). Stasis, or lack of movement, can lead to bacterial imbalance. This can occur if you:
· Had surgery that changed the small intestine’s structure, such as Roux-en-Y gastric bypass surgery, or surgery on the right colon with removal of the ileocecal valve, or surgery on the last part of the small bowel.
· Have adhesions (scar tissue) that developed after radiation therapy or after multiple abdominal surgeries
· Have amyloidosis (a buildup of amyloid protein deposits) — deposits can accumulate in the small intestine and change its structure
Use of certain medications could be linked to SIBO. These include:
· Narcotic medications
· Anti-spasm medications for irritable bowel syndrome (IBS), such as hyoscyamine or dicyclomine
· Long-term use of proton pump inhibitors (PPIs) — medications that decrease acid in the stomach to control heartburn
· Frequent use of antibiotics, which may alter the bacteria in the small bowel
Chronic systemic conditions can cause motility issues. If you have these conditions, you may be at a higher risk for SIBO:
What is the problem with rifaximin?
Rifaximin is a generic antibiotic used to treat traveler’s diarrhea, irritable bowel syndrome and SIBO.
In much of the world Rifaximin is very cheap, it costs a few dollars/euros where I live, but in the US it costs thousands of dollars a year.
So, the land of the free is where big pharma is free to make obscene profit margins, as they do even with life-saving drugs like insulin. In developed countries Type-1 diabetic people get their insulin free and there is universal healthcare.
There are many other drug options other than Rifaximin and in the study below they found some herbal treatments as effective as Rifaximin.
Herbal Therapy Is Equivalent to Rifaximin for the Treatment of Small Intestinal Bacterial Overgrowth
Objective:
Patients with small intestine bacterial overgrowth (SIBO) have chronic intestinal and extraintestinal symptomatology which adversely affects their quality of life. Present treatment of SIBO is limited to oral antibiotics with variable success. A growing number of patients are interested in using complementary and alternative therapies for their gastrointestinal health. The objective was to determine the remission rate of SIBO using either the antibiotic rifaximin or herbals in a tertiary care referral gastroenterology practice.
Design:
One hundred and four patients who tested positive for newly diagnosed SIBO by lactulose breath testing (LBT) were offered either rifaximin 1200 mg daily vs herbal therapy for 4 weeks with repeat LBT post-treatment.
Results:
Three hundred ninety-six patients underwent LBT for suspected SIBO, of which 251 (63.4%) were positive 165 underwent treatment and 104 had a follow-up LBT. Of the 37 patients who received herbal therapy, 17 (46%) had a negative follow-up LBT compared to 23/67 (34%) of rifaximin users (P=.24). The odds ratio of having a negative LBT after taking herbal therapy as compared to rifaximin was 1.85 (CI=0.77-4.41, P=.17) once adjusted for age, gender, SIBO risk factors and IBS status. Fourteen of the 44 (31.8%) rifaximin non-responders were offered herbal rescue therapy, with 8 of the 14 (57.1%) having a negative LBT after completing the rescue herbal therapy, while 10 non-responders were offered triple antibiotics with 6 responding (60%, P=.89). Adverse effects were reported among the rifaximin treated arm including 1 case of anaphylaxis, 2 cases of hives, 2 cases of diarrhea and 1 case of Clostridium difficile. Only one case of diarrhea was reported in the herbal therapy arm, which did not reach statistical significance (P=.22).
