(PHA) 2.13 Immunopharmacology - Dr. Marbella PDF

2.
13 IMMUNOPHARMACOLOGY PHARMACOLOGY

Dr. Angeles D. Marbella | October 18, 2018

TRANS GROUP: Valdez, Valencia, Valenzuela, Vea LE 2 TRANS 13
TRANS HEADS: Tagorda

OUTLINE • Due to breakdown of self-tolerance
3. Isoimmune diseases
• Also known as Alloimmunity is an immune response to
I. INTRODUCTION
nonself antigens from members of the same species, which
A. Classification of Immunopharmacologic Drugs
B. Uses of Immunosuppression are called alloantigens or isoantigens.
C. Signals for T-cell Activation 4. Prevention of cell proliferation
II. CLASSIFICATION OF IMMUNOSUPPRESIVE AGENTS
A. Corticosteroids C. Signals for T-cell Activation
B. Calcineurin Inhibitors

C. Cytotoxic Agents
D. Proliferative Signal Inhibitors 1. SIGNAL 1: Engagement of antigen to T-cell receptor by the
E. Biologicals (Ab) MHC peptide complex
III. IMMUNOSUPPRESSION IN RENAL TRANSPLANTATION 2. SIGNAL 2: Binding of co-stimulatory molecules, CD80 &
A. IS Renal Transplantation CD86 on dendritic cells (APC) to CD28 on t-cell
B. Hydroxychloroquine 3. SIGNAL 3: Engagement of cytokines to specific receptors on
IV. Monoclonal Antibodies T-cell surface
A. Anti-Tumor Mabs
• RESULT: Clonal proliferation of t-cells
B. Immune Checkpoint Inhibitor Mabs
C. Mabs and Fusion Proteins • TREATMENT: targeted therapy on specific receptors on t-cell
V. Overview of the Mechanisms of Pharmacologic surface
Immunosuppression
VI. Immunomodulators
A. Levamisole
B. Thalidomide
C. BCG
D. Cytokines
1. Hematopoietic growth factors
2. Interferons
3. Interleukin-2
4. Therapeutic antibodies

LEARNING OBJECTIVES

1. Explain the mechanism of action, the PK and PD for most commonly
used immunosuppressive agents
2. Identify major side effects and toxicities
3. Identify the uses/indication for immunosuppressants

LEGEND

Remember Lecturer Book Prev. Trans Notes
G U & 4 !

I. INTRODUCTION
A. Classification of Immunopharmacologic Drugs
1. Immunosuppresants – ê immune response
2. Imuunomodulators – é immune response
3. Immunologicals

B. Uses of Immunosuppressants
1. Organ transplantation Figure 1. T-cell activation
• Terminologies:
o Autograft – within own body • DEVELOPMENT OF DIFFERENT IMMUNOSUPPRESANTS:
o Isograft – between twins o 1950’s – used radiation on organ transplants between twins
o Allograft – same species o 1960’s – use of steroids
o Xenograft – different species o 1970’s – use of Azathioprine
• Can be done on almost all organs. Most commonly o 1980’s – discovery of Cyclosporine, which revolutionized
transplanted is the kidney (you add a 3rd kidney) organ transplantation;; introduction of CYA improved
success
• Used to prevent immune attack on transplanted organ
o 2000’s – targeted therapy on specific antibodies, CD 25 &
• History:
CD22
o 1954 – 1st kidney transplant of Herrick twins
o 1959 – started transplanting non-identical HLA
individuals
o 1962 – 1st diseased donor organ
2. Autoimmune diseases
• Host immune system attacks own tissues, mistaking self-
antigens as foreign antigens
LE 2 TRANS 13 1 of 10
2.14 IMMUNOPHARMACOLOGY

