At least we are finding significant differences to drive further research and testing. That’s usually how it begins.

The important part is:

>Based on our results we propose that immune exhaustion perpetuates long-COVID due to the seemingly complete reduction of IFNγ and IL-8, as well as significant decreases in IL-2, IL-4, IL-6, IL-13, and IL-17. Identifying these and other deficiencies will provide clues towards methods to intervene and possibly restore immune function in the context long-COVID. Although functional assays that test the ability of immune cells from individuals with long-COVID to respond to pathogenic stimuli will be required to support this theory.

I got sick for at most a day in Nov 21 and this all hit my suddenly end of Jan 22. They can’t even be sure I had COVID but given how I had sudden LC symptoms that’s what my doctor said was very likely. Always wondered why it came months after like a 1 day mild fever.

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State your study here - I don't believe this stat...

That stat can’t be true. HALF? We’d see it all around us

My friend hasn't tasted or smelled for 2 years. The fatigue is still quite prevalent too.

How long did you have it?

Glad you’ve recovered

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Permanezzy brezzy

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Lactoferrin has immune modulating properties. Among other benefits as an anti viral, bacterial, and fungal. Also gut modulating properties.

Get a micronutrient test done, check your Zinc and Vitamin C levels. They're likely depleted. Zinc and Vitamin C have fundamental roles in nourishing the gland which creates Cytokine molecules (Thymus Gland). Vitamin D also plays a crucial role. If we are insufficient in the nutrition that's responsible for Cytokine function, I would imagine that by bringing the nutrients to healthier levels would lead to higher cytokine levels. Issue is is that prolonged malnutrition of the Thymus gland actually leads it to have atrophy, which will mean lessened fundamental function. The sooner we replenish our Thymus, the better.

Virus's love to deplete Vitamin C and Zinc, because Vitamin C and Zinc are so readily necessary for Cytokine (immune fighting T Cells) to deploy and fight the virus. So not only will the virus deplete these key nutrients, but the key nutrients will be depleted leading to insufficient immune fighting function. Its a loop if you will.

For example, I have had a micronutrient panel done, I have resoundingly low levels of Zinc and Vitamin C. And now looking back realizing that during my last infection, I didn't even have a fever. It was extremely mild. Which is and could be in indication of a under functioning deployment of Killer T Cells to be sent out to fight the virus. As a indication that your T cells are busy fighting the virus is to have a fever, it is the body's natural process for killing viral material. Which makes me think, "Just think how many of us had "mild" or "asymptomatic" infections (no fever). Maybe even from the jab itself. Could our immune system of just been depleted? Hence leading to viral persistence within us still?"

GUY BELOW ME KNOWS MORE When a virus invades the host. The body's bacteria along with antibodies find and detect its existence. They then go to deploy Cytokine molecules from the Thymus gland to seek out and kill the viral matter through cells called "T cells", typically called "Killer T Cells". These cells engage the virus and begin to fight it. You usually experience symptoms like Fatigue, Fever, or other bodily dysfunctions during this time as your body is using natural processes to kill viral matter and protect itself.

In the above article it is stating that they are finding people with Long Covid don't have an overreactive immune system. But that they have an underreactive immune system. Specifically lessened Cytokine molecules aka T cells. T cells are the most crucial, when deployed they give the sensations of a "fever" and those other aforementioned bodily dysfunctions.

The Thymus gland produces Cytokine and T Cells. And it is fueled off of Vitamin C and Zinc. Vitamin C and Zinc are shown to be lessened in people with Long COVID. With insufficient nutrition the Thymus gland will have atrophy and shrink. This leading to a understrength baseline Immune System response in the future.

I'm now theorizing that our mild or asymptomatic infections are really red flags that our immune system was underprepared to fight off the virus. Or that our bodies did not have adequate antibodies or [gut] signaling bacteria to detect the existence of the virus for defense or deployment.

From the paper:

>Also referred to as the neutrophil chemotactic factor, IL-8 recruit’s neutrophils and NK-cells to sites of inflammation where they can clear infected cells and promote wound healing.

>It is possible that the apparent lack of IL-8 in long-COVID patients may be responsible for at least some of the debilitating symptoms including post-exertional malaise, fatigue, and persistent cough, shortness of breath and chest pain.

>In this scenario, the acute SARS-CoV-2 infection damages the lungs, the cytokine milieu unfolds as described above, recruiting cells to the site of damage where the cells can either (a) help control the infection and induce a wound healing environment and the individual recovers normally; or (b) the infection causes abundant cellular infiltration leading to a high concentration of immune cells in a relatively small physical space, ultimately causing more tissue damage, which is not efficiently repaired in the absence of IL-8.

>Predictably, under scenario ‘b’ the individual remains having difficulty with oxygen transfer from the lungs into the blood stream. Therefore, if the macrophages and other cells that secrete IL-8 become exhausted or are otherwise incapable of secreting IL-8, neutrophils will not be recruited to assist in the wound healing process in the lung once the infection has been cleared [63]. Scenario ‘b’ therefore emerges as a potential model to explain certain long-COVID complications based on lack of IL-8.

>IFNγ is secreted by the innate immune Natural Killer cells (NK) and Natural Killer T cells (NKT) as well as the adaptive immune CD4+ Th1 and CD8+ Cytotoxic T Lymphocytes (CTL) after the development of antigen-specific immunity [64]. Together with IL-12, IFNγhelps drive the differentiation of Th1 cells, which in turn can secrete IL-2, TNFα, and IFNγ [65]. The observed lack of circulating IFNγ (Figure 1 and Table 2) in the plasma of patients suggests either severe immune dysfunction or exhaustion.

The war in the lungs is over, but there are too many soldiers still there, hanging out, causing drama. What's not happening: they need to be transported away and the engineering+construction crews need to come in to start rebuilding.

How do you find these things out? I don't even know my blood type or how to find out.

There aren’t agreed upon bio markers yet which is partially why research like this is so important

Because you basically can't test for it yet.

James Patterson MD does some blood testing but insurance doesn’t cover it and it’s expensive. Go over to r/covidlonghaulers there’s mixed reviews on him.