Conclusion:
SIBO is widely prevalent in a tertiary referral gastroenterology practice. Herbal therapies are at least as effective as rifaximin for resolution of SIBO by LBT. Herbals also appear to be as effective as triple antibiotic therapy for SIBO rescue therapy for rifaximin non-responders. Further, prospective studies are needed to validate these findings and explore additional alternative therapies in patients with refractory SIBO
Table 1
Conditions That Predispose Toward the Development of Small Intestine Bacterial Overgrowth
Achlorhydria (surgical, iatrogenic, autoimmune)
Motor abnormalities
Scleroderma
Intestinal pseudo-obstruction
Diabetic enteropathy
Vagotomy
Abnormal communication between colon and small bowel
Fistulas between colon and small bowel
Resection of ileocecal valve
Structural abnormalities
Systemic and intestinal immune deficiency states
Surgical loops (Billroth II, entero-entero anastomosis, Rou-en-Y)
Duodenal or jejunal diverticula
Partial obstruction of small bowel (stricture, adhesions, tumors)
Large small Intestine diverticulosis
Systemic diseases (celiac disease, cirrhosis, pancreatic exocrine insufficiency, non-alcoholic fatty liver disease)
Alcoholism
Table 2
Protective Factors That Protect Against the Development of Small Intestine Bacterial Overgrowth
• Gastric acid
• Pancreatic enzymes
• Bile acids
• Cholecystectomy
• Motility
• Migrating motor complex
• Biofilm
• Secretory immunoglobulin A
Table 3
Extrinsic Factors That Alter the Gut Microbiome and May Influence the Development of Small Intestine Bacterial Overgrowth
FODMAPsa (fructose, lactose, galactans, fructans, sugar alcohols)
Proton pump inhibitors
Anti-motility agents
Fiber
Prebiotics
Probiotics
Antibiotics
Table 4
Antibiotic Regimens Used for Small Intestine Bacterial Overgrowth
Agent Dose Frequency
Amoxicillin-clavulanate 500 mg 3 times/day
Cephalexin 250 mg 4 times/day
Chloramphenicol 250 mg 4 times/day
Ciprofloxacin 500 mg twice daily
Doxycycline 100 mg twice daily
Metronidazole 250 mg 3 times/day
Neomycin 500 mg twice daily
Norfloxacin 400 mg twice daily
Rifaximin 400 mg 3 times/day
Tetracycline 250 mg 4 times/day
Trimethoprim- 1 double- twice daily
Sulfamethoxazole strength tablet
Conclusion
I think PS-128 is very likely to be a winner for many people diagnosed with Tourette’s syndrome.
Repetitive behaviors in autism that are caused by a dopamine anomaly may well respond to PS-128. Note that a serotonin anomaly can cause a dopamine anomaly.
Undoubtedly, some people with autism are going to develop a motor/verbal tic when they take PS-128. They should stop taking it and the tic should fade away, just like the negative reaction to Biogaia Gastrus fades away in those so affected.
Anxiety is a common feature in autism, but has numerous underlying mechanisms, so I think PS-128 will help some and not others. It is certainly worth trying.
Tics and stereotypy get confused and the causes may indeed overlap. Dopamine anomalies can lead to tics and movement disorders. Serotonin anomalies can lead to repetitive behaviors and of course anxiety. Oxidative stress can lead to stereotypy and even compulsive behavior like Trichotillomania (pulling out your own hair).
Autoimmune encephalopathy can give symptoms of tics, OCD and/or stereotypy, and even schizophrenia depending on which receptors in the brain are affected - PANS/PANDAS is a subtype of autoimmune encephalopathy.
· Low dose Buspirone. It is not an SSRI, but this anxiety medicine at very low doses (2.5 to 5 mg) looks interesting for serotonin-type stereotypy
· Inositol (it’s cheap and OTC)
· Prednisone for Autoimmune encephalopathy
You might think the supplement 5HTP would help with the serotin type of stereotypy; 5HTP is a precursor of serotonin that is sold widely for anxiety etc. Long term use may cause you problems.
5-HTP efficacy and contraindications
The most significant side effects and adverse reactions may occur with long-term use (many months or longer). Administration of 5-HTP alone depletes catecholamines (dopamine, norepinephrine, and epinephrine). When dopamine depletion is great enough, 5-HTP will no longer function. If other centrally acting monoamine-related disease processes involving catecholamines are present, administration of 5-HTP alone may deplete dopamine, norepinephrine and epinephrine thereby exacerbating these conditions
Some doctors and indeed autism self-advocates think that stereotypy is a healthy calming behavior. These autism self-advocates tend to be the ones that had a terrible time during their school years, because they were not accepted and now feel that qualifies them to give advice to others. I not so sure they are right, I would rather take autism advice from happy/successful Aspies, rather than bitter ones.
I think that uncontrollable stereotypy gets in the way of normal life and learning in particular; if its origin is biological, it can be treated. Since there are multiple possible mechanisms at work, it can take time to find your effective therapy. As usual, perseverance yields results in most cases.
Back to the SIBO part of this post
I think most people with intestinal dysbiosis do not have SIBO. If you live in the US, it looks quite easy to get a breath test for SIBO.