B. PHARMACOLOGIC EFFECT
Adaptive immune response
• T-cells (Cell-mediated)
o Lyse and induce the redistribution of lymphocytes
o Inhibits T cells from making IL-2
o Activation of cytotoxic T-lymphocytes is inhibited
o Pro-inflammatory cytokines (Il-1 and IL-6) are
downregulated
• B-cells (Humoral)
o Curtail activation of NF-KB (Nuclear Factor – kappa
enhancer of B-cells)
Innate immune response
• Neutrophils and monocytes displays poor chemotaxis and
decreased lysosomal enzyme release
OTHERS: Regulates the transcription of numerous other genes
Figure 2. Development of Different Immunosupressants

II. CLASSIFICATION OF IMMUNOSUPPRESSIVE AGENTS
1. Corticosteroids
2. Calcineurin inhibitors
3. Cytotoxic agents (Mycophenolate mofetil)
4. Proliferative signal inhibitors
5. Biologicals (Antibodies)

A. Corticosteroids
• G Cornerstone in immunologic regimens in renal
transplantation and autoimmune diseases
A. MECHANISM OF ACTION

1. Glucocorticoid (S) is released by corticosteroid binding
globulin (CBG) and combines with receptor (R) in the
cytoplasm.
2. Binding induces conformational change in R releasing Figure 4. Pharmacological effects of glucocorticoids in inflammatory
HSP90 cells and structural cells.
3. Activated steroid-R dimer enters the nucleus and binds with
glucocorticoid response element (GRE) • Effect on inflammatory cells – Usually decrease in
4. U Inhibit mRNA synthesis and further protein numbers
synthesis so your production of cells are diminished o Decrease number of lymphocytes eosinophils
o Decrease in cytokines
o Decrease action of macrophages and
o Decrease number of dendritic cells
o Increase WBC count in CBC

Note: U Paradoxical effect on WBC Count
• If glucocorticoids are immunosuppressants, you might
expect the drug to decrease WBC count
• HOWEVER, the WBC count will usually INCREASE
(Leukocytosis) which is due to an INCREASE IN
NEUTROPHIL (Segmenters)
• De-margination of neutrophils → neutrophils detach from
endothelial lining and become available in the blood stream
• Steroids also diminishes migration of neutrophils to
target tissues making them more available in blood stream
• EXAMPLE: Patients in steroids after weeks if you repeat
CBC, WBC count will be as high as 30,000 with 92%
segmenters but patient is NORMAL with no fever and other
Figure 3. Mechanism of action of glucocorticoids.
symptoms → NOT AN INFECTION

& KATZUNG MOA: Interfere with cell cycle of active lymphoid
cells, cytotoxic to certain subset of T-cells – however some say it
is due to their ability to modify cellular functions rather than to • Effect on structural cells
direct cytotoxicity. Humoral immunity (antibodies) are less affected o Epithelial: Decrease in release of cytokines and mediators
but primary antibody response can be diminished also, with o Endothelial: Decrease leakiness of capillaries
continued use, previously established antibody responses are also o Airway smooth muscle: Increase B2-Receptor activity
decreased. (Vasodilation) and decrease cytokine production
o Mucous glands: decrease secretion
→ Effects on Airway smooth muscle and Mucus glands explain
why steroids are important in controlling Asthma U


Table 1. Comparison of Systemic Adrenocorticosteroids
Anti- Na- • Complications of Chronic Use (Not sure why Ma’am
Equivalent
Compound inflammatory retaining separated chronic from long term use)
dose
potency potency o Suppression of HPA Axis
Hydrocortisone 1 1 20mg § You are giving exogenous steroids
Cortisone 0.8 0.8 25mg § No endogenous production due to feedback mechanism
Deoxycorticosterone 0 100 - § G If your patients are in prolonged steroid use, you
Aldosterone 0 3000 - have to taper the doses gradually
Prednisone 4 0.8 5mg
- G Give time for the adrenal glands to produce the
Methylprednisolone 5 0 4mg
endogenous steroids (Ma’am said remember this)
Triamcinolone 5 0 4mg
o Patients that are considered not suppressed:
Dexamethasone 30 0 0.75
§ Any patient who has received any non-parenteral dose

