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DEVELOPMENT OF IMMUNE SYSTEM
• - GESTATIONAL TOLERANCE• (PREVENTING REJECTION)
• - FETAL/NEONATAL PROTECTION
• - VACCINATION/IMMUNIZATION
VACCINATIONS
• BIRTH BCG (BACILLUS CALMETTE-GUERIN)• ORAL POLIO• HEPATITIS
• 6 WEEKS• DPT (DIPHTHERIA, TETANUS, PERTUSSIS• ORAL POLIO 2ND DOSE• HEPATITIS 2ND
• 10 WEEKS• DPT (DIPHTHERIA, TETANUS, PERTUSSIS)• ORAL POLIO 3RD
• 14 WEEKS• DPT 3RD
• ORAL POLIO 4TH
• 6-9 MONTHS• ORAL POLIO 5TH
• HEPATITIS B
• 9 MONTHS• MEASLES
• 15-18 MONTHS• MMR (MEASLES, MUMPS, RUBELLA)• DPT booster dose• ORAL POLIO 6TH
• 5 YEARS• DPT 2ND booster• ORAL POLIO 7TH
• 10 YEARS• TT (TETANUS) 3RD booster• HEPATITIS B booster • 15-16 YEARS• TETANUS booster
** Taken from the Scientist;17(2004)
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Progression of Vaccine Development **
Function of Immune System is PROTECTION against:
1. Bacteria2. Virus3. Fungus/ multicellular parasites4. Cancer5. Toxins 6. ( 5,000 daltons--protein/lipid/CHO/nucleic
acids)
Tissues and Organs Important for Immune Function
•Cells derived from stem cells: liver, bone marrow
• Cells are stored, multiply, interact, and mature in: thymus, spleen, lymph nodes, blood
•Transport: lymphatic vessels
Accessory Organs
•Appendix, tonsils, intestines
Cell Types1. Lymphocytes: derived in bone marrow from
stem cells include both T cells and B cells. 1012
A) T cells: stored & mature in thymus-migrate throughout the body
-Killer Cells Perform lysis (infected cells)Cell mediated immune response
-Helper CellsEnhance T killer or B cell activity
-Suppressor CellsReduce/suppress immune activityMay help prevent auto immune
disease
Lymphocytes (cont.)
B)B-Cells: stored and mature in spleen
• secrete highly specific Ab to bind foreign substance (antigen: Ag), form Ab-Ag complex
• responsible for humoral response• perform antigen processing and
presentation• differentiate into plasma cells (large Ab
secretion)
Lymphocytes (cont.)
2. Neutrophils- found throughout body, in blood-phagocytosis of Ab-Ag CX
3. Macrophages- throughout body, blood, lymphatics-phagocytose non-specifically (non Ab coated Ag)-phagocytose specifically Ab-Ag CX-have large number of lysosomes (degradative enzyme)-perform Ag processing and presentation-present Ag to T helper cell-secrete lymphokines/ cytokines to stimulate T helper
cells and immune activity
4. Natural Killer Cells-in blood throughout body-destroy cancer cells-stimulated by interferons
Bacterial Infection
Macrophage
Bacteria
ComplementSeries of enzymes which are sequentially
activated and result in lysis of cell membrane of infected cell at bacterium
Permeabilizes membrane leaky
Complement binding and activation
~35 enzymes and factors involved in cascade
CDC involves: 1) recognition, 2) attachment of complement-fixing antibodies to tumor specific surface antigens, 3) complement activation, 4) formation of MAC resulting in transmembrane pores (perforins) that disrupt the osmotic barrier of the membrane and lead to osmotic lysis.
5 classes of IgIgG: 150,000 m.w.
most abundant in blood, cross placental barrier,fix complement, induce macrophage engulfment
IgA: associated with mucus and secretory glands, respiratory tract, intestines, saliva, tears, milk
variable size
IgM: 900,000 m.w.2nd most abundant , fix complement,induce macrophage engulfment, primary
immune response
5 Classes of Ig
IgD: Low level in blood, surface receptor on B- cell
IgE: Binds receptor on mast cells (basophils)secretes histamine, role in allergic reactions
Increased histamine leads to vasodilation, which leads to increase blood vessel permeability. This induces lymphocyte immigration swelling and redness.
