Primary Progressive Apasia and Aluminum

Proposed Causes and Treatment of Primary Progressive Aphasia (PPA)

Dennis N. Crouse

February 16, 2021

Primary Progressive Aphasia (PPA) is a type of neurodegenerative condition that symptomatically is a slow deterioration of language ability (i.e., aphasia). PPA is associated with other neurodegenerative diseases such as Alzheimer’s (i.e., 1/3 of PPA cases) and frontotemporal lobar degeneration (i.e., 2/3 of PPA cases). PPA is therefore called a neurological syndrome.

The primary symptom of PPA is slowly progressing aphasia occurring as the dominate feature and lasting for at least the first two years of the disease. The first symptoms of PPA are declining speech and language capability followed later by memory loss manifesting itself as difficulty with word finding and object identification (i.e., anomia) and in many cases, finally progressing to a nearly total inability to speak (i.e., mutism). PPA is slowly progressive unlike other forms of aphasia that arise suddenly from stroke or brain injury. PPA is also unlike Alzheimer’s disease as PPA patients have aphasia as the dominant symptom before memory loss and can take care of themselves, maintain their daily living skills, and even remain employed. 

Bird Watching as a Test for PPA

In later life I have resumed the hobby of bird watching that I first began in my early teens. Warblers are my favorite group of birds as they can be easily identified by their plumage and nuanced songs. The art of being a successful warbler watcher hinges on the ability to spot the bird either visually and/or audibly (i.e., sensory processing), identify the name of the warbler from a memorized lexicon of key features (i.e., semantic processing), and finally call out the name of the warbler to others (i.e., articulation). In my teens this three-step process could be carried out in less than a second. But as I have grown older it has been slowed by what is called a “tip-of-tongue delay” caused by temporary anomia. If this delay becomes progressively longer and more frequent over a two-year period it could be a symptom of PPA.

 Brain Atrophy as a Causal Factor of PPA

Brain atrophy (e.g., cortical thinning) of specific areas of the brain is correlated with different symptomology in both patients with PPA and language variants of frontotemporal lobar degeneration (FTLD) as shown in table 1^1,2.

Table 1. Variants of PPA and FTLD, Symptoms, and Location of Brain Atrophy1,2
PPA Variant	Primary Symptom	Location of Brain Atrophy
Agrammatical (PNFA)	Effortful and Halting Speech	Left inf. frontal lobe & ins. cortex
Semantic (SemD)	Anomia	Bilaterally in ant. temporal lobes
Logopenic	Impaired Single Word Retrieval	Left pos. temporal & parietal lobes

PNFA = Progressive Nonfluent Aphasia; SemD = Semantic Dementia; inf. = inferior; ins. = insular; ant. = anterior; pos. = posterior

As PPA or language variants of FTLD progress, brain atrophy extends to other lobes of the brain following a distinct pattern that depends upon the variant². Brain atrophy is also a characteristic of AD, with brain atrophy observed in the frontal and entorhinal cortexes and hippocampus³.

 Brain atrophy in AD is due to the programmed death of neurons during what is called neuronal cell cycle events (CCEs)⁴. The cause of this programmed death is a cytokine modulated cascade that starts with a xenobiotic chemical or pathogen infecting the brain and causing inflammation. Tumor necrosis factor (TNF-alpha) is the primary cytokine responsible for CCEs⁴.  TNF-alpha is a cytokine released by both some white blood cells, called macrophages, and microglial cells in the brain to alert the immune system of an infective agent, such as a toxic metal or pathogen, and induce the process of inflammation.

Higher than normal levels of microglial derived TNF-alpha may play a central role in pathogenesis of Alzheimer’s disease^4,5, late stage dementia⁶, and have been documented in the cerebrospinal fluid of patients with frontotemporal dementia⁷. Therefore, because PPA is associated with both Alzheimer’s and frontotemporal dementia, excess TNF-alpha is also likely involved with brain atrophy observed in PPA^1,2.

Blood-Brain Barrier as the Brain’s Leaky Roof

The blood-brain barrier acts as a protective roof over the brain to keep environmental factors, such as toxic metals and pathogens, from leaking into the brain. This roof becomes leaky due to chemically or physically induced trauma(s). Chemical trauma includes environmental toxins and oxygen deprivation (i.e., hypoxia) caused by stroke or white matter hyperintensities. Physical trauma includes traumatic brain injury due to a blow to the head. Leaks are sporadic and result in localized brain atrophy due to chronic exposure to leaking toxins. 

