Doxycycline interferes with tau amyloid aggregation abolishing its associated neuronal toxicity

Medina, Luciana; González‐Lizárraga, Florencia; Dominguez-Meijide, Antonio; Ploper, Diego; Parrales,; Sequeira, Sabrina; Ms, Cima-Omori; Zweckstetter, Markus; E, Del Bel; Michel, Patrick P.; Tf, Outeiro; Raisman‐Vozari, Rita; Chehı́n, Rosana; Sb, Socias

doi:10.1101/2020.11.18.388561

Cited by 2 publications

(4 citation statements)

References 77 publications

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“…[16,23] Additionally, our previous research on the subject pointed to the importance of maintaining a specific structural motif in tetracyclines, which is crucial to interact with cross-β structures characteristic of amyloid aggregates of α-Syn. [19] The substitution at the C 9 position was already studied in the tetracycline class to modulate their antibiotic activity; [28][29][30][31] however, nothing was reported about 4-des-N-dimethylamino tetracyclines with substituents at the C 9 position. Indeed, to prepare these new analogs, the aromatic D ring appears to be well suited to achieve aromatic electrophilic substitutions at either positions C 9 or C 7 .…”

Section: Chemical Synthesismentioning

confidence: 99%

“…Fluorescence emission was recorded from 410 to 610 nm using a Fluoromax-4 spectrofluorometer. [19] Additional discussion and UV-absorbance and fluorescence spectra are available in supporting information.…”

Section: Orthogonal Assaysmentioning

confidence: 99%

“…[9][10][11] In particular, DOX was able to prevent or modulate the aggregation process of α-Syn, [12,13] reduce oxidative stress, repress neuroinflammatory processes, [13,14] in either ex vitro and in vitro assays as well as in vivo models that mimic PD neurodegenerative events. [12,[15][16][17] These pieces of evidence, along with DOX's ability to cross the blood-brain barrier [18] and its safe toxicological profile make this tetracycline a good candidate for neuroprotection in PD but also for Alzheimer's disease, [19,20] Huntington's disease [11] and other neurodegenerative disorders. [10,17,21] However, using DOX for long-term treatment of patients may lead to potential antibiotic resistance and microbiota disruption.…”

Section: Introductionmentioning

confidence: 99%

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C9‐Functionalized Doxycycline Analogs as Drug Candidates to Prevent Pathological α‐Synuclein Aggregation and Neuroinflammation in Parkinson's Disease Degeneration

Rose,

Tomas‐Grau,

Zabala

et al. 2024

ChemMedChem

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Doxycycline, a semi‐synthetic tetracycline, is a widely used antibiotic for treating mild‐to‐moderate infections, including skin problems. However, its anti‐inflammatory and antioxidant properties, combined with its ability to interfere with α‐synuclein aggregation, make it an attractive candidate for repositioning in Parkinson's disease. Nevertheless, the antibiotic activity of doxycycline restricts its potential use for long‐term treatment of Parkinsonian patients. In the search for non‐antibiotic tetracyclines that could operate against Parkinson’s disease pathomechanisms, eighteen novel doxycycline derivatives were designed. Specifically, the dimethyl‐amino group at C4 was reduced, resulting in limited antimicrobial activity, and several coupling reactions were performed at position C9 of the aromatic D ring, this position being one of the most reactive for introducing substituents. Using the Thioflavin‐T assay, we found seven compounds were more effective than doxycycline in inhibiting α‐synuclein aggregation. Furthermore, two of these derivatives exhibited better anti‐inflammatory effects than doxycycline in a culture system of microglial cells used to model Parkinson’s disease neuroinflammatory processes. Overall, through structure‐activity relationship studies, we identified two newly designed tetracyclines as promising drug candidates for Parkinson’s disease treatment.

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Section: Chemical Synthesismentioning

confidence: 99%

Section: Orthogonal Assaysmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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C9‐Functionalized Doxycycline Analogs as Drug Candidates to Prevent Pathological α‐Synuclein Aggregation and Neuroinflammation in Parkinson's Disease Degeneration

Rose,

Tomas‐Grau,

Zabala

et al. 2024

ChemMedChem

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“…Doxycycline can penetrate the blood brain barrier [24]. This antibiotic blocks tau amyloid aggregation and its associated neuronal toxicity in vitro [25,26]. Doxycycline can inhibit the aggregation of Aβ42 amyloid fibrils and disassemble mature amyloid fibrils [27].…”

Section: Doxycycline and Minocyclinementioning

confidence: 99%

Possible Treatments for COVID Vaccine Induced Prion Disease

2023

Recent Adv Clin Trials

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Many COVID-19 “vaccines" are considered bioweapons and are known to have the ability to cause prion disease. Prion inducing agents have been researched extensively as potential bioweapons and the field of prion research is infiltrated by clandestine bioweapons operatives. In order for prion disease inducers to be an ideal bioweapon the target population needs to believe there is no cure while the attacker knows of an treatment/ antidote to save its own population if there is “blowback”, where the attackers' population gets exposed to the bioweapon. The narrative in the prion field is that there is no effective treatment for prion disease. However false narratives are the norm in the current COVID-19 related bioweapons attack. The author performed a literature search to determine if any effective treatments to COVID “vaccine" induced prion disease may exist but hidden from the public. The author believes several such candidates may exist and their use for treating COVID “vaccine" induced prion disease needs to be explored. These agents include doxycycline and related minocycline, quinacrine and ivermectin. The nature of this paper is speculative in large part because of the use of bioweapons in the current civil war. It is of no surprise to many that people working in government, medicine, science, and the pharmaceutical industry are deliberately trying to cause harm while pretending to help humanity. One only has to read the long list of influential people associated with Mossad operative Jeffrey Epstein to realize the extent of evil in today’s world.

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Doxycycline interferes with tau amyloid aggregation abolishing its associated neuronal toxicity

Cited by 2 publications

References 77 publications

C9‐Functionalized Doxycycline Analogs as Drug Candidates to Prevent Pathological α‐Synuclein Aggregation and Neuroinflammation in Parkinson's Disease Degeneration

C9‐Functionalized Doxycycline Analogs as Drug Candidates to Prevent Pathological α‐Synuclein Aggregation and Neuroinflammation in Parkinson's Disease Degeneration

Possible Treatments for COVID Vaccine Induced Prion Disease

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