Thymus Involution
Repertoire of lymphocytes shift with aging (membrane components shift)
ORGAN AND T-CELL DEVELOPMENT
• YOLK SAC
• LIVER• (4 Weeks)
• BONE MARROW• (4-5 Weeks )
• THYMUS• (7-10 Weeks)
• BLOOD LYMPH• (14 Weeks)
• SPLEEN
• (16 Weeks)
• T-cells migrate and appear in tissues with development and increase in number
throughout Gestation
B-CELLS
• FIRST appear in immature state - Liver at 7 weeks
• LATER –appear mature by 14-20 weeks
• CAN DIFFERENTIATE INTO IMMUNOLOGICALLY COMPETENT ANTIBODY-PRODUCING PLASMA CELLS
NATURAL KILLER CELLS • FIRST APPEAR IN FETAL BONE MARROW AROUND 13
WEEKS GESTATION• FOUND THROUGHOUT BODY • NK CELLS HAVE DIMINISHED ACTIVITY BEFORE BIRTH
COMPARED TO ADULT • STIMULATED BY INTERFERON AFTER 27 WEEKS
COMPLEMENT PROTEINS • ARISE FROM LIVER • FIRST DETECTED 5-6 WEEKS GESTATION • INCREASE GRADUALLY IN CONCENTRATION • AT ABOUT 28 WEEKS COMPLEMENT PROTEINS ARE AROUND
2/3 THAT OF ADULT CONCENTRATIONS • INDIVIDUAL VARIATION
SEVERE COMBINED IMMUNODEFICIENCY DISEASE (SCID)
CHARACTERISTICS:
GENERALLY CAUSED BY DEFECT OF SINGLE GENE NEEDED FOR T-CELL AND B-CELL FUNCTION
—SUBJECT EXHIBITS NO CELL MEDIATED RESPONSE
––SUBJECT CANNOT MAKE ANTIBODIES
ABOUT 25% OF CASES INVOLVES DEFECTIVE GENE FOR THE ENZYME ADENOSINE DEAMINASE
(REQUIRED FOR PURINE BREAKDOWN)
SEVERE COMBINED IMMUNODEFICIENCY DISEASE (SCID)
• TREATMENT OPTIONS:
• GERM FREE ENVIRONMENT• BONE MARROW TRANSPLANT• ROUTINE INJECTIONS OF ADENOSINE DEAMINASE ENZYME (ADA)
• GENE THERAPY USING SUBJECTS OWN CELLS• (RETROVIRUS CONTAINING ADA TO “INFECT” • SUBJECTS BONE MARROW STEM CELLS)
Agents Which Affect the Agents Which Affect the Immune ResponseImmune Response
Rheumatoid ArthritisRheumatoid ArthritisDisease that leads to
inflammation of the joints and surrounding tissues
Can affect organsThe immune system
confuses healthy tissue with foreign and begins to attack itself
Occurs at any age, usually affects women more than men
Affects joints on both sides equally◦ Wrists, fingers, knees, feet,
ankles
http://www.scienceclarified.com/images/uesc_01_img0050.jpg
Systemic Lupus Systemic Lupus ErythematosusErythematosus
Autoimmune diseaseSymptoms:
◦ Chest pain, fatigue, fever, general discomfort, hair loss, mouth sores, sensitivity to sunlight, skin rash, swollen lymph nodes, arrhythmias, blood in urine, abdominal pain, coughing up blood, patchy skin colors
Other form: lupus nephrititis◦ Can cause kidney failure
and lead to dialysis
http://www.taconichills.k12.ny.us/webquests/noncomdisease/lupuspic.jpg
Other Immunological Other Immunological DiseasesDiseases
• Type I diabetes mellitus• Multiple sclerosis• Asthma• Allergies• SCID
Treatment StrategiesTreatment Strategies
1. Immunosuppression – involves downregulating immune system activity
2. Tolerance – the idea that a body can be taught not to reject somthing
3. Immunostimulation – involves upregulating immune system activity
4. Immunization – active or passive
Immunosuppression – Immunosuppression – GlucocorticoidsGlucocorticoids
• Usually co-administered with other suppressive agents to treat auto-immune disorders or treatment of transplant rejection
• Exact mechanism not elucidated• Very broad anti-inflammatory effects• Downregulate IL-1 and IL-6• Cause apoptosis in activated cells
Immunosuppression – Immunosuppression – GlucocorticoidsGlucocorticoids
• Side Effects– Toxic– Causes increased infection risk– Poor wound healing– Hyperglycemia– Hypertension
http://img.medscape.com/article/588/548/588548-fig3.jpg
Immunosuppression – Immunosuppression – GlucocorticoidsGlucocorticoids
Prednisone
Dexamethasone
Cortisol
Immunosuppression – Immunosuppression – Calcineurin InhibitorsCalcineurin Inhibitors
– Calcineurin – protein phosphatase that activates T Cells by dephosphorylating transcription factors, including NFAT (nuclear factor of activated T cells).
