Objectives
— Definition
— Primary Immunodeficiencies
- —Characteristics—Types of primary immunodeficiency disorders—Mode of inheritance—Diagnosis and Treatment
—
Secondary Immunodeficiency
- —Human Immunodeficiency Virus—Transmission
- —Therapy and prevention of AIDS
Immunodeficiency
Defect in 1 or more components of immune
system
Types:
—
Primary or Congenital:
- —Born with the immunodeficiency—Inherited (Mutation in gene controlling immune cells)—Susceptible to recurrent, severe infection; starting in children—Cannot recover without treatment—>125 immunodeficiency disorders
—
Secondary or Acquired: As a consequence of other diseases or environmental factors
(e.g.
infection, malignancy, aging, starvation, medication, drugs) – Human Immunodeficiency
Virus
Hematopoiesis
Hematopoietic Stem Cell (HSC) deficiency
- —HSC are multipotent (differentiate into all blood cell types)—Self renewing cells—Lineage negative (mature B/T cell, granulocyte, Mf markers absent)—CD34+, c-Kit+, Stem cell Ag (Sca-1+) on cell surface—Defect in HSC results in Reticular Dysgenesis—Affects development of all leukocytes—Patients are susceptible to all infections (bacterial, viral, parasitic and fungal)—Fatal without treatment—Treated with bone marrow or HSC transplantation
Allogeneic BM/HSC Transplantation
Myeloid Progenitor Cell Differentiation
Defect
- —Myeloid Progenitor Cells develop into neutrophils and monocytes—Defect in differentiation from myeloid progenitor cells into neutrophils results inCongenital Agranulocytosis—Recurrent bacterial infections seen in patients
- —Treated with granulocyte-macrophage colony stimulating factor (GM-CSF) or G-CSF
Defective Neutrophils
- Patients have neutrophils that are defective in production of reactive oxygen species that is
responsible for
killing of phagocytosed microrganisms.
- —Nitroblue tetrazolium test: reduction by superoxide (-ve)
- —This results in accumulation of granulocytes, Mf and T cells forming granulomas. These patients suffer from
Chronic
Granulomatous Disease.
- Have recurrent bacterial infections
- Commensals become pathogenic
- —X-linked or autosomal recessive
- —Treated with IFN-g against infections
Inheritance
- 22 pairs of autosomes and 1 pair of sex chromosomes (X and Y)
- —Autosomal recessive (most AA normal; Aa carrier; aa affected)
- —Autosomal dominant (Aa affected; aa is normal)
- —X-linked (XX carrier daughter; XY affected son)
Carrier x Carrier
Mother Father
Aa Aa
| M | A | a |
|---|---|---|
| F | ||
| A | AA | Aa |
| Normal | Carrier | |
| a | Aa | aa |
| Carrier | Affected |
Autosomal Recessive
Normal x Affected
Mother Father
aa Aa
| M | A | a |
|---|---|---|
| F | ||
| a | Aa | aa |
| Affected | Normal | |
| a | Aa | aa |
| Affected | Normal |
Autosomal Dominant
Normal x Affected
Mother Father
Xx XY
| M | X | Y |
|---|---|---|
| F | ||
| X | XX | XY |
| Normal | Normal | |
| x | Xx | xY |
| Carrier | Affected |
X-linked
- Adhesion molecule (e.g.CD18) may be lacking on T cells and monocytes.
- Autosomal recessive
- Results in defective extravasation
- Recurrent infections
- Impaired wound healing Treated with BM (depleted of T cells and HLA matched) transplantation or with gene therapy
Defect in Lymphoid Progenitor
- —Results in Severe Combined Immunodeficiency (SCID)
- —Lack T, B and/or NK cells
- —Thymus does not develop
- —Myeloid and erythroid cells are normal.
- —Generally lethal
- —Susceptible to bacterial, viral and fungal infections.
- —In infants, passively transferred maternal Abs are present.
- —Live attenuated vaccines (e.g. Sabin polio) can cause disease.
Types of SCID
—RAG-1/2 (Recombinase activating gene)
deficiency: Required for TCR and Ig
gene rearrangement
IL-2R gene defect
ADA
Adenosine deaminase (ADA) deficiency Adenosine-------->Inosine------>Uric acid T, B and NK cell
deficiency due to toxicity of accumulated metabolites
First successful gene
therapy done in patient
DiGeorge syndrome
Precursor
T cell differentiation defect
- Athymic - DiGeorge Syndrome
- Lack of T helper (Th) cells , Cytotoxic T cells (CTL) and T regulatory (Treg) cells
- —B cells are present but T-dependent B cell responses are defective
- —Anti-viral and anti-fungal immunity impaired
- —Developmental defect in the 3rd and 4th pharyngeal pouch
- Results in facial defect and congenital heart disease
- —Treated with thymic transplant
- Autosomal dominant trait
Nude
Athymic mouse
nu/nu gene (autosomal recessive)
Hairless
Should be maintained
in pathogen-free environment
T helper cell defect
Results in impaired cytotoxic T cell activity and Th-dependent B cell
responses due to Th cell defect
Accept xenografts
X-linked Agammaglobulinemia (x-LA)
—Absence of Igs and B cells
—Arrest at Pre-B cell
stage (H-chain rearranged not L chain)
Hyper IgM Syndrome
—Deficiency in IgG, IgA and IgE
—Increased IgM in serum
—B cells express IgD and IgM on membrane
—X-linked
Selective Ig class deficiency
—e.g. IgA deficiency
—Due to defect in isotype switching
—Recurrent
respiratory, gastrointestinal and/or genitourinary infection
Common
Variable Immunodeficiency
—B cells are normal
—Defect in maturation
to plasma cells
—Decreased IgM, IgG and IgA or only IgG and IgA
—Susceptible to
bacterial (e.g. pneumococci) infections
—Low Ab titers against DPT
or MMR Vaccines
—Usually not detected
in children because of maternal Abs
—Also called Late-onset hypogammaglobulinemia, Adult-onset
agammaglobulinemia or Acquired agammaglobulinemia
—Ig replacement therapy
and antibiotics
Other
Immunodeficiencies
—Bare lymphocyte
syndrome:
Lack MHC class II on
B cells, macrophages and dendritic cells
—Complement Deficiency
Primary
Immunodeficiencies
Adaptive
Immunity Deficiency
—T cell deficiency
—Susceptible to intracellular bacterial infection e.g. Salmonella typhi, Mycobacteria
— Susceptible to viral, parasitic and fungal infection
—B cell deficiency
—Susceptible to extracellular bacterial infection e.g.