Rifaximin seems to benefit many people with autism and GI problems; they may well not have SIBO. For people outside the US, Rifaximin looks a good choice, for recurring use. Our reader Maja is a big fan of Rifaximin for her daughter.
If you have to pay thousands of dollars a year for Rifaximin, you may want to look at both the drug and herbal alternatives.
For SIBO caused by long term use of PPIs (acid reducing drugs) you can try alternate day dosing, or the old remedy of drinking diluted apple cider vinegar. Both methods should increase acidity in the small intestine making it hostile to unwanted bacteria, the way nature intended. If you drink apple cider vinegar you have to rinse your mouth out afterwards or you will damage your teeth.
Probiotics have been in widespread use to treat GI problems in some countries for half a century. That is plenty time to judge their effectiveness, if people care to look.
Probiotics have been shown to have far reaching effects beyond the gut and this causes many people to have serious doubts. How can your gut affect your brain, your eczema or your asthma?
When it comes to the brain, the research has proved that there is bidirectional communication between the brain and the gut via the vagus nerve. Sever the vagus nerve (which used to be a medical procedure for IBS) and the effect is lost.
Many probiotics sold lack potency either because they were not stored correctly, and the bacteria died or because the producer has included too few bacteria to start with.
The users of Biogaia Gastrus for autism are taking 5 tablets a day, because one tablet contains only 100 million CFU.
I'd suggest if this is going to be effective, it may be best delivered rectally via enema, or as part of milk kefir grains administered via rectal syringe (probably best under medical advice/supervision). Some people are treating Chrohn's with this method. I personally have experienced sensitivity to Lactobacillus orally, and there is a view that oral probiotics could worsen sibo and small intestinal permeability may form part of this. I think this with low-dose Naltrexone (for motility issues relating to SIBO and immunomodulation) and Helminths could potentially be a useful anti-inflammatory treatment for many if the issue stems from the gut, as I believe is my case. Rifaximin is best sourced generically via canadian online pharmacies (CIPA registered), making it significantly cheaper.
ReplyDeleteYou deliver relevant findings again and again Peter. I liked the part on serotonin-dopamine connection.
ReplyDeleteWondering, that 5-HT2A and 5-HT2C receptor agonist DOI induced tics, but in another paper stereotypy was rescued by a 5-HT7 + 5-HT1 agonist. What does this tell us?
/Ling
Hi Peter,
ReplyDeleteI saw that you are referencing an article above from Dr. Hinz "5-HTP efficacy and contraindications". I read some of his work before and have always been skeptical given the mercantile aspect linked to his research. Here is a link I found this morning about it:
https://quackwatch.org/11ind/hinz/
I have been taking 5-HTP supplements for over 10 years to deal with a variety of problems and it has been a life changing supplement in my case. I started experimenting with it after trying SSRIs for about a year and switching to 5-HTP was like day and night.
Chris
Chris, what is your view on why 5-HTP works for you while SSRI:s don't?
Delete/Ling
Chris, that is very interesting, 10 years is a long time.
DeleteI imagine some people are less lucky and may get a negative reaction, after a while.
In the post below I did mention 5-HTP is suggested by Dr Ramaekers as a therapy.
Secondary Monoamine Neurotransmitter Disorders in Autism – Treatment with 5-HTP and levodopa/carbidopa?
https://epiphanyasd.blogspot.com/2017/02/secondary-monoamine-neurotransmitter.html
Peter, Ling, I don’t have a clear answer myself, the link about Dr. Ramaekers’ work is a clear possibility, i.e. genetic mutation leading to serotonin system dysfunction/lack of production. If there is a deficit of cells producing serotonin or malformed cells, SSRI can only help so much. I have Asperger, my daughter is pretty much like me at her age (much better actually because of this blog). My sister has her own similar issues, her son is much worse with PDD-NOS and her daughter is better with some attention deficit issues.
DeleteSSRIs helped some but had little effect on several of the problems I had at the time (2007), a result from chronic work related stress. I also was not a fan of how they made me feel. I wasn’t depressed but in retrospect, I had serious serotonin deficiencies given the symptoms I had and how 5-HTP dramatically reduced or eliminated most of them. As far as the effect of 5-htp on the brain vs the rest of the body, I can’t really distinguish, 5-htp modulates symptoms pretty much at the same pace for both.