– Blocks T Cell proliferation• Decreased immune response
Immunosuppression – Immunosuppression – Calcineurin InhibitorsCalcineurin Inhibitors
Tacrolimusa.k.a. FK-506
Cyclosporin A
http://drtedwilliams.net/cop/753/753CalcineurinInhibitors.GIF
Immunosuppression – Immunosuppression – Anti-proliferative and Anti-Metabolic Anti-proliferative and Anti-Metabolic
DrugsDrugs– Azathioprine
• Purine anti-metabolite
Tioguanine
Azathioprine Mercaptopurine
Guanine
Immunosuppression – Immunosuppression – Anti-proliferative and Anti-Metabolic Anti-proliferative and Anti-Metabolic
DrugsDrugs– Mycophenolate Mofentil (CellCept®)– Hydrolyzed to mycophenolic acid
• IMPDH inhibitor (inosine monophosphate dehydrogenase enzyme
• Important in biosynthesis of guanine• Good alternative to azathioprine when
toxicity is an issue
Mycophenolic acid
Immunosuppression – Immunosuppression – Monoclonal AntibodiesMonoclonal Antibodies
http://www.facetbiotech.com/images/moa_illustrations/FACET_MoA_ELOTUZUMAB.jpg
ToleranceTolerance
• Strategy is to induce and maintain tolerance
• Useful strategy for organ transplantation• Very much the target of research today• Would represent a true cure for
autoimmune conditions without side effects of immunosuppressive agents
• “Holy Grail” of immunomodulation
ImmunizationImmunization
• Active or passive– Active – stimulation with antigen to develop
antigens for future prevention– Passive – administration of antibodies to
individual already exposed or about to be exposed to antigens
• Vaccines – active; administration whole, killed organism, live organism, or specific peptide from organism
• Immune Globulin – used in passive immunization; used in individuals deficient in antibodies
Genes• Are carried on a chromosome
• The basic unit of heredity
• Encode how to make a protein– DNARNA proteins
• Proteins carry out most of life’s function.
• When altered causes dysfunction of a protein
• When there is a mutation in the gene, then it will change the codon, which will change which amino acid is called for which will change the conformation of the protein which will change the function of the protein. Genetic disorders result from mutations in the genome.
Picture of a Chromosome
http://www.accessexcellence.org/RC/VL/GG/genes.html
What is Gene Therapy
• It is a technique for correcting defective genes that are responsible for disease development
• There are four approaches:1. A normal gene inserted to compensate for a
nonfunctional gene.2. An abnormal gene traded for a normal gene3. An abnormal gene repaired through selective
reverse mutation4. Change the regulation of gene pairs
The Beginning…
• In the 1980s, Scientists began to look into gene therapy.– They would insert human genes into a bacteria
cell.– Then the bacteria cell would transcribe and
translate the information into a protein– Then they would introduce the protein into
human cells
The First Case• The first gene therapy was
performed on September 14th, 1990– Ashanti DeSilva was treated for
SCID• Sever combined immunodeficiency
– Doctors removed her white blood cells, inserted the missing gene into the WBC, and then put them back into her blood stream.
