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    Pro-oxidant therapy (w/ vitamin K) may treat cancer

    Literature Review
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    • H
      haidut
      last edited by

      The study is very new so I can’t get access to its full contents yet, but I wanted to post about it ASAP as it is one of the first studies in a major journal that specifically targets cancer’s redox nature – i.e. “cancer” cells are in a highly reduced state and administering pro-oxidant therapy (i.e. oxidizing agents or NAD+ precursors) is likely to be therapeutic. As my readers know quite well, quinone molecules are some of the most widely used for basic research and redox modulation, and the naphthoquinone family has been studied extensively specifically for cancer. Vitamin K and its analogs are napththoquinones that have been getting a lot of attention lately, culminating in the FDA approval of a cancer drug called Apatone (combination of vitamin K3 and vitamin C), which works exclusively through redox/metabolic mechanisms. Well, the study below used just vitamin K3 specifically for its pro-oxidant effects and found that it greatly diminished prostate cancer growth. The mechanism of action was generic (i.e. redox state) and applicable to every cell, healthy or “cancerous” alike. The study had an in-vivo component, and since most prostate cancer mouse models are done with xenograft models (human tumor hosted by another organism), the findings of study suggests that the effects of vitamin K(3) are relevant for human cancer. Since I cannot get access to the full study, I don’t know what dose they used and for how long the administration lasted. However, most human studies with the closely-related vitamin K2 (MK-4) typically use 30mg-45mg for cancer, and there are already highly promising human cancer trials with vitamin K2 (MK-4). In fact, the rumor is that vitamin K2 (MK-4) may soon be approved as a prescription drug for preventing/treating liver cancer, as well as various blood cancers (leukemias, lymphomas, etc). So, it looks like medicine is finally waking up from its “slumber” and recognizing that metabolism and redox state sit at the very core of “cancer” and should be primary targets for its treatment.

      https://pubmed.ncbi.nlm.nih.gov/39446948/

      “…In this work, we show that a pro-oxidant vitamin K precursor [menadione sodium bisulfite (MSB)] suppresses PC progression in mice, killing cells through an oxidative cell death: MSB antagonizes the essential class III phosphatidylinositol (PI) 3-kinase VPS34-the regulator of endosome identity and sorting-through oxidation of key cysteines, pointing to a redox checkpoint in sorting. Testing MSB in a myotubular myopathy model that is driven by loss of MTM1-the phosphatase antagonist of VPS34-we show that dietary MSB improved muscle histology and function and extended life span. These findings enhance our understanding of pro-oxidant selectivity and show how definition of the pathways they impinge on can give rise to unexpected therapeutic opportunities.”

      https://medicalxpress.com/news/2024-10-vitamin-supplement-prostate-cancer-mice.html

      “…Prostate cancer is a quiet killer. In most men, it’s treatable. However, in some cases, it resists all known therapies and turns extremely deadly. Published in the journal Science, a new discovery at Cold Spring Harbor Laboratory (CSHL) points to a potentially groundbreaking solution. CSHL Professor Lloyd Trotman’s lab has found that the pro-oxidant supplement menadione (vitamin K3) slows prostate cancer progression in mice. The supplement is a precursor to vitamin K, commonly found in leafy greens. The story begins more than two decades ago.”

      Via: http://haidut.me/?p=2698

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      • S
        sneedful @haidut
        last edited by sneedful

        @haidut is leucomethylene blue safe to take? It is what is left over after turning ascorbic acid ----> dehydroascorbic acid with MB. You've said before the mixture can be left out after the LMB and DHAA are produced and the LMB will oxidize back to MB, yet I'm unsure if the DHAA degrades in the meantime. I've thought of bubbling air back into the solution to get it to go blue again. And then again, I have the suspicion that the redox state of MB/LMB is pretty much inconsequential as it cycles between the forms relatively rapidly once ingested. My urine still changes color wether I take MB by itself or LMB + DHAA.

        I like taking it during winter.

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