When I switched to 5-HTP, I started with 25mg and the effect was tremendous compared to SSRIs in helping me having a good night sleep, solving my dysphagia/reflux/digestive system issues, neuropathic pains, etc. 25mg is not much and shows how low I must have been. The dosage increased over 13 years but seemed to have somewhat plateaued in the last 4 years around 200mg a day. I also take 440mg L-Tryptophan daily and other supplements from this blog (ketotifen, PEA, choline, B6, B12, etc).
I tried reducing 5-HTP a few times but after a few days most of the symptoms start to come back. They are mostly gone or greatly attenuated with 5-HTP (and completely eliminated with the addition of the other supplements). As I mentioned in another post, taking too much magnesium seems to counteract the effect of 5-HTP for me and makes my daughter very anxious.
My low serotonin problems, I had some for most of my life:
Panic disorder
Generalized anxiety disorder
GERD leading to throat inflammation -> nerve irritation and shoulder bursitis
Easily geting nerve injuries from repetitive movements/positions
Dysphagia
Diarrhea
Digestive difficulties
Random nerve pains
Frequent Heart PVC
Tinnitus
Feeling of shortness of breath
Derealization/Depersonalization
Sleeping difficulties
Ruminating thoughts
Waking in the night with a feeling of rage, without cause
Increased rhinitis/food intolerance symptoms
Chris
Thanks for the great response Chris! I'll be looking into these things very soon, and your full description with symtoms and all will be very useful to have. :-)
DeleteDoes tryptophan help you too? (Obviously if you yse it...)
Peter has a very old post on serotonin/tryptophan with an article on that subject in autism. It contains a description with all the genes involved in the different conversion steps. Maybe it can be of help to understand where your best interventions are acting.
/Ling
Tryptophan has been a gray area for me. I don't remember it making a big difference but I still thought taking it might help in the long run. At the time, I read it was a neurotransmitter in it's own right. Taking more made me feel a bit queasy.
DeleteI think it's pretty well known that tryptophan metabolism is off in autism. It really sounds that in your case it is not converted to 5-HT by TPH1 and TPH2 (the latter in the brain) as well as it should. Maybe it is converted to something else (kynurenine pathway?), which is why you find higher doses negative.
DeleteWorth reading up on.
/Ling
Hi Peter, I am currently taking doxycycline monohydrate 100mg twice a day, when/how is the best time to take probiotics while on antibiotics? Also, is there a way to benefit from probiotics at the same time as daily doxycycline?
ReplyDeleteMartin, some probiotics tell you on the information leaflet which antibiotics will kill them and which are compatible.
DeleteSome probiotics are sold specifically to be taken while using antibiotics. This is to counter any damage done by the antibiotic.
Lactobacillus rhamnosus and Saccharomyces boulardii are recommended in a Cochrane review for Antibiotic-associated diarrhea. These probiotics are taken together with the antibiotic.
Thanks Peter. So far I've been doing floranex twice a day prescribed from my colitis stay; and then I'm doing Kefir and Bragg's ACV twice a day. I've been on prescribed pantoprazole PPI for at least six months and either cimetidine.or famatodine since ranitidine is recalled/withdrawn here in us.
ReplyDeleteI also have been on buspirone 5mg three times daily for about 2 years. I had read about it being a prokinetic before and helping shakes in Raynaud's but I initially only tried it when I was determined to avoid taking ssris.
I've always wanted to try the pro biotic strain that you've mentioned on your other probiotic posts that produces oxytocin in the gut.
I forgot to say I've looked at systematic sclerosis papers before looking at buspirone having a positive effect on esophageal sphincters
ReplyDelete15 days into sulforaphane (Prostaphane) we are shocked. I have a diary where I input daily events and I have to type 10 minutes each day now. Huge steps forward, cognitively and behaviourally.
ReplyDeleteGreat news!
DeleteCongeatulations tpes! It's great when you nail it. :-)
Delete/Ling
Hi there May I ask if you could tell me the taste of the powder inside Prostaphane capsule?
DeleteMy 26-mo hates the typical supplement for its smell and flavor. Wonder if I can try Prostaphane.