of GC for less than 3 weeks
Emphasized in the table
§ Patients treated with alternate day steroids at
• U Dexamethasone – highest anti-inflammatory property physiologic doses
• U Followed by methylprednisolone o Patients that are suppressed:
o Although in the table it’s the same as triamcinolone § Anyone who has received more than 20mg of
• U The lowest is the Hydrocortisone prednisone a day for more than 3 weeks
o U Lowest because it is in the endogenous form § Any patient who has clinical Cushing’s syndrome (since
o Although in the table cortisone to aldosterone have lower patient already manifested symptoms of prolonged use
potency of steroids)

C. PHARMACOKINETICS • Minimizing GC(Glucocorticoids aka steroids) side-effects
• 50 – 90% Bioavailability o Exercise programs
• Absorption: delayed by food o Ca2+and vitamin supplements (Vitamin D, Bisphosphonates)
o U Notorious for inducing peptic ulcer disease o Estrogen therapy for menopausal women
o Usually given with food to avoid side effects of hyperacidity § Estrogen is also an exogenous steroid by why should
o Prevent side effects of hyperacidity we administer estrogen concomitantly with GC? Mainly
• Peak plasma levels: 30-100 min after drug intake because it protects menopausal women from bone loss
• Half-life is 3 hours – hence Calcium and Vitamin D are given.
• Metabolism in the liver o Alternate day steroid (Patients receive entire total dose that
• Excretion in the kidney would be given for 2 days. Example: You need 2 grams
• All forms are bioequivalent daily, take 4 grams for today, don’t take the next day, then
• Prednisone is NOT yet the active form take another 4 grams)
o It is converted to Prednisolone in the liver for it to be active
o TIP: “-solone” means activated form E. CLINICAL USE OF STEROIDS
• Clearance decreases with age varies with time of day • Rheumatoid and other arthritides
o Best time to give steroids is in the morning because the is • SLE, systemic dermatomyositis
the time for peak steroid excretion. Administration is in sync • Psoriasis and other skin conditions
with the physiologic body processes for lesser side effects • Asthma and other allergic disease
• Inflammatory renal diseases
D. SIDE EFFECTS • Inflammatory ophthalmic disease
• Autoimmune hematological disorders
• Acute exacerbation of Multiple Sclerosis

B. Calcineurin Inhibitors (CnI)
• U You only need to remember 2:
o Cyclosporin A (CsA)
§ from fungus Tolypocladium inflatum
§ & Treatment of Graft vs Host transplantation (mainly
Renal transplant) and Autoimmune disorders
o Tacrolimus (TAC)
§ macrolide antibiotic from Streptomyces tsukubaensis
§ Same indication as Cyclosporin but is also used for
organ and stem cell transplantation
Figure 5. Cushing Syndrome that may be a side effect of steroid use
§ & Standard prophylactic agent for graft versus host
Table 2. Immediate and Long-term effects of Cushing Syndrome disease
Immediate effects Long term effects § 50-100x more potent than CsA. (& 10-100x) Main diff.
Peptic ulcer disease Osteoporosis between CsA and TAC
Cushingoid features Growth retardation
Weight gain Skin atrophy
1. Both are structurally related but binds to different intracellular
(prolonged use)
mediators
Hypertension and Hyperlipidemia Avascular necrosis
• CsA binds to Cyclophilin (CpN)
(10-15% with high
doses) • TAC binds to FK-Binding Protein 12 (FKBP-12)
Diabetes (5 – 10%;; transient) 2. Both have the same inhibitory target → Calcineurin
3. Block the intracellular T-cell signal responsible for cytokine
Cataracts (10% with high doses)
production
Acne, hirsutism
Mood changes/ Psychiatric disturbances
Infection (Susceptible to opportunistic inf. –
viral /fungal. Why? Immunocompromised)