– This strengthened her immune system
– Only worked for a few months
How It Works
• A vector delivers the therapeutic gene into a patient’s target cell
• The target cells become infected with the viral vector
• The vector’s genetic material is inserted into the target cell
• Functional proteins are created from the therapeutic gene causing the cell to return to a normal state
Principle
http://encarta.msn.com/media_461561269/Gene_Therapy.html
Viruses
• Replicate by inserting their DNA into a host cell
• Gene therapy can use this to insert genes that encode for a desired protein to create the desired trait
• Four different types
Retroviruses• Created double stranded DNA copies from RNA
genome– The retrovirus goes through reverse
transcription using reverse transcriptase and RNA
– the double stranded viral genome integrates into the human genome using integrase• integrase inserts the gene anywhere
because it has no specific site• May cause insertional mutagenesis
– One gene disrupts another gene’s code (disrupted cell division causes cancer from uncontrolled cell division)
– vectors used are derived from the human immunodeficiency virus (HIV) and are being evaluated for safety
Adenoviruses
• Are double stranded DNA genome that cause respiratory, intestinal, and eye infections in humans
• The inserted DNA is not incorporate into genome
• Not replicated though– Has to be reinserted when more cells divide
• Ex. Common cold
Adenovirus cont.
http://en.wikipedia.org/wiki/Gene_therapy
Adeno-associated Viruses• Adeno-associated Virus- small, single stranded DNA that insert genetic material at a
specific point on chromosome 19• From parvovirus family- causes no known disease and doesn't trigger patient
immune response. • Low information capacity• gene is always "on" so the protein is always being expressed, possibly even in
instances when it isn't needed.• hemophilia treatments, for example, a gene-carrying vector could be injected into a
muscle, prompting the muscle cells to produce Factor IX and thus prevent bleeding.– Study by Wilson and Kathy High (University of Pennsylvania), patients have not
needed Factor IX injections for more than a year
Herpes Simplex Viruses
• Double stranded DNA viruses that infect neurons
• Ex. Herpes simplex virus type 1
http://www.ucmp.berkeley.edu/alllife/virus.html
Non-viral Options• Direct introduction of therapeutic DNA
– But only with certain tissue– Requires a lot of DNA
• Creation of artificial lipid sphere with aqueous core, liposome– Carries therapeutic DNA through membrane
• Chemically linking DNA to molecule that will bind to special cell receptors
– DNA is engulfed by cell membrane– Less effective
• Trying to introduce a 47th chromosome– Exist alongside the 46 others– Could carry a lot of information– But how to get the big molecule through membranes?
Current Status• FDA hasn’t approved any human gene therapy
product for saleReasons:• In 1999, 18-year-old Jesse Gelsinger died
from multiple organ failure 4 days after treatment for omithine transcarboxylase deficiency.– Death was triggered by severe immune
response to adenovirus carrier • January 2003, halt to using retrovirus vectors
in blood stem cells because children developed leukemia-like condition after successful treatment for X-linked severe combined immunodeficiency disease
Problems with Gene Therapy• Short Lived
– Hard to rapidly integrate therapeutic DNA into genome and rapidly dividing nature of cells prevent gene therapy from long time
– Would have to have multiple rounds of therapy• Immune Response
– new things introduced leads to immune response– increased response when a repeat offender enters
• Viral Vectors– patient could have toxic, immune, inflammatory response– also may cause disease once inside
• Multigene Disorders– Heart disease, high blood pressure, Alzheimer’s, arthritis and diabetes are
hard to treat because you need to introduce more than one gene• May induce a tumor if integrated in a tumor suppressor gene because
insertional mutagenesis
Unsuccessful Gene therapies• Jesse Gelsinger, a gene therapy patient who lacked ornithine
transcarbamylase activity, died in 1999.
• Within hours after doctors shot the normal OTC gene attached to a therapeutic virus into his liver, Jesse developed a high fever. His immune system began raging out of control, his blood began clotting, ammonia levels climbed, his liver hemorrhaged and a flood of white blood cells shut down his lungs.
• One problem with gene therapy is that one does not have control over where the gene will be inserted into the genome. The location of a gene in the genome is of importance for the degree of expression of the gene and for the regulation of the gene (the so-called "position effect"), and thus the gene regulatory aspects are always uncertain after gene therapy
Successful Gene Therapy for Severe Combine Immunodeficiency
• Infants with severe combined immunodeficiency are unable to mount an adaptive immune response, because they have a profound deficiency of lymphocytes.
• severe combined immunodeficiency is inherited as an X-linked recessive disease, which for all practical purposes affects only boys.
• In the other half of the patients with severe combined immunodeficiency, the inheritance is autosomal recessive — and there are several abnormalities in the immune system when the defective gene is encoded on an autosome.