I have a really strange request - I was considering adding to our therapy, either verapamil or atorvastatin. Then, on an old blog post here, I read in the comment section that one of those has an interaction with something we take but Peters son does not - either azithromycin or propranolol most likely. I am now really leaning towards atorvastatin and I can’t find the comment to recheck what it said. I think the interaction was explained and its not one of the official listed ones. If anyone remembers this or wrote it in tje first place, let me know.
ReplyDeleteI think it might be combining the statin with azithromycin
Deletehttps://www.ncbi.nlm.nih.gov/pmc/articles/PMC2766483/
Verapamil with Propranolol is also not usually advised, but in reality needs monitoring, because people do safely take both.
spent the last two hours trawling here and elsewhere, I think it was verapamil and diflucan. which I didnt mention but she also takes. its really hard to remove therapies which have several modalities (like azithro and difl) they can help through, because its hard to estimate how the child reacts when you take them away.
ReplyDeleteIs there any way to get Prostaphane in the US or Vancouver BC / Canada? If not is there a capsule / pill version of Sulforaphane that any of the parents here would recommend?
ReplyDeleteI believe Avmacol is on Amazon.com which is one of the two versions of active Sulforaphane available in the world.
DeleteHello Peter, my son's GI problems have improved with verapamil, it's been days he doesn't wake up at night with a stomach ache, he is still on bumetanide and he has improved in other aspects, which maybe only I notice. Before treatment his feet were really red at night before going to sleep because of his hyperactivity and stimming, I couldn't even touch them or cut his nails, I can see his cognition has improved and his speech has progressed, he tries to tell me more things even though I see it's really hard for him to form a sentence, he mostly has echolalic language and refers to himself in third person. He knows how to count, the colors and shapes, he even knows dinosaur names but he can't have a conversation, he also can ride his bike like a pro, but he has difficulty with his fine motor skills. He still stims a lot, he frecuently flaps his hands and walks on tiptoes, and is hyperactive but he has been a bit calmer since treatment. I didn't know that it's prohibited to import supplements from USA, and the NAC that I ordered is taking ages to arrive. Now that we've been in quarantine there have been very difficult days mostly due to temper tantrums and OCD like behaviour, he also has been vocal stimming a lot, schools here where I live will remain closed until next year and he was about to receive language therapy when the quarantine started so I have to see what I can do for him here at home. I have been reading your blog every day and some medications such as Atorvastatin and Diamox I can find locally, I hope I can buy Bumetanide from an online pharmacy from Canada because I can't find Miccil here in Mexico so I don't have to stop his treatment. My concern is also about dosage, my son is almost 4 but he is tall and weighs about 24 kilos, he is taking 1mg of bumetanide and 20 mgs of verapamil, I've been very careful to start with a minimal dose and raise it slowly, always observing his reaction to it, in a post I read you said it's better to take the minimal dose, but I think sometimes that I'm giving him much less, can you suggest me what dose is better?, and should I wait for NAC to arrive and let him get used to verapamil or should I try with one of the medications available locally?
ReplyDeleteThank you for all your help.
I started on verapamil myself and at first got a weird sensation in my forehead, it's been several days now and my sinusitis is much better, I really didn't expect that.
By the way if you ever want to move your blog to a wordpress installation I can do it for you free of charge, I design wordpress websites.
Lisa, a recent clinical trial confirmed that Verapamil does indeed help sinusitis.
DeletePatients with severe chronic rhinosinusitis show improvement with Verapamil treatment
https://www.sciencedaily.com/releases/2017/01/170123093954.htm
One reader in Brazil, where Bumetanide tablets are also not sold, reported that he could get the compounding pharmacy, probably at a large hospital, to make him the tablets. The pharmacy has the base chemical and they just make customized doses. Maybe this is possible in Mexico.
Another reader found that in Spain they cannot currently buy bumetanide. Perhaps the reason is the supply chain back to China/India?
I would always use smaller doses, if they are effective. This reduces the chances of any negative effects, which can occur with any drug.
Atorvastatin and Diamox may indeed be helpful. In my son Diamox caused reflux/GERD, so was not suitable, but other people have no side effects. Hundreds of millions of people take Atorvastatin, but not many 4 year olds, so this is experimental use.
Atorvastatin show its effect very quickly, so you just need a few days to be sure if your son is a responder.