  

Aluminum Induces TNF-alpha Expression

TNF-alpha is deadly to neurons because with the enzyme JNK a self-amplifying loop is created that induces the generation of reactive oxygen species (ROS) that kills neurons⁸. Toxic metals also induce the production of reactive oxygen species (ROS) in microglial cells of the brain that can kill neurons. The metal that tops the list for ROS production in microglial cells is aluminum as shown in table 2⁹.

Table 2 - Metal Ion Induction of ROS in Human Microglial Cells9
Metal Sulfate	Relative Induction of ROS
Aluminum	10
Iron	6
Manganese	4.5
Zinc	4
Nickel	3.5
Lead	3.5
Gallium	3
Copper	3
Cadmium	3
Tin	2
Mercury	1.5
Magnesium	0
Sodium	0

 

In 1999 it was discovered that aluminum in drinking water (i.e., 0, 5, 25, and 125ppm) for one month enhances the expression of TNF-alpha in mice in a dose-dependent manner .This increased expression due to aluminum was only observed in the cerebrum not in peripheral cells suggesting that microglial cells were the source of increased TNF-alpha¹⁰. Five years later in 2004 this discovery was duplicated by another group. Aluminum lactate in drinking water (i.e., 0.27, 2.7, and 27ppm of aluminum)  for 10 weeks up-regulated TNF-alpha expression, and enhanced reactive microglia in the striatum of mice¹¹. Therefore, aluminum induces the production of TNF-alpha and ROS resulting in a deadly cocktail for neurons causing PPA, AD, and frontotemporal lobar degeneration.   

 

Aluminum Induces Brain Atrophy in AD

Aluminum hotspots in the AD brain were first observed in 1973¹². Aluminum hotspots in the brain are dependent upon where aluminum leakage across the blood-brain-barrier occurs. The location of these hotspots can be random making PPA, AD, and frontotemporal lobar degeneration all primarily sporadic diseases. The sporadic location of aluminum hotspots can account for the variability in symptoms and disease diagnosis of PPA as shown in table 1. Likewise, the locations of aluminum hotspots coincide with the locations of brain atrophy in AD as shown in tables 3 and 4^3,13.

Table 3. Brain Atrophy in Humans with AD and Non-demented Controls During 1 Year3
Regions of Brain Analyzed	AD Longitudinal                  % Change	Controls Longitudinal            % Change
Entorhinal Cortex	-2.42	-0.55
Hippocampus	-3.75	-0.84
Frontal Cortex (caudal)	-1.60	-0.40
Frontal Cortex (ventral)	-1.06	-0.38

 

Table 4. Brain Aluminum in Humans with AD and Non-demented Controls13
Regions of Brain Analyzed	AD                                      (Al mcg/g of brain tissue)	Controls                                 (Al mcg/g brain tissue)
Entorhinal Cortex	10.2 + 9.0	1.5 + 0.6
Hippocampus	4.9 + 3.0	1.4 + 0.6
Frontal Cortex (caudal)	6.8 + 4.3	1.8 + 0.6
Frontal Cortex (basal/ventral)	6.4 + 2.9	2.5 + 0.7

 

Autopsy and analysis of 242 brains of people diagnosed with AD, as reported in six studies, have revealed that in all cases AD brains have higher than normal levels of aluminum^13,14,15-18. Autopsy and analysis of brains from people with early^13,14,18 or late onset AD^13,14,15-17 and with familial^15,16, sporadic^13,14,17 or occupational AD¹⁸ all had higher than normal levels of aluminum. Because of the role played by aluminum in brain atrophy, it could be theorized that it may also play a role in PPA and frontotemporal dementia. However, there are no studies of aluminum in the brains of patients who had been diagnosed with either frontotemporal dementia or PPA prior to death.

Synaptic Loss in PPA

The loss of synapses in neurodegenerative diseases, such as AD, is better correlated with cognitive decline than is neuronal loss^19,20. Synaptic loss impairs the ability of neurons to communicate and underlies the cognitive deficits seen in those with PPA²¹. This loss of synapses was observed in Broca’s area of the brain in a patient with PPA²¹. Impaired cortical synaptic connections in the part of Broca’s area with synaptic loss could account for the symptoms of PPA seen in the patient²¹.

The loss of synapses (e.g., synaptic integrity) is correlated with the loss of synaptophysin, a major synaptic vesical protein. The pathological severity of AD is negatively correlated with the amount of synaptophysin mRNA in temporal cortex neurons²². In addition, the amount of synaptophysin was reduced by 30% of normal levels in the prefrontal cortex of those with severe AD^23,24. Synaptic vesicle formation in vitro and therefore the amount of synaptophysin at synapses is inhibited by aluminum fluoride commonly found in fluoridated drinking water²⁵.