Severe Combine Immunodeficiency Continued
• A previous attempt at gene therapy for immunodeficiency was successful in children with severe combined immunodeficiency due to a deficiency of adenosine deaminase.
• In these patients, peripheral T cells were transduced with a vector bearing the gene for adenosine deaminase.
• The experiment was extremely labor intensive, because mature peripheral-blood T cells were modified rather than stem cells, and the procedure therefore had to be repeated many times to achieve success.
Successful One Year Gene Therapy Trial For Parkinson's Disease
• Neurologix a biotech company announced that they have successfully completed its landmark Phase I trial of gene therapy for Parkinson's Disease.
• This was a 12 patient study with four patients in each of three dose escalating cohorts. All procedures were performed under local anesthesia and all 12 patients were discharged from the hospital within 48 hours of the procedure, and followed for 12 months.
• Primary outcomes of the study design, safety and tolerability, were successfully met. There were no adverse events reported relating to the treatment.
Parkinson's Disease Cont.• The gene transfer procedure
utilized the AAV (adeno-associated virus) vector, a virus that has been used safely in a variety of clinical gene therapy trials, and the vehicle that will be used in all of the company's first generation products, including epilepsy and Huntington's disease. In its Parkinson's disease trial, Neurologix used its gene transfer technology.
Recent DevelopmentsRecent Developments
• Genes get into brain using liposomes coated in polymer call polyethylene glycol– potential for treating Parkinson’s disease
• RNA interference or gene silencing to treat Huntington’s– siRNAs used to degrade RNA of particular sequence– abnormal protein wont be produced
• Create tiny liposomes that can carry therapeutic DNA through pores of nuclear membrane
• Sickle cell successfully treated in mice
http://www.wellesley.edu/Biology/Courses/219/Gen_news/i3_Gene_Therapy.jpg
VIRAL VECTORS IN GENE THERAPYVIRAL VECTORS IN GENE THERAPY
Gene TherapyGene TherapyThe introduction of nucleic acids into cells for the purpose of altering the course of medical condition or disease. AdministrationAdministration
• ex vivo- cells removed, genetically modified, transplanted back into a patient
• in vivo- direct transfer of genetic material into patient
The Ideal Vector for Gene TransferThe Ideal Vector for Gene Transfer• High concentration of virus allowing many cells to be infected or transducedHigh concentration of virus allowing many cells to be infected or transduced
• Convenience and reproducibility of productionConvenience and reproducibility of production
• Ability to transduce dividing and non-dividing cellsAbility to transduce dividing and non-dividing cells
• Ability to integrate into a site-specific location in the host chromosome, or to be Ability to integrate into a site-specific location in the host chromosome, or to be successfully maintained as stable episomesuccessfully maintained as stable episome
• A transcriptional unit that can respond to manipulation of its regulatory elementsA transcriptional unit that can respond to manipulation of its regulatory elements
• Ability to target the desired type of cellAbility to target the desired type of cell
• No components that elicit an immune responseNo components that elicit an immune response
Introduction of Genes Into AnimalsIntroduction of Genes Into Animals
METHODS METHODS MAJOR LIMITATIONS MAJOR LIMITATIONS
Calcium PhosphateCalcium Phosphate
DEAE DextranDEAE Dextran Low EfficiencyLow Efficiency
Cationic Lipids, LiposomesCationic Lipids, Liposomes
Direct DNA InjectionsDirect DNA Injections Low EfficiencyLow Efficiency
ElectroporationElectroporation Transient expressionTransient expression
Introduction of Genes Into AnimalsIntroduction of Genes Into Animals
VIRAL VECTORSVIRAL VECTORS MAJOR LIMITATIONSMAJOR LIMITATIONS
Papova (SV40, Polyoma) Size; Host range
Papilloma (BPV) Size; Integration, Transformation
Adeno associated (AAV) Size; production
Adeno Size; antigenicity, episomal DNA, toxicity
Herpes/Vaccinia Pathogenic, cytotoxic, lytic
Retroviruses Inability to infect post-mitotic cells
Lentiviruses Safety, integration
Genetic DiseasesGenetic Diseases
Cystic FibrosisCystic Fibrosis
Blood DisordersBlood Disorders
Muscular DystrophyMuscular Dystrophy
DiabetesDiabetes
Acquired DiseasesAcquired Diseases
CancerCancer
CardiovascularCardiovascular
Neurological DisordersNeurological Disorders
Infectious Disease (AIDS)Infectious Disease (AIDS)
Genetic Defects that are Candidates for Gene Therapy
Recombinant Vaccinia virus Expression Vector:
Construction of an infectious vaccinia virus expressing the influenza virus HA gene
Adenoviral vectors:Advantages:
Higher titer
Efficient transduction of nondividing cells
in vitro and in vivo
Disadvantages:
Toxicity
Immunological response
Prior exposure
Adenovirus particle structure:Adenovirus particle structure:
• Nonenveloped particle
• Contains linear double stranded DNA
• Does not integrate into the host genome
• Replicates as an episomal element in the nucleus
Adenoviral vectors:Adenoviral vectors:• Double-stranded DNA viruses, usually cause benign respiratory disease; serotypes 2 and 5 are used as vectors.