Diamox has multiple possible beneficial effects and so I think a longer trial, like 2 weeks would be needed. Note that Diamox lowers both sodium and potassium, whereas bumetanide generally only causes a problem with low potassium. You have to be careful.
Thank you Peter for your response and your advice, I will be careful, your blog has been changing our lives, today I asked my son a question and for the first time he responded and didn't repeat what I said. I was thinking about inositol, I read about it a few years ago, when I was mostly reading Amazon reviews instead of more complicated research, there was a review from a woman that started taking inositol for her OCD and at first she thought she'd found the cure, but later she updated her review very disappointed 9 months later, saying that all her symptoms came back, why would a vitamin stop working? It reminded me about a scene from the movie Awakenings when Robert De Niro's character relapsed and needed more medicine, but they couldn't give him more because he needed more and more till there was no effect. I always thought that medicine was supposed to cure even with some side effects, but to what could be happening in the body of someone that needs more and more medicine, could it be making more harm than good? I am familiar with drug addiction and alcoholism, so it seems to me like a similar effect, and I try to avoid that, it seems scary. But after reading your blog I think that there many things involved such as allergy. I want to try inositol for my son, I guess it will be in about 2 months until it arrives. I did get clonazepam and it seemed easier and cheaper to obtain than the supplements but I still want to read more about it before trialing, for the moment I'll wait several days before I try anything. I reread some posts because every time I read them again I understand more. Have a nice day Peter.
DeleteHi Peter,
ReplyDeleteMy 3.5-yo son with ASD, now turned verbal but still with other ASD traits, has developed facial tic for a week or 2. It didn't start abruptly into the a high level of severity, but it seems to be on a worsening trend over last week. It was first noticed by his ABA therapist today, which she described, if my son had dry eyes, thus his facial grimacing during the class. I then noticed his facial grimacing as he sat through his 15-min episode of Peppa Pig. He has no other infectious symptoms. He is fully recovered from COVID-19 early March. He took ibuprofen only to contain the fever. Lastly, he has been taking PS128 for almost 1 year, on a daily basis.
Now I am not seeing behavioral changes per se (knock knock), and wonder what can I do to help him. He did tell me with his limited language that he felt pains below his left and right eye, as I asked him if he feels unwell on his face. What may I do / read / check to see if this is part of a bigger problem? Is tic related to oxidative stress actually? Thanks Peter.
MG, tics can have multiple causes. One common cause relates to dopamine, this is thought of as what drives Tourette Syndrome. Some drugs and supplements affect either dopamine or its receptors, and can causes tics. You might want to check whether PS128 has caused the tics. Take a break for a week or two.
DeletePeople with Tourette’s do report that they get pain from their tics. Your son’s eye pain may be a result of the tics.
It would be a good idea to go to your doctor and see if there is an identifiable medical reason for the eye pain; it is also possible that whatever is causing the pain might also cause the tics.
Stress can also cause the onset of tics.
Hi Peter
DeleteThe tic has subsided in recent weeks. It seems to be related to PS128, as I have stopped it for a month. Would see how it goes.
Hi Peter,
ReplyDeleteMy daughter seemingly responded very well for PS128, her spontaneous cryings (sometimes followed by laughther and cry again, which looks very strange) did go away with 1 sachet a day (30B CFU of PS128). Recently, PS128 has been out of stock (very few sellers of it) and i had to cut to half sachet and i see those cryings are back. Does this mean her underlying issue was with serotonin/dopamine regulation perhaps? just thinking what to do if PS128 is not back in stock, any alternatives might help? Thanks in advance for your advice, Peter.
regards
Timur
Timur, this type of bacteria will grow in milk and so you can make your own yogurt or kefir. There are tutorials on Youtube showing how to do this. It is not hard and then you will have a constant supply of PS128. People also do this with the Biogaia probiotics.
ReplyDeleteThanks Peter, interesting, thanks for sharing, didnt know that homemade homemade version would be possible. make sense and perhaps it would be mixed strains of L Plantarum as a result.
DeleteTricky part is, she has diary intolerance (and gut dysbiosis with some yeast overgrowth and we follow gluten-diary-free regime), so fermenting milk won't be an options for us. i am trialing herbs (Lomatium, Pau Darco, Olive leaf) along with diet to get yeast under control.