§ Hypertension and Hyperlipidemia
o Hepatic
§ Increased bilirubin – cholestasis
§ Increase hepatic enzymes from centroacinar
degeneration of hepatocytes
o Neurologic
§ Tremors
§ Nausea
§ Anorexia
o Epithelial
§ Hirsutism – increase hair growth
§ Gingival Hypertrophy (ppt;; in recordings she said
hyperplasia)
o Immunologic
§ Infections
Figure 6. U Cyclosporine A (CsA) binds to cyclophilin intracellularly § Malignancies
(CpN) and Tacrolimus (FK-506 old name) binds to FKBP-12 → Both

inhibit the activation of calcineurin (CaN) → inhibit the
dephosphorylation of nuclear factor of activated T-Cell (NF-ATc) → • TACROLIMUS
activation and proliferation of gene will not push through U o Table below compares CsA and TAC based on incidence of
(manufacturing and cloning of the T-cell 4) diabetes
o KEY FINDING: TAC has a higher incidence of new onset
B. PHARMACOKINETICS diabetes → metabolic effect
CYCLOSPORIN A
• 2 forms: Table 4. Studies comparing CsA and TAC for DM Incidence.
o Sandimmune – oil based, 100mg/ml Definition of Glucose
o Neoral – microemulsion formulation (gel like TAC CsA
Intolerance
preparation) US Kidney Trial New Onset DM
20% 4%
• Oral Bioavailability: 30-45% (Pirsch) (>30 days of Insulin)
• Food tend to enhance absorption of CyA European Kidney New Onset DM (>30 days of
8% 2%
• Narrow therapeutic index Trial Insulin)
o U Can be toxic thus a need to monitor blood levels US Liver Trial Hyperglycemia 47% 38%
European Trial All cases of DM 15% 9%
TACROLIMUS 5-
Miller et al. 2000 New Onset DM N/a
• Oral capsule: 5mg, 1 mg, 0.5mg, administered 2x a day 19%
• Absorbed in the small intestine Ahsan et al. 2001 New Onset DM 6% 4%
• Oral bioavailability: 25%
• Excretion: bile, minimal renal excretion • COMPARISON OF ADVERSE EFFECTS
o CsA is more causative for hypertension and hyperuricemia,
• Not significantly dialyzed
hypercholesterolemia. More causative of gum hypertrophy,
C. DRUG INTERACTIONS and hirsutism
CYCLOSPORIN A o TAC has more effects on the pancreas. May also exhibit
Neurotoxicity, Hairloss, and GI side effects.
• CYP Inducers: Decrease CsA levels

• CYP Inhibitors: Increase CsA levels Table 5. Comparison of AE between CsA and TAC.
o U Clinical – if you want to be economical, you can give Adverse Effect CsA TAC
combination of CsA with CYP inhibitors but monitor with Nephrotoxicity + +
blood levels Hyperkalemia + +
• Nephrotoxic drugs: Nephrotoxic Synergy Hypomagnesemia + +

Hypertension and Na Retention ++ +
Table 3. Drug Interactions of CsA
Hyperuricemia ++ +
Nephrotoxic
Decreased CsA Increased CsA Pancreatic Islet Toxicity (Glucose Intolerance) + ++
Synergy
levels levels Neurotoxicity + ++
(Nephrotoxic
(CYP Inducers) (CYP Inhibitors)
drugs) Hirsutism + -
Carbamazepine Diltiazem Acyclovir Gum Hypertrophy + -
Phenobarbital Erythromycin Aminoglycosides Hypercholesterolemia + -
Phenytoin Fluconazole Amphotericin B Hair Loss - +
Rifampin Itraconazole Furosemide GI Side Effects - +
Rifabutin Ketoconazole Ganciclovir
Nafcillin Metoclopramide H-2 Antagonists C. Cytotoxic Agents
Octreotide Methylprednisolone Melphalan
U I will not discuss this in detail. More of this will be discussed in
Ticlopidine Nicardipine NSAIDs
Orlistat Verapamil TMP/SMX cancer chemotherapy. I will just discuss mycophenolate
St. John’s Wort Grapefruit Juice Vancomycin mofetil (MMM)
Protease Inhibitors
Sirolimus • Classifications
o Antimetabolite
D. ADVERSE EFFECTS § Azathioprine
• CYCLOSPORIN A § Methotrexate
o Renal § Mycophenolate Mofetil (MMM)
§ Nephrotoxicity – Isometric Vacuolization and Interstitial § Leflunomide
Fibrosis o Alkylating agent
§ Hyperkalemia and Hyperuricemia § Cyclophosphamide