Therefore, aluminum not only causes the loss of neurons but also aluminum bonded to fluoride causes the loss of synapses by inhibiting synaptic vesicle formation as seen in those with PPA^21,25.    

Treatment of PPA

Because of the role played by TNF-alpha in brain atrophy, it has been suggested that TNF-alpha inhibitors, such as Etanercept, could be used to treat PPA^26,27 and Alzheimer’s disease²⁸.  Although published results in 2008 looked good on the basis of a single case of PPA²⁶, there has not been a published duplication of this case study on a larger number of PPA cases with controls.

Aluminum accumulation in the brains of those with PPA could be targeted for detox with orthosilicic acid (OSA) in drinking water²⁹. There are no published studies of OSA treatment of patients with PPA. However, OSA in drinking water has been shown to improve cognition in some AD patients and has been shown to remove aluminum from the brains of rats^30-32. In addition, drinking OSA rich water is correlated with a lower risk of AD as shown in an epidemiological study³³.

Conclusion

Primary Progressive Aphasia (PPA) is a neurological syndrome associated with either Alzheimer’s disease (AD) or frontotemporal lobar degeneration (FTLD). Neuronal and synapse atrophy, along with higher-than-normal levels of the cytokine tumor necrosis factor (TNF-alpha), has been observed in patients with PPA, AD and FTLD symptoms. Aluminum in drinking water enhances the expression of TNF-alpha in mice and is a putative causative factor of AD. Both aluminum and TNF-alpha are associated with increased ROS generation in glial cells of the brain that can result in neuronal and synapse atrophy. Since orthosilicic acid (OSA) in drinking water facilitates the removal of aluminum in rat brains and can improve cognition in AD patients, it is hypothesized that OSA in drinking water can also decrease symptomology in PPA patients.     

References

1.      Matias-Guiu, J.A. and Garcia-Ramos, R.; Primary progressive aphasia: From syndrome to disease; Neurologia; 28(60:366-74 (2013)

2.      Rohrer, J.D., et al.; Patterns of cortical thinning in the language variants of frontotemporal lobar degeneration; Neurology; May; 72:1562-9 (2009)  

3.      Fjell, A.M., et al.; One-year brain atrophy evident in healthy aging; J. Neurosci.; Dec.; 29(48):15223-31 (2009)

4.      Bhaskar, K., et al.; Microglial derived tumor necrosis factor-alpha drives Alzheimer’s disease-related neuronal cell cycle events; Neurobiol. Dis.; Feb.; 62:1-29 (2013)

5.      Fillit, H., et al.; Elevated circulating tumor necrosis factor levels in Alzheimer’s disease; Neurosci. Lett.; Aug.; 129(2):318-20 (1991)

6.      Bruunsgaard, H., et al.; A high plasma concentration of TNF-alpha is associated with dementia in centenarians; J. Gerontology; Medical Sciences; 54A(7):M357-M364 (1999)

7.      Sjogren, M., et al.; Increased intrathecal inflammatory activity in frontotemporal dementia: pathophysiological implications; J. Neurosurg. Psychiatry; 75:1107-11 (2004)

8.      Blaser, H., et al.; TNF and ROS crosstalk in inflammation; Trends Cell Biol.; Apr.; 26(4):249-61 (2016)    

9.      Pogue, A.I., et al.; Metal-sulfate induced generation of ROS in human brain cells: detection using an isomeric mixture of 5- and 6-carboxy-2’,7’-dichlorofluoresein diacetate (carboxy-DCFDA) as a cell permeant tracer, Int. J. Mol.; 13:9615-26 (2012)  

10.  Tsunoda, M., and Sharma, R.P.; Modulation of tumor necrosis factor alpha expression in mouse brain after exposure to aluminum in drinking water; Arch. Toxicol.; Nov.; 73(8-9):419-26 (1999)

11.  Campbell, A., et al.; Chronic exposure to aluminum in drinking water increases inflammatory parameters selectively in the brain; J. Neurosci. Res.; Feb.; 75(4):565-72 (2004)

12.  Crapper, D.R., Krishnan, S.S., Dalton, A.J.; Brain aluminum distribution in Alzheimer’s disease and experimental neurofibrillary degeneration; Science, May, 180(4085):511-3 (1973)

13.  Andrassi, E., et al.; Brain Al, Mg, an P contents or control and Alzheimer-diseased patients; J. Alzheimer’s Dis.; 7:273-84 (2005)