• Can infect dividing and non-dividing cells, can be produced at high titers.
• Replication-deficient adenovirus vectors can be generated by replacing the E1 or E3 gene, which is essential for replication.
• The recombinant vectors are then replicated in cells that express the products of the E1 or E3 gene and can be generated in very high concentrations.
• Cells infected with recombinant adenovirus can express the therapeutic gene, but because essential genes for replication are deleted, the vector can’t replicate.
• Adenoviral vectors can infect cells in vivo, causing them to express high levels of the transgene. However, expression lasts for only a short time (5-10 days post-infection).
• Immune response is the reason behind the short-term expression.
• Immune reaction is potent, eliciting both the cell-killing “cellular” response and the antibody producing “humoral “ response.
• Humoral response results in generation of antibodies to adenoviral proteins and prevents any subsequent infection if a second injection of the recombinant adenovirus is given.
Adenoviral vectors- LimitationsAdenoviral vectors- Limitations
Adeno-associated viral vectors:Adeno-associated viral vectors: • AAV is a simple, non-pathogenic, single stranded DNA virus dependent on the helper virus (usually adenovirus) to replicate. • It has two genes (cap and rep), sandwiched between inverted terminal repeats that define the beginning and the end of the virus and contain the packaging sequence. • The cap gene encodes viral capsid proteins and the rep gene product is involved in viral replication and integration. • It can infect a variety of cell types and in the presence of the rep gene product, the viral DNA can integrate preferentially into human chromosome 19.
AAV vectors:AAV vectors:
Gene therapy
• Gene therapy: – to correct a genetic defect by transferring of a functional normal
copy of the gene into cells
• Examples of diseases caused by genetic defect– Ornithine transcarbamylase (OTC deficiency)– Hemophilia (blood coagulation factors VIII or IX)– SCID( severe combined immunodeficiency)– Muscular dystrophy – Cystic fibrosis– Sickle cell anemia
Application of gene therapy
• Genetic disorder (deficiency): OTC• Cancer
– Genetic predisposition– Mutation in oncogene or tumor suppressor gene
• Autoimmunity diseases: rheumatoid arthritis– Delivery of counteracting gene
• Diseases involve several genes and the environmental interact: diabetes
Factors to be considered in Gene therapy
• How to deliver genes to specific cells, tissue and whole animals? (methods of delivery)
• How much and how long the introduced gene will be expressed?
• The site and dose of gene delivery
• Is there any adverse immunological consequence of both delivery vehicle (Virus) and the gene in animals?
• Is there any toxic effects?
Methods of gene delivery
• Viral Vectors: – Adenovirus– Retrovirus– Lentivirus– Adeno-associated virus (AAV)– Herpes simplex virus (HSV)
• Non-viral vector based– Naked DNA (plasmid DNA): injection or genegun– Liposomes (cationic lipids): mix with genes
• Ex-vivo• In vivo
Why use viral vectors
• Virus are obligate intracellular parasites• Very efficient at transferring viral DNA into host
cells• Specific target cells: depending on the viral
attachment proteins (capsid or glycoproteins)• Gene replacement: non-essential genes of virus
are deleted and exogenous genes are inserted
The application of an adenoviral vector leads to innate and
adaptive imm
une responses that ultimately lead to the
neutralization of the adenovirus as well as to the elim
ination of the transduced cells.