o Sirolimus binds to FKBP-12 (similar to Tacrolimus) and the
MYCOPHENOLATE MOFETIL complex binds and inhibits kinase mTOR (mammalian
- Potent cytostatic effects on T & B lymphocytes target of Rapamycin)
- Inhibits Ab production by B lymphocytes (Sirolimus – inhibits mTOR;; Tacrolimus – inhibits
- Inhibits T-cell proliferation after mitogen and allogenic calcineurin)
stimulation
- Prevents glycosylation of adhesion proteins (inhibits
recruitment of lymphocytes to inflammatory foci)

Clinical use
• Prevention of organ rejection
• Autoimmune Diseases
• & First line drug for preventing or reducing chronic
allograft vasculopathy in cardiac transplant recipients

• Reversibly inhibits inosine monophosphate
dehydrogenase (IMPDH)
• IMPDH is the rate limiting enzyme in the de-novo synthesis
Figure 7. Distinction of CsA, TAC, with Sirolimus based on MoA.
of purine building block of DNA (guanine & adenine)

• IMPDH prevents the conversion of Inosine monophosphate CsA vs TAC vs Sirolimus
to Xanthine Monophosphate Binding proteins: Cyclophilin and FKBP12
• Prevent proliferation of both T & (B cells → Inhibit antibody Effector proteins: Calcineurin and mTOR
production) 1. Calcineurin is a key enzyme in cell cycle progression
from Go to G1 (CsA and TAC: Inhibit IL-2 Message)
B. PHARMACOKINETICS 2. mTOR is a key enzyme in cell cycle progression from G1
• Rapidly absorbed and hydrolyzed to Mycophenolic Acid to S phase (Sirolimus: Inhibit IL-2 Response)
(MPA), the active immunosuppressive moiety, in the
liver, peak level 1-2hrs B. PHARMACOKINETICS
o MMM is not yet active. It must be converted to • Sirolimus
mycophenolic acid and conjugated with glucuronic acid o 1mg or 2 mg capsule
in the liver to become mycophenolic acid glucoronate o Peak: 1-2hours
• Bioavailability of capsule form: 90%, T1/2: 12 hrs o T1/2: 62 hours (U MAIN DIFFERENCE: Sirolimus has a
• 1 gm BID dose is recommended longer half-life)
• May be adjusted based on tolerance: GI/hematologic • Everolimus (NOT DISCUSSED)
Adverse effects o Similar to sirolimus but with shorter T1/2
• G MMF is not co-administered with azathioprine o T1/2: 23 hours
o U They are both antimetabolites and they act on the cell
cycle purine synthesis • Both metabolized by Cyp3A and P glycoprotein
• Not dialyzed o Has interactions with drug inhibitors and inducers
• Excretion: Renal minimal
C. ADVERSE EFFECTS • Target trough(minimum concentration): 5-15 ng/dL
• Gastrointestinal disturbances • Should be given 4 hrs after the CsA dose
o Nausea and Vomiting
o Diarrhea C. ADVERSE EVENTS
o Dyspepsia • Hyperglycemia
• Suppression of Bone Marrow • Hypercholesterolemia
o Leukopenia (Decrease WBC count) • Lymphocoele
o Thrombocytopenia (Decrease Platelet Count) • U G Impaired wound healing
o Not part of regimen in post kidney transplant since wound
G IF YOU ARE ASKED: Which of the ff drugs is most likely taken
healing is impaired
when there is a decrease in WBC Count → MMF has this effect o May be given after a month or 2, after the wound has
healed
• Enteric-Coated Mycophenolic Sodium ( EC-MS ) • Impaired renal function – U be wary of this effect
“Myfortic”
• Blood effects: cytopenia, thrombocytopenia, anemia
o Same therapeutic activity w/ MMF

