1.4 Primary or Secondary Immune Deficiencies

Question 1

Primary Immune Deficiency

Answer 1

• Primary cause of immune deficiency

- Rare, inherited genetic disorders

Question 2

Secondary Immune Deficiencies

Answer 2

• Caused by a condition outside the immune system

Question 3

Primary Immune Deficiency Diseases (PIDD)

Answer 3

• Results from a defect in the immune system
• Rare and genetic
• Increased risk of having chronic debilitating infections such as Epstein-Barr Virus (EBV) that increase risk of cancer.
• HALLMARK SIGN IS RECURRENT INFECTIONS
• Many patients with PIDD also have autoimmune disorders (Rheumatoid Arthritis, Thyroid Disease, Inflammatory Bowel Disease)

MOST FREQUENT TYPE OF INFECTIONS
- Sinopulmonary Infections (Sinusitis, bronchitis, pneumonia) and otitis media (ear infection)

SEVERE COMBINED IMMUNODEFICIENCY (SCID)

• Group of disorders with defective T and B cell numbers and function
• Predisposes patients to infection with any pathogen

Question 4

Secondary Immunodeficiency Diseases

Answer 4

• Most commonly caused by aging, malnutrition, medications, or HIV

SCREENING TO RULE OUT PRIMARY IMMUNODEFICIENCY (PID)

• CBC
• Serum Immunoglobin Quantification
• Biochemistry Panel (Basic Liver and Kidney Function, Total Protein and Albumin)

Question 5

Transplantation and Immunosuppression

Answer 5

Patients must take the correct dosage of immunosuppressants when they receive a transplant

• Insufficient dose can cause organ rejection
• Excessive dose can cause organ failure (due to immunologic compromise)
• Excessive doses also allow opportunistic infections (cytomegalovirus, varicella-zoster) to invade and impede organ function
• Usually starts with a loading dose and then they change it to the smallest effective dose.

Question 6

Tissue and Organ Transplant

Answer 6

• Inadequate immunosuppressants (especially with solid organs) can cause graft vs host disease with lymphoid-rich organs (produces a lot of lymphocytes) like bone marrow or stem cells.
• Liver transplant can also cause GVHD because it is a lymphoid rich tissue.

Question 7

Immune Response

Answer 7

• Third line of defense (specific)
• When organs get transplanted into a body, the body recognizes it as foreign and tries to reject it or kill it. Immunosuppression is designed to stop this from happening.

Question 8

Organ Rejection Medications

Answer 8

• imus - Immunosuppressant (Tacrolimus and Sirolimus)
• cept - Receptor modules that reduce strength of bodies immune system (Cellcept, Belatacept)
• mab - Monoclonal antibodies target and attach to cells (antigens) created by rejection activity of leukocytes (rituximab, adalimumab)

Question 9

Immunosuppressants

Answer 9

Induction Phase - Period of time between when the organ is transplanted until the second week of transplantation.
- Immunosuppressants are usually started in the OR. After the medication has been started, they level out dosage to a stable dose, then implement a maintenance dose

Maintenance Regime - Starts around 3 months after transplant and lasts for a lifetime
- Maintenance dose is the lowest effective dose of medication

• THIS CAN ALSO BE USED TO TREAT ORGAN REJETION

Question 10

Triple Therapy

Answer 10

• THE MOST EFFECTIVE IMMUNOSUPPRESSANT REGIME

This is the usage of 3 different immunosuppressant classes to promote optimal function of transplanted organ

• Corticosteroids
• Antimetabolites
• Calcineurin Inhibitors (CNIs)

Question 11

Corticosteroids

Answer 11

• Maintenance therapy standard
• Suppresses immune system and inflammation
• Blocks Interleukin-1 which suppresses activation/growth of T-cells and decreases formation of antibodies by B-cells

Acute Phases - IV Methylprednisolone
Oral Route - Prednisone

• They are metabolized in the liver and excreted in the kidneys
• CAUTION FOR PATIENTS WITH LIVER TRANSPLANTS

Question 12

Antimetabolites

Answer 12

• Antiproliferative Drugs (Used for Maintenance)
• Inhibit proliferation of B-cells and T-cells
• When cells ingest these they are unable to divide. They attack cells at specific phases in the cycle and are classified by when in the cycle they interfere.