Staphylococcal infection
Secondary or Acquired Immunodeficiencies
—Agent-induced
immunodeficiency: e.g. infections, metaboic disturbance, trauma, corticosteroids,
cyclosporin A, radiation,
chemotherapy
—HIV
Human
Immunodeficiency Virus
—Discovered in 1983 by
Luc Montagnier and Robert Gallo
—Retrovirus (RNA
virus)
—HIV-1 (common) and
HIV-2 (Africa)
—Patients with low CD4+ T
cells
—Virus prevalent in
homosexual, promiscuous heterosexual, i.v. drug users, transfusion, infants born to infected
mothers
—Opportunistic
infections with Pnuemocystis carinii, Candida albicans, Mycobacterium avium, etc.
—Patients with HIV
have high incidence of cancers such as Kaposi sarcoma
Kaposi
Sarcoma
Incidence
of HIV
Course
of AIDS
Structure of HIV
—Virus grows intracellularly
—Abs develop after ~3
weeks.
—Thus cannot be used
as a diagnostic test initially (Reverse transcriptase is a sensitive test)
—Abs are not
neutralizing
Role
of T cells in development of AIDS
—Initially Th cells control viral
load
—Cytopathic virus
—Syncitium formation with
infected/uninfected cells
—Surviving Th cells are anergic
—Destruction of
infected Th cells by CTL
—CTL that develop are
ineffective because of high viral mutations
—Lack of Th affects CTL
activation
—Resistance to CTL by downregulation of class I MHC on
target cells
Animal
Models
—Primate Model:
—HIV grows in chimpanzees but do not develop AIDS
—Simian immunodeficiency virus (SIVagm in African green
monkey – no disease; SIVmac in
Macaques – AIDS
like);
—Feline
immunodeficiency virus (FIV)
—Mouse Model:
—Grows in Severe Combined Immunodeficiency (SCID) mice
reconstituted with human lymphocytes
Viral Replication
Coreceptors of HIV
—Chemokine receptors
—T cell-tropic (Syncitium-inducing; X4 virus strain)
 |
| CXCR4 : Ligand is SDF1 (Stromal cell derived factor) |
—Macrophage-tropic (Nonsyncitium-inducing; R5 virus strain)
 |
| CCR5 : Ligands are RANTES (Regulated on activation, normal T cell expressed and secreted), MIP1a, MIP1b (Macrophage Inflammatory Protein); |
Therapy
—Inhibit binding of
gp120 with CD4 by
—Use of soluble CD4
—Use of anti-CD4 Abs
— Use of anti-gp120
—Inhibit binding of
HIV to coreceptors by chemokines such as RANTES
Host
Factors influencing course
—Transmission of HIV
—Sexual contact
—Breast feeding
—Transfusion
—During birth
—Sharing needles
—Resistance to HIV in
individuals
—CCR5D32
—Some HLA types
(HLA-A2) are resistant while others (HLA-B35) are susceptible)
Therapeutic
targets
Treatment
and Prevention
—Highly active
anti-retroviral therapy (HAART; combination therapy) + IL-2 (to reconstitute
the immune system)
—Vaccines: Proteins,
DNA, subunit and recombinant virus (SIV-HIV chimeric virus)
Problems
with therapy
—HIV-1 infection gives rise to AIDS despite the presence
of Abs
—Low immunogenicity of virus
—Vaccine alone leads to destruction of CD4+ T
cells
—Integration of virus in host genome
—Virus undergoes mutations
—High rate of virus replication (109
viruses/day)
—Live attenuated may result in AIDS
—Heat killed organism is not antigenic
—Vaccine administered through oral or respiratory route
(Route of exposure to HIV is through genital tract)
—Lack of animal models and in vitro testing system
—Drugs do not cross blood-brain barrier to reach virus in
brain
Summary
—Primary immunodeficiencies are inherited
—They can affect
hematopoietic stem cells, lymphoid or myeloid cells.
—Secondary immunodeficiencies are due to
infections, aging, cancer or chemical exposure
—HIV affects immune
system by eliminating CD4+ T cells
—Vaccine development
has been hindered by lack of an experimental model, antigenic variation, rapid
proliferation of the virus
Reading
—Immunology
By Male, Brostoff, Roth and Roitt
7th
Edition
Pages299-324