o Less GI Adverse Effects
D. OTHER EFFECTS

• Oncologic effect (anti-neoplastic)t: anti-angiogenesis, arrests
D. Proliferative Signal Inhibitors
malignant cell growth in G1 –S phase
• Sirolimus (Rapamycin or Rapammune) • Also given for patients with malignancies
• Everolimus
• Temsirolimus E. Biologicals (Antibodies)

• Two Types: Polyclonal or Monoclonal
A. Polyclonal Antibodies
• SIROLIMUS (SRL) aka (Rapamycin or Rapammune)
• Contains antibodies with multiple distinct antigen combining
o Note: Only drug in this class discussed in lecture for
sites
MoA is Sirolimus
o Only 2% of antibodies produced are specific to immunizing
o Isolated from Streptomyces hygroscopicus
antigen
o Structurally similar to tacrolimus (TAC)
• Purified Ig preparation from animals after immunization with
o 27x more potent than TAC
human thymocytes or lymphocytes

• Usually given as induction therapy for kidney transplantation I. T-CELL DIRECTED ANTIBODIES (MUROMONAB OKT3)
o Induction therapy – first phase of treatment for multiple MECHANISM OF ACTION
myeloma to reduce number of plasma cells in the bone • The first therapeutic monoclonal antibody
marrow and the protein that they secrete. o Antibody directed specifically against the CD3 receptor on
• Anti-Thymocyte Globulin or ATG T cells
o & Antiserum is usually obtained by immunization of o Effective in preventing and treating rejection
horses, sheep, or rabbits, with human lymphoid cells o Significant Side effects:
§ Rabbit ATG (rATG) – from rabbit § G Cytokine release syndrome – results from the
§ Equine ATG (eATG) – from horses release of cytokines from cells targeted by the
antibody
- First Dose effect
- Fever, chills, rigors, “Shake and Bake”
- Pulmonary Edema
§ Sensitization
§ Risk of serious infections and cancer (due to
immunosuppression)
• Manufactured via Hybridoma Technology

Figure 8. Polyclonal Antibody Manufacturing. U Thymocyte,
lymphoblast, or thoracic duct lymphocyte from humans are injected to
animals. After some time, serum will be pooled and unwanted Ab are
removed. Sterilization is done to remove unwanted antibodies.
Stabilizers are added and sample is tested for microbial presence.
Afterwards they are stored in ampules

