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Blood clotting disorders and ME

Discussion in 'Other treatments' started by Binkie4, Feb 8, 2018.

  1. Binkie4

    Binkie4 Senior Member (Voting Rights)

    Messages:
    2,307
    @Liv aka Mrs Sowester and @ukxmrv thank you for your description of your experiences . I need to do loads more reading. Am surprised I've not come across Berg's protocol before.

    Also I usually have low O2. It was 92% when I was in hospital last week. I think there may be a thread here from someone else who has this.

    EDIT: thread started by @Mattie
     
  2. BeautifulDay

    BeautifulDay Established Member (Voting Rights)

    Messages:
    75
    Location:
    United States
    I have Factor V Leiden (FVL) heterozygous mutations (rs6025) plus the FV R2 heterozygous mutation (rs180059). FVL heterozygous by itself increases the risk of thrombosis by 3.5-4.4X. The combined FVL plus FV R2 compound heterozygous mutation makes one significantly more prone to blood clots.

    23andme had both of these called correctly for me and confirmed by my doctor with a medical lab. If 23andme tested you for both of these, then going into raw data and typing in F5 should pull up your list of F5 gene location calls.

    That FV R2 mutation by itself (without FVL mutation) is usually thought of as making one bleed easier. In theory, it reduces the amount of Factor V produced by the body, and since Factor V helps with clotting, having less of it reduces how easily someone clots. Yet, as we know the body generally has overlapping safeguards so it's not quite reduced in half.

    What they found is that people who have FVL and that FV is more clotty, and then they don't produce any other FV (FV R2 mutation) -- therefore, all the FV produced is clotty.

    This article in the American Society of Hematology's journal Blood, does a much better job explaining it than I.
    http://www.bloodjournal.org/content/94/9/3062?sso-checked=true

    My hematologist has me on two low dose aspirins a day for this. I know the symptoms of when I'm more clotty, and during those times I'll up my daily low dose aspirin to 3. I also know how my body reacts to too much aspirin, and I cut down on the aspirin when my teeth bleed upon brushing or when I slightly bump into something and it hurts like the dickens.

    There is a blood test that my hematologist gives me every once in a while to make sure I'm not taking too much aspirin for my body.

    I didn't pass the compound heterozygous mutations to the kids. I did pass the FVL heterozygous down to one of our children with mitochondrial disease. She often has severe pins and needles in her feet like I do. None of the other kids with MitoD have the pins and needles in their feet to the extent the two of us with FVL do. When I am good with taking my aspirins, it really helps with my pins and needles in my feet.

    One of our children doesn't have the FVL mutation, but does have the FV R2 mutation. That child gets severe nose bleeds, which makes sense given that child has half (or somewhat less) Factor V clotting in the blood.

    I believe a lot of genetics is this complex. This is why the researchers are going for the easier pickings of looking for mutations that cause X disease. But for every one of those easy picking mutations, there are many others that are more complex. I have no doubt they'll get around to how all the mutations interact, but not this year. ;)
     
  3. Jonathan Edwards

    Jonathan Edwards Senior Member (Voting Rights)

    Messages:
    13,269
    Location:
    London, UK
    The original blog does not make any scientific sense. The trial quoted does not provide any reliable information. I think it is a pity that people wander into recommending things they do not understand at all. I cannot see any good reason why any form of hyper coagulability should give rise to symptoms of ME.
     
    TiredSam and BeautifulDay like this.
  4. BeautifulDay

    BeautifulDay Established Member (Voting Rights)

    Messages:
    75
    Location:
    United States
    Thank you @Jonathan Edwards . I agree that the original trial sited at the beginning of the thread is very thin and has recommendations that are questionable and unsupported.

    I don't believe hyper coagulability by itself gives rise to ME. Our daughter who does not have FVL has debilitating fatigue, POTS, muscle spasticity, vocal cord and diaphragm paraperesis, exercise intolerance, quick turnover from aerobic to anaerobic, severe migraines, etc....

    However, for the two of us in the family with both FVL and MitoD, keeping our blood flowing does seem to put us in the best position to not have additional symptoms or compounding of symptoms.

    I believe keeping ourselves in the best health possible keeps our MitoD symptoms to the least we can. It's a matter of doing what is within our reach. For example, all of us with MitoD suffer from severe headaches. We have all noticed that when we let a tooth cavity go too long (even the smallest one), it increases the number and severity of headaches. If we can reduce the factors that bring on the symptoms, it definitely helps.

    Therefore, while I don't believe hyper coagulability by itself gives rise to ME, I do believe not keeping it within a normal range does exasperate other MitoD symptoms.
     
    Inara likes this.

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