I also give her 10B CFU of L Plantarum 299V. Maybe i should double up on that dose. I also ordered Garden of Life's Mood priobiotic which has anxiety reducing L Plantarum, helveticus, casei etc. will see how that goes.
it is amazing, how response varies with specific type of a strain - good response to PS128 perhaps means her need to serotonin/dopamine balancing. Her earlier good response Picamilon and L-theanine, also implies EI imbalance which if i am not wrong links to serotonin as well.
regards,
Timur
Timur, it seems that people are now making non-dairy yoghurt at home using Almond Milk, look on Youtube. There are also commercial products, so it must work.
DeleteI would just keep on using PS128, rather than finding alternatives.
When it is in stock, fill your fridge.
I just bought a 1 year supply of Ponstan, while we were in Greece at Easter. It cost me 20 EUR/USD.
Well of course Peter would have a posting on PS128 :) I just started for my son - 5 days in. The first few days I gave it in the morning and on those days, he napped. Which is not something he does. I’ve now switched to evening dosing - no naps. Haven’t noticed anything so far other than that. Anyone else using? Any updates from those who have?
ReplyDelete~Tanya
Tanya, how did it go with PS128? I have a 5 year old who is very sensitive to anything and social anxiety is a big challenge for him (per other posts from you I think your kid is similar). I purchased PS128 recently and waiting to get it delivered.
DeleteHi Tanya, my 7 years old taking PS128 with night snack (i just pepper it over cereral before adding almond milk and mix so is not visible, doves farm chocostar cereal is good one). whether it helps, i think it does mainly for sleep and anxiety.
DeleteAlejandra- sorry I am just now seeing your question: well, my son started having tic-like behavior with his lips - he would pucker them off and on all day. Also started humming a lot - which is very unnerving. I stopped and started the ps128 twice and with each time it happened. So I don’t think it’s for him. On the other hand, it’s been great for my sudden mid-life anxiety.
DeleteAnonymous- yes I was really hoping it would help with some situational anxiety he still has (he’s 23 now!). No such luck for us
DeleteHello, for 2 months my 3-year-old son has been consuming PS128, I did not see any significant change, it seems that my son's issue is not on the gastrointestinal side. After reading this article I will try inositol to calm the stereotype (move your right hand in front of his face); I have reached the maximum dose with the NAC 900mg / day for his age.
ReplyDeleteFor 2 days I raised it to 1200 and I saw a reduction in the frequency, so it seems that his oxidative stress contributes to his stereotyping, but I would not want to increase his NAC any more. I have searched the blog for suggested doses of inositol but have not found any suggestions?
Greetings
Hello, is there anyone who has tried valtrex with success, did you have any side reactions, I would like to try it for Denis, I understood that it affects the kidneys, and Denis has a bit of kidney fatigue, I am waiting for an answer. Peter, what do you think, do you think that it's worth trying, considering that after the MMR (MMR) vaccine, Denis suddenly regressed with bouts of crying and howling. 2 months before the vaccine, he had chicken pox
ReplyDeleteDragos, do have access to rapamycin? If you think it's a post viral infections it could possibly help.
Deletehttps://www.sciencedirect.com/science/article/abs/pii/S0166354215002181
Hi Stefan, I see that here in Romania, you can find sirolimus rapamune, it is quite expensive, but in the end I will try to buy a box. Do you think it would synergize with valaciclovir. Denis had some improvement from all antimalarial and antiparasitic drugs. I am convinced that there is no autism in my son, it is a viral autoimmune encephalitis triggered by the MMR vaccine. I have tried almost all the neuropsychiatric drugs, none of them did anything, except for a momentary improvement. I hope that someone from the doctors to hear me and help us once and tell us exactly what kind of virus we are dealing with. This virus that inflames the immune and digestive system and messes up the brain.
DeleteAgreed, Rapamycin is very expensive. But it will calm the immune system down. I have have two sons, one with Profound asd and the other with receptive and speech delay. I learned from my mistakes with my first son that has profound asd. My second son had no screen time, no vaccines, no antibiotics, and no viruses since we were in quarantine from covid. But he still ha d learning issues. I tested him for Folate antibodies and he was positive for both. Leucovorin does work, I use it for both my sons and we avoid dairy. However, the only thing that really helps my son with Profound asd is rapamycin.
