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Memantine Cured Me.. But Why?

memantine

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#61 jack black

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Posted 20 December 2016 - 01:59 PM

Memantine seems to be an H3 agonist, and with H3 being an autoreceptor, would presumably worsen a mast cell disorder rather immediately due to the H3 agonism leading to more histamine synthesis and release from other histamine receptors. I agree a mast cell disorder or other histamine intolerance is too paradoxical given the OP's experience.

Http://forum.mindandmuscle.net/38826-memantine-activation-brain-histaminergic-neurotransmission


Did you actually read the discussion you linked? The concerns raised there mirror my own re: agonism of H3 leads to histamine inhibition.
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#62 BioFreak

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Posted 20 December 2016 - 03:11 PM

 

I just found out that memantine does actually activate histamine neurons in the brain.


This is news to me. Are you sure?

 

 

https://www.ncbi.nlm...pubmed/21057059 says:

 

 

In vivo, a single administration of memantine increased histamine neuron activity, as shown by the 60% increase of tele-methylhistamine (t-MeHA) levels observed in the brain of mice.



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#63 Omega 3 Snake Oil

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Posted 21 December 2016 - 03:47 AM

Are you guys noticing any improvements in your sleep at all?

 

I'm seeing a new neurologist in January for my insomnia and dysautonomia, which I'm thinking are both caused by some sort of thalamic dysfunction, maybe I should try and get on it?



#64 iseethelight

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Posted 26 December 2016 - 06:48 PM

I can't count the number of times I thought I had found a supplement that cured my disorders only to return to below baseline state a few days later. I've learned to never claim anything cured me until after months of testing. I haven't found that cure yet.


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#65 Caravaggio

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Posted 14 April 2018 - 09:44 AM

I'm currently investigatin in mercury toxicity as the cause of my symptoms. The symptoms in your Google document sound very familiar.

 

I found a connection between Memantine and Methylmercury:

 

Neurotox Res. 2013 Oct;24(3):320-37. doi: 10.1007/s12640-013-9386-3. Epub 2013 Mar 16.

Protective effects of memantine against methylmercury-induced glutamate dyshomeostasis and oxidative stress in rat cerebral cortex.
Liu W1, Xu Z, Deng Y, Xu B, Wei Y, Yang T.
 
Methylmercury (MeHg) is one of the ubiquitous environmental toxicant that leads to long-lasting neurological deficits in animals and humans. The identification of the underlying mechanisms has been a main focus of research in the neurotoxicology field. Glutamate (Glu) dyshomeostasis and oxidative stress have been identified as two critical mechanisms mediating MeHg-induced neurotoxicity. However, little has been known of the interaction between these two mechanisms that play in MeHg poisoning in vivo. We, therefore, developed a rat model of MeHg subchronic poisoning to evaluate its neurotoxic effects and investigated the neuroprotective role of memantine, a low-affinity, noncompetitive N-methyl-D-aspartate receptors (NMDARs) antagonist, against MeHg-induced neurotoxicity. Ninety rats were randomly divided into five groups: control, memantine control, MeHg-treated (4 and 12 μmol/kg), and memantine pretreated. Administration of 12 μmol/kg MeHg for 4 weeks significantly elevated total Hg levels, disrupted Glu metabolism, overexcited NMDARs, and led to intracellular calcium overload, which might be critical to excessive reactive oxygen species (ROS) formation in cerebral cortex. Meanwhile, MeHg administration reduced non-enzymatic (non-protein sulfhydryl, NPSH) and enzymatic (superoxide dismutase, SOD and glutathione peroxidase, GSH-Px) antioxidants; caused lipid, protein, and DNA oxidative damage; and enhanced neurocyte apoptosis in cerebral cortex. Moreover, glutamate/aspartate transporter (GLAST) and glutamate transporter-1 (GLT-1) appear to be inhibited by MeHg exposure. Pretreatment with memantine at a dose of 5 μmol/kg significantly prevented MeHg-induced alterations of Glu metabolism and oxidative stress, alleviated neurocyte apoptosis, and pathological injury. In conclusion, the results suggested that Glu dyshomeostasis and oxidative stress resulting from MeHg exposure contributed to neuronal injury. Memantine possesses the ability to attenuate MeHg-induced neurotoxicity through mechanisms involving its NMDARs-binding properties and indirect antioxidation.

https://www.ncbi.nlm...pubmed/23504438







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