Azathioprine
Mycophenolic Acid
Cyclophosphamide

• Metabolized in Liver, Excreted by Kidneys

Question 13

Calcineurin Inhibitors (CNIs)

Answer 13

• Inhibit proliferation of Helper T-cells and how cytokines express themselves

TWO MOST COMMON TYPES (REVIEW THESE MEDICATIONS)

• Cyclosporine (nephrotoxic)
• Tacrolimus (nephrotoxic)
• Dosage depends on when patient was transplanted, history of rejection, present infections.

BIGGEST ISSUE IS THEY CAN RESULT IN CHRONIC NEPHROTOXICITY

• GRAPEFRUIT JUICE INCREASES ABSORPTION OF CYCLOSPORINE AND TACROLIMUS

Question 14

Mammalian Target of Rapamycin (mTOR) Inhibitor

Answer 14

• Sirolimus (Rapamycin)
• Suppresses T-cell Activation/Proliferation
• Used with low-dose CNIs for organ rejection
• Lowers risk of nephrotoxicity, viral infections and malignancies of CNIs
• Triple shift is aiming at getting rid of antimetabolites and adding mTOR

Question 15

Acute Organ Rejection

Answer 15

Acute Reaction
- Occurs 10 days to few months post-transplant OR if immunosuppressant medication are stopped.

CHARACTERISTICS

• Signs of organ failure
• Vasculitis lesions (lesions of small vessels) which leads to arterial narrowing/obliteration. They narrow to the point where there is no more blood flow going through them.

EXAMPLES
Kidney Transplant - Look at GFR and creatinine to check for organ failure
Liver Transplant - Look at liver function tests.

Question 16

Chronic Organ Transplant

Answer 16

• Organ works fine for months to years

Characteristics

• Progressive failure of transplanted organ (gradual)
• Fibrosis or Hardening of vessels
• Checked with periodic biopsy of transplanted organ looking for signs of fibrosis. Looking to make sure the organ is not deteriorating too rapidly.

Question 17

Managing Transplant Medications

Answer 17

• Patients may take 10-15 medications daily
• Trough levels of medication must be drawn to help maintain optimal function
• MONITOR PATIENT FOR BONE MARROW SUPPRESSION WHICH CAN INCREASE PATIENT RISK OF INFECTION OR BLEEDING (Neutropenia, Thrombocytopenia, Anemia)

Question 18

Monoclonal Antibodies

Answer 18

• Mimics response of antibodies produced in the body
• Lab-made antibodies to react to certain proteins
• Targets specific protein present on T-Cell and B-Cell surfaces
  (Binds to target epitopes of the cell surface where they exert their immunomodulatory effects.

Basiliximab and Daclizumab - Act on IgG (Interleukin-2 Receptor Antagonist)
(Inhibits lymphocyte proliferation and cytokine production)

Question 19

Muromonab-CD3 (Monoclonal Antibody)

Answer 19

• Acts against and blocks CD3 Receptor on surfaces of T-cells (essential for T-cell activation)

Question 20

Medications

Answer 20

Antigen Presenting Cell -> Interleukin 1 -> T-Helper Cell -> Interleukin 2 -> Cytotoxic T Cells and B Cells.

• Glucocorticoids block antigen presenting and interleukin 1 presenting
• Muromonab-CD3 blocks receptors on helper T-cells which prevents T-cell activation
• Cyclosporine/Tacrolimus blocks interleukin 2 production
• Basiliximab/Declizumab - Blocks interleukin 2 receptors (which prevents cytotoxic cell production)
• Sirolimus/Everolimus - Blocks enzymes in cell growth cycle (blocks cytotoxic cell proliferation)
• Glucocorticoids/Mycophenolic Acid/Azathioprine/Methotrexate Leflunomide - Blocks T/B Cell Proliferation