MECHANISM OF ACTION (ATG)
o Inhibit and suppress T-cell mediated immune response
§ Depletion of circulating T-cells
§ Modulation of cell surface receptor molecules
§ Induction of anergy Figure 9. Hybridoma Technology in Mab Manufacturing. UThe antigen
o Absence of normal immune response to an is injected in a mouse and the mouse produces (Ab-producing plasma
allergen or antigen cells). These cells are fused to preformed cancerous plasma cells and
§ Apoptosis of activated T-cells form hybridomas. These cells (hybidromas) are cultured and clones will
o Side Effects be chosen and tested for the desired Ab. Hybridomas can be
§ 75 % - infusion related reactions (e.g. fever, chills) proliferated by injecting it in another mouse OR the desired clones are
§ 40 % - formation of anti–antibodies frozen and eventually processed. Very expensive
o Impairs the function of introduced antibodies
§ 20 –50 % - leukopenia II. IL-2 RECEPTOR ANTAGONISTS
§ 6% - serum sickness • Directs against IL-2 receptor alpha chain antigen (CD25)
expressed on T-lymphocyte surface
Table 6. Comparison of Polyclonal Antibodies
ATGAM THYMOGLOBULIN Table 7. Chimeric mAb vs. Humanized mAb
Removing borders is Chimeric mAb Humanized mAb
Dose 15 mg/kg/day 75% human 90% human
suggested Composition
Shading rows with gray is 25% murine protein 10% murine protein
Regimen 5 -14 days Well-tolerated, but
suggested
Efficacy ++ Monitor CD2/3 may cause
Side effects Well-tolerated
Fever, chills, serum Fever chills, low plts, low hypersensitivity rxn
Safety (foreign substance)
sickness WBC
Predictable suppression of T Example Basiliximab Dacilizumab
Benefits Comfort level • TIP: (-Ximab: MiXture – chimeric) ;; (-Zumab: HumaniZed)
cells better tolerated
CRS – premed required;;
CRS – premed required;;
Risks slow infusion;; similar rates of
slow infusion
infection/malig
UThey are mostly the same. Not elaborated in the lecture.

B. Monoclonal Antibodies (categorized under antibodies but
will have a separate section later for thorough discussion)
• Ab derived from a single clone that is active against a single
antigen
o T-cell directed antibodies – Muromonab CD3 (OKT3)
o IL-2 receptor antagonists


Table 8. IL-2 receptor competitive antagonists • Humanized mAb
Agent Target MOA • Cell lysis and long lasting depletion
Targets: Binds to and • Therapeutic uses:
CD 25 (IL-2 blocks IL-2 receptor on T-
Basiliximab o Induction of immunosuppression
receptor α cells
Daclizumab o Acute rejection in kidney transplant
chain) Result: Inhibit IL-2 induced
T-cell activation • Not for maintenance therapy
Targets: Receptors on T & • Minimal side effects
B cells, monocytes,
Alemtuzumab CD52 macrophages & NK cells D. Rituximab (ANTI- CD20)
Result: cell lysis and long- • Anti-B cell
lasting depletion • Chimeric Mab approved for treatment of refractory non-
Targets: B cells Hodgkin’s lymphoma
Ritumixab CD20 Result: B cell lysis and
• Specific for CD20 markers on B cell
depletion
• Mediates cell lysis and depletion
Target: complement C5
protein • Therapeutic uses:
Complement Result: inhibit cleavage to o Treatment of refractory non-Hodgkin’s lymphoma
Eculizumab o Treatment of Post-Transplant Lymphoproliferative
protein C5 C5a & C5b, prevent
terminal complement Diseases (PTLD)
complex C5b-9 o Treatment and prophylaxis of Ab-mediated rejection
o Limited evidence for kidney transplant
A. Dacilizumab (Zenapax®) U4
E. Eculizumab (Recombinant Humanized mAb) U4
• 90% human, 10% murine protein (mouse)
• inhibition of critical cellular immune response involved in • Anti-tumor monoclonal antibodies
allograft rejection • Binds to complement protein C5, inhibiting cleavage to C5a &
• Therapeutic use: C5b
o Prophylaxis for acute organ rejection in kidney transplant • Prevent generation of terminal complement complex C5b-9
patients
• Adverse reactions: Table 9. Summary of Sites of Action of Selective Immunosuppressants
o GIT disorders (67%) on T-cell activation
o CMV infections (16%) Drug Site of Action
Glucocorticoid response element in DNA
• Dose: Glucocorticoids
(regulate gene transcription)
o 1 mg/kg in 50 mL 0.9% NSS IV for 15 min given 24 hrs
T-cell receptor complex (block Ag
before transplant Muromonab-CD3
recognition)
o Subsequent doses every 14