the TLDR here is they have quantified the energy consumption and fermentation of cancer cells and show that only glucose and glutamine can produce ATP in cancer cells. This has large implicates for cancer treatments.
Would we potentially be looking at treatments that locally cut off the supply of glucose and glutamine to the cancers, or is the implication different?
yes, I think so. Not locally, the whole body has to reduce the glucose and glutamine availability because everything is interconnected through the blood
https://hackertalks.com/post/8609461
Here is the proposed press-pulse protocol : https://pubmed.ncbi.nlm.nih.gov/28250801/ - Press-pulse: a novel therapeutic strategy for the metabolic management of cancer
Here is a application of that protocol for glioblastomas : https://pubmed.ncbi.nlm.nih.gov/39639257/ - Clinical research framework proposal for ketogenic metabolic therapy in glioblastoma
The press-pulse model shows lots of promise, and there are multiple ongoing studies with glioblastomas using this protocol.
Basically - deep ketosis, then periods of medicine to reduce glucose and glutamate
I swear, if keto cures cancer we'll never hear the end of it.
I'm sure someone is working on a epidemiological association right now!
Dr. Seyfried also has a conversational video talking about the paper https://www.youtube.com/watch?v=Pl5Nt3WrV5E
summerizer
In this video, Professor Seyfried discusses his recent paper that challenges long-standing assumptions in cancer treatment, specifically focusing on the Warburg hypothesis. He argues that many contemporary theories about cancer are based on misinterpretations of data from influential scientists like Otto Warburg and Sydney Weinhouse. Seyfried emphasizes that cancer is primarily a metabolic disease, driven by energy dysregulation instead of traditional genetic mutations. He introduces new insights into the role of mitochondrial function and the necessity of fermentable fuels like glucose and glutamine in cancer cell metabolism.
Key Points
Cancer Misunderstandings
Professor Seyfried outlines how modern cancer treatment theories derive from incorrect interpretations of ancient data, particularly misrepresenting the energy metabolism of cancer cells. He argues that this has led the cancer research field astray for decades.
Warburg Hypothesis Re-evaluated
Seyfried discusses the Warburg hypothesis, which posited cancer as a disorder of energy metabolism due to insufficient oxidative phosphorylation. He explains how earlier interpretations of data failed to acknowledge other forms of ATP production in cancer cells.
Oxygen Consumption vs ATP Production
The video highlights Seyfried's findings that oxygen consumption does not accurately correlate with ATP production in cancer cells, as opposed to normal cells where oxygen consumption is an effective marker. This distinction is crucial for understanding cancer metabolism.
Mitigating Cancer Growth with Fuel Restrictions
Seyfried suggests a paradigm shift in cancer treatment—removing glucose and glutamine as energy sources—since these fuels drive cancer cell growth. He proposes ketogenic metabolic therapy as a more viable approach for managing cancer.
Mitochondrial Function in Cancer
The discussion emphasizes that cancer cells exhibit mitochondrial dysfunction, leading to altered energy production mechanisms and excessive lactic acid and lipid droplet accumulation. These abnormalities are signals of compromised oxidative phosphorylation capabilities.
Demand for New Cancer Treatment Models
Finally, Seyfried calls for a review of cancer treatment strategies based on understanding its metabolic origins rather than purely genetic approaches, asserting the need to develop management techniques that address the metabolic dysfunctions of tumors.
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