LTT - Immune Function

Use of LTT in immune function testing

The lymphocyte transformation test (LTT) was first used in the early 1980ies; at that time exclusively to study the immunocompetence of T helper cells. Twenty more years had to pass before allergy and infection testing were added to its indications.

Over the years, LTT Immune Function (LTT-FU) has developed into a method capable of providing quantitative measurements of the functioning of immune cells extracted from blood. The basic principle underlying the test is to stimulate lymphocytes by exposing them to components of common pathogens or vaccines. These represent memory antigens which should trigger a strong immune reaction in people with a healthy immune system. When the LTT is performed, these antigens are first prepared by monocytes and dendritic cells and then presented to T helper cells. The specific T cells are activated and stimulated to divide, subject to the current state of immunocompetence. Quantitative measurements of DNA synthesis which always goes along with cell division are then performed. Strong activation in the LTT is indicative of intact immune function. It is also possible to use the LTT to monitor immune function over time. In this way it can be checked whether an improvement in the immune function has been achieved by immunostimulatory treatments (therapy monitoring).

The LTT Immune Stimulation is more extensive compared with the LTT Immune Function. With this test, selected immunogenic immunostimulants are tested in addition to the 6 memory antigens.

Especially when used for therapy monitoring, the LTT Immune Stimulation helps to individually select suitable immunostimulatory products or to detect early on any loss in efficacy (see here).

Clinical cardinal symptoms of a cellular immunodeficiency include:

  • Reduced resistance to infection
    Mainly against viruses, persisting intracellular bacteria and yeasts (Candida) with primary manifestation at the mucous membranes of the upper respiratory tract and the intestines.
  • Significantly prolonged convalescence after acute infections
  • Wound healing disorders
  • Reduced immunocompetence against tumour cells

Cellular immunodeficiencies can be congenital (primary immunodeficiencies, some with late manifestation at an advanced age) or secondary to an underlying disease, such as malignancies, chronic inflammatory conditions, infections (not only HIV!), or immunosuppressive treatment (secondary immunodeficiencies).

The most common causes of secondary cellular immunodeficiencies in patients with chronic inflammatory diseases is the impact of the systemic inflammation on the immune system itself. These can be triggered or promoted by malnutrition and unhealthy eating habits, chronic stress, allergic conditions and chronic persistent infections.

The interaction of the endocrine system, the nervous system and the immune system make the immune defence against pathogens and also tumour cells so complex that it is difficult to assess.

Without advanced cellular immune function tests it is impossible to obtain quantitative measurements of the severity of immune function disorders, especially as the Mérieux multitest has been taken off the market because of its low reproducibility.

Today, effective immunomodulatory treatments are available. Therefore, high-quality qualitative tests are of utmost importance to support the selection of adequate treatment options and to monitor efficacy.

Indications for the LTT Immune Function (LTT-FU)

  • Increased susceptibility for infections / Frequent acute or chronic infections
    Mainly caused by viruses, persisting intracellular bacteria and yeasts (Candida).
  • In cancer patients
    To determine the functional immune status before and after surgery or chemotherapy and radiotherapy as well as over the course of immunostimulatory treatments.
  • In chronic inflammatory diseases
    To assess the secondary immunodeficiency resulting from systemic inflammation.
  • In HIV infection
    To determine the current immunological status, before and over the course of antiviral therapy (evidence of restoration of a functional immune system).
  • Where immunodeficiency is suspected
    due to malnutrition (vitamin, zinc, protein and iron deficiency).

What sampling material is required?

20 mL heparin blood and 5 mL whole blood.
Please request the collection material (LTT blood collection set) from the laboratory free of charge: Fon: +49 30 77001-220, Fax: +49 30 77001-236, E-Mail: LTT@imd-berlin.de

No more than 24 hours must elapse from the time the blood is collected to the time of receipt of the sample in the laboratory. During this time the blood samples should be stored at room temperature. We offer a free nationwide courier service.

Blood samples for cellular function tests should not be stored in the fridge!

LTT - Immune stimulation

Can the LTT also test the efficacy of immunostimulatory products?

CD4 helper and cytotoxic CD8 lymphocytes play a critical role in the defence against viruses and persisting intracellular bacteria and are also critical for tumour surveillance. Functional deficits of these cells can be both cause and consequence of chronic debilitating diseases.
The reconstitution of the immune system is a cornerstone of the treatment of lowered infection resistance and central to the support and aftercare with curative cancer treatments.
Today, the Biological Response Modifiers (BRMs) most commonly used in a medical practice environment are plant lectins (Echinacea, mistletoe products), bacterial lysates (e.g. Arthrokelan®, Gynatren®) and organo-peptides (thymus, spleen, mesenchyme).
For only a few of these substances used for immunostimulation the efficacy has been firmly established in placebo-controlled clinical trials. However, this situation is partly due to the fact that financing studies of this type is almost impossible for already approved products (no longer patentable).
It is often overlooked that critics have reported only very limited data demonstrating the lack efficacy of these treatments.
Insights from published case reports about BRMs and numerous studies investigating the mechanisms of action of the products show the following:

  • An unspecific stimulation of lymphocytes by BRMs can be scientifically explained and measured in the lab.
  • However, the proportion of patients in whom a treatment effect can be demonstrated amounts only to 30-60% and varies with regard to substance class and even with the respective product.
  • Monotonous continuous administration of the same product does typically not achieve lasting immunostimulation as the immune system adapts.
  • Continued immunostimulation after achieving optimum (for this patient) immune function can result in “flipping“ into immunosuppression. This “flipping“ can be best explained by an increase in regulatory CD4 and CD8 lymphocytes.

Our Institute was involved in a study investigating the bystander effect of a treatment with mistletoe products. If you are interested we will send you a full-text copy of the paper.
This study showed that a positive result, i.e. a stimulation index >3 in response to an immunostimulant, indicates the presence of T cell reactivity against antigen structures in this product.

Thus it is at least very likely that an immostimulant which tested positive in the LTT induces an immune response in the body with every application and consequently triggers a cytokine response.
The cytokines released in the process, especially IL-2 and IFN-γ, act as endogenous immunostimulants.
This mechanism of action is based on the so-called bystander mechanism and has been verified in the meantime for many products used therapeutically. Not only for mistletoe lectins, but also for products made of killed bacterial pathogens, organ preparations and plant-based immunostimulants with higher-molecular ingredients.

The LTT Immune Stimulation includes the LTT Immune Function (left side of the results report) and tests up to 6 additional products (free choice).

To obtain a list of the immune products available at the lab for in-vitro testing, call Tel.: +49 30 77001-220 or visit here.

Please note: In contrast to this qualitative method, the cellular immune status which is based on a quantitative analysis of CD4, CD8 and NK cells is not a functional parameter and thus of only very limited use for monitoring immunostimulating treatments. This test can at best show long-term immunocompetence improvements.

What patient sampling material is required for the LTT Immune Stimulation?

The LTT Immune Stimulation is almost identical with the LTT Immune Function. The only difference is the additional testing of immunostimulants. As this does not require extra blood, the LTT Immune Function can be performed with 20 mL heparin blood and 5 mL whole blood.

For the LTT Immune Stimulation, please note the products to be tested on the request form (you can choose up to 6 products).

We can provide you with a list of all products available at our laboratory. Other products have to be sent in together with the blood samples (Storage in the laboratory for follow-up testing can be arrange over the phone).