14.  Rusina, R., et al.; Higher aluminum concentrations in Alzheimer’s disease after Box-Cox data transformation; Neurotox. Res.; 20, 329-33 (2011)

15.  Mirza, A., et al.; Aluminum in brain tissue in familial Alzheimer’s disease; J. Trace Elements in Medicine and Biology; Mar.; 40:30-36 (2017)

16.  Mold, M.; et al.; Aluminum and amyloid-B in familial Alzheimer’s disease; J. Alz. Dis.; 1:1-8 (2019)

17.  McLachlan, D.R.C., et al.; Aluminum in neurological disease – a 36 year multicenter study; J. Alzheimer’s Dis. Parkinsonism; 8: 457 (2018)

18.  Exley, C., and Vickers, T.; Elevated brain aluminum and early onset Alzheimer’s disease in an individual occupationally exposed to aluminum: a case report; J. Med. Case Reports; 8:41 (2014)

19.  Terry, R.D., at al.; Physical basis of cognitive alterations in Alzheimer’s disease: Synaptic loss if the major correlate of cognitive impairment; Ann. Neurol.; Oct.; 30(4):572-80 (1991)

20.  Masliah, E., et al.; Immunohistochemical quantification of the synapse-related protein synaptophysin in Alzheimer’s disease; Neurosci. Lett.; Aug.; 103(2):234-9 (1989)

21.  Lippa, C.F. and Rosso, A.L.; Loss of synaptophysin immunoexpression in primary progressive aphasia; Am. J. Alzheimer’s Dis. Other Dementias; 27(4):250-3 (2012)

22.   Heffernan, J.M., et al.; Temporal cortex synaptophysin mRNA is reducted in Alzheimer’s disease and is negatively correlated with the severity of dementia; Exp. Neurol.; Apr.; 150(2):23509 (1998)

23.  Shimohama, S., et al.; Differential involvement of synaptic vesicle and presynaptic plasma membrane proteins in Alzheimer’s disease; Biochem. Biophys. Res. Commun.; Jul.; 236(2):239-42 (1997)

24.  Minger, S.L., et al.; Synaptic pathology in prefrontal cortex is present only with severe dementia in Alzheimer’s disease; J. Neuropath. Exp. Neurol.; Oct.; 60(10):929-36 (2001)

25.   Cleves, A.E., et al.; ATP-dependent formation of free synaptic vesicles from PC₁₂ membranes in vitro; Neurochem. Res.; Aug.; 22(8):933-40 (1997)

26.  Tobinick, E.; Perispinal Etanercept produces rapid improvement in primary progressive aphasia: Identification of a novel, rapidly reversible TNF-mediated pathophysiologic mechanism; Medscape J. Med.; Jun.; 10(6):135 (2008)

27.  Griffin, W.S.T.; Perispinal Etanercept: Potential as an Alzheimere therapeutic; J. Neuroinflammation; Jan.; 5:3 (2008)

28.  Chang, R., et al.; Tumor necrosis factor alpha inhibition for Alzheimer’s disease; J. Central Nerv. Sys. Dis.; 9:1-5 (2017)

29.   Crouse, D.N.; Increasing IQ, cognition and COVID-19 cure rate with essential nutrients; Etiological Publishing (2021)

30.  Exley, C., at. al.; Non-invasive therapy to reduce the body burden of aluminum in Alzheimer’s disease; J. Alzheimer’s Dis.; Sept., 10(1):17-24 (2006)

31.   Davenward, S., et al.; Silicon-rich mineral water as a non-invasive test of the ‘aluminum hypothesis’ in Alzheimer’s disease; J. Alzheimer’s Dis.; 33(2):423-30 (2013)

32.  Belles, M., et al.; Silicon reduces aluminum accumulation in rats: Relevance to the aluminum hypothesis of Alzheimer’s disease; Alzheimer Disease Associated Disorders; 12(2):83-87 (1998)

33.   Rondeau, V., et al.; Aluminum and silica in drinking water and the risk of Alzheimer’s disease or cognitive decline: findings from 15-year follow-up of the PAQUID cohort, Am. J. Epidemiol. 169:489-96 (2009)

 

Increasing IQ, Cognition and Cure Rate of COVID-19 with Essential Nutrients ( my third book)

 I have just published my third book “Increasing IQ, Cognition and COVID-19 Cure Rate with Essential Nutrients”.  The book is now available as a softcover or Kindle e-book at Amazon. IQ of children born after World War II interests me as it had been rising until it began taking a nosedive in seven countries during the 70’s. My interest in finding out why this “brain drain” was happening came full circle with what I had researched in the 70’s and resulted in my new book. Brain drain is primarily due to environmental chemicals and viruses that impact both brain development, lowering IQ in the very young and killing neurons causing cognitive decline and Alzheimer’s in aging adults. These brain drainers are summarized in my new book.