DeleteHello Stephen,
DeleteThats interesting that rapamycin works, I always had a theory for it on asd but not for anti-viral purpose. What dose do you use for you son?
I started my trial with 1mg a day. It worked. He started saying words I never heard him say and his cognition increased. Downside, he caught every cold in his ABA center. I was trying to stop his folate receptor autoantibodies. I then switched to 0.5mg every day. Same results, same colds. Since then I have learned he has a type 1 inferonopathy which makes him sick all the time. However, xolair has stopped most of his illness. But he won't qualify for ivig since all his igg levels are normal. I'm about to start a jak inhibitor his immunogist has suggested and see if that helps. Most subtypes of ASD are the results of a dysfunction immune system so rapamycin should work.
Delete-Stephen
Rapamycin also helps shut off mTOR in the brain, which induces autophagy which could also reduce synaptic connections in the brain. One of the things research has found about post mortem ASD brains is that they have more synaptic connections than a normal brain (they have less pruning during childhood years). If you find long term that your son keeps progressively getting better under rapamycin this could also be the reason. Unfortunately rapamycin is not tried a lot and not under many trials as its only seen as a organ transplant medication when it could have so many other uses.
DeleteHello, better try disulfiram, it has the same properties as rapamycin with fewer adverse reactions, I mean on the immunity side, it stops inflammation and anxiety
DeleteDragos, what dose are you using now?
Delete-Stephen
Since June, 2023 I also did a trial of Dupixent (il4 and il13 blockers) vs Xolair (anti-ige). Dupixent is a great anti-anxiety monoclonal however it comes with the removal of fear and sleep jagging. So I'm just sticking with Xolair for his asthma.
ReplyDelete-Stephen
Stephen dove compri la rapamicina?
ReplyDeleteHi Diego, my family friends are doctors so they just write my scripts. But I bet you can buy it from India if you want to try.
DeleteDiego, I know it's not the same but you can also try high dose biotin.
Delete"In conclusion, autophagy inhibition by biotin uncouples protein synthesis to promote lipogenesis by eliciting endoplasmic reticulum stress and differential phosphorylation of mechanistic targets of rapamycin complex 1 substrates."
https://www.sciencedirect.com/science/article/pii/S1355814523017261
High-dose biotin normalized the hyperactivation of mTORC1, thus restoring lipid homeostasis.
https://pubmed.ncbi.nlm.nih.gov/32511826/
-Stephen
In addition, MgB treatment significantly regulated the neurotoxicity-related cytokines and neurotransmission-related markers. For instance, MgB significantly decreased the expression level of TNF-α, IL-6, IL-17, CCL-3, CCL-5, and CXCL-16 in the brain, compared to the control group (p < 0.05). These data demonstrate that MgB may ameliorate dysfunctions in social behavior, learning and memory and reduce the oxidative stress and inflammation indexes of the brain in a rat model.
Deletehttps://www.ncbi.nlm.nih.gov/pmc/articles/PMC8955994/#:~:text=The%20present%20study%20showed%20that,based%20on%20exposure%20to%20PPA.
You can buy it off of amazon. No clue if it would work...
InstaRelief® Hair Growth with Lustriva® - Clinically Shown to Grow Thicker, Healthier Hair in 3 Weeks, Reduce Wrinkles and Fine Lines, with Biotin, Silicon, and Arginine, 60 Tablets
My son does not seem to be a responder to NAC for intense galloping, jumping, pacing, talking to himself, vocal noises and finger waving in front of his face. Have tried varying doses and forms (regular and NAC Sustain). The only other thing he is on right now is Bumetanide (still trialing; dose is now at 1 mg per day each afternoon after school). He is 101 lbs/approx 46 kg. He may be more in the category of an Aspie except for the extreme stereotypy. I am interested in trying either the PS 128 or the low-dose Buspar to try to get a handle on the stereotypy. Is there a way to know which might be good to try first, along with continuing the bumetanide? Thank you.
ReplyDeleteAW there is no way really to know what will help. Try lots of interventions. Try PS128, try other bacteria. Try one that stimulates oxytocin. One interesting one from the past is now sold with a very healthy number of CFU (colony forming units) to treat osteoporosis, but it has numerous effects, it is sold in the US as Osfortis. Most commercial probiotics lack potency and so do not deliver their full potential.
Delete