Philippe Grandjean in his book “Only One Chance” asked the following question: “Could science develop some kind of antidote to counteract brain drain?”  The answer to Grandjean’s question is YES antidotes to counteract brain drainers have now been identified, tested, and are described in my new book. Essential nutrients as brain savers are identified that are scientifically based and tested antidotes to counteract brain drain in children and adults. Two brain savers are identified in my book and described anecdotally as detoxing brain drainers causing attention deficit hyperactivity disorder (ADHD), autism spectrum disorder (ASD), and seizures in children. Also, the “Crouse Protocol” is described that uses essential nutrients as brain savers and nootropics to reverse mild cognitive impairment (MCI) and possibly prolong and save the lives of those with Alzheimer’s disease, such as my mother.

While writing my new book during 2020 it was discovered that SARS-CoV-2, the virus responsible for the COVID-19 pandemic, was a brain drainer. Also, while writing this book it was discovered that three brain savers not only target the detox of brain drainers but also enhance the immune system. These three over-the-counter essential nutrients as brain savers have been shown during 2020 to make humans more likely to be cured and survive the COVID-19 pandemic.

I hope you find my new book useful and as interesting to read as it was to write. 

Stay Healthy, Dennis

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https://www.amazon.com/Increasing-Cognition-COVID-19-Essential-Nutrients/dp/B08TZ7HLNX/ref=sr_1_4?dchild=1&keywords=dennis+n+crouse&qid=1612120912&sr=8-4

 

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Safety of OSA Augmentation

Safety of OSA Augmentation

OSA and its salt, sodium silicate, are not silica (SiO₂ silicon dioxide). Dissolved in water, OSA and sodium silicate can’t be converted to silica and silica is not converted to OSA in the human body. Therefore, the toxicology of silica does not apply to OSA or its salt, sodium silicate. 

It is safe to drink bottled OSA rich water and beer. For a list of waters and beers see appendices I and II. It is also safe to drink handcrafted Silicade made by neutralizing a sodium silicate produced by PQ Corporation and sold online that is 99.5% water soluble (see appendix III). This product is sold by PQ Corporation directly and distributed through Brenntag to many U.S. community water departments that add it to public drinking water. In addition to being a brain saver, OSA provides corrosion protection. This PQ Corporation product meets the ANSI standard specification set by the American Water Works Association (AWWA) for silicates added to drinking water, as it contains only a 0.5% water insoluble impurity²²².

OSA is commonly found in rivers, lakes, aquifers, and drinking waters around the world¹⁴⁰. Dissolved OSA from soluble silicates added to drinking water in the U.S. is identical to dissolved OSA in beer and mineral waters^140,232.  The amount of OSA in drinking water varies widely depending upon the source¹⁴⁰.  In the U.S. 160ppm of dissolved silicates as OSA are generally recognized as safe (i.e., GRAS) in drinking water by the FDA²²¹. The adequate intake of water per day is 3 liters for men and 2.3 liters for women. This level of water intake corresponds to a maximum safe level of OSA intake per day of 480mg for men and 368mg for women. Therefore, drinking 4 cups (approximately 1 liter) of OSA rich water each day containing 50 to 150mg per liter of OSA is well below the GRAS level for dissolved silicates.

It is safe to ingest dissolved silicates, such as OSA, at concentrations well below the saturation level (i.e., less than 200ppm of OSA) in order to ensure that they will not become supersaturated and crystallize in the kidney lumen. Ingesting OSA above the saturation level (i.e., 200ppm) can result in kidney stones (a.k.a. nephrolithiasis) in dogs but almost never in humans. There is one report of kidney stones resulting from too much silicate salt, erroneously labeled as silica (SiO₂), used as an inactive ingredient (a.k.a. excipient) in several over-the-counter drugs such as Uncaria Tomentosa, Digestive Advantage, and FlexProtein supplements⁵⁰⁷. 

Excerpt from book

Increasing IQ, Cognition and Cure Rate of COVID-19 with Essential Nutrients

Targeted Detox Improves Children’s IQ, ADHD Behavior, and Adult Cognition

by Dennis N Crouse The book will be published in Jan 2021 and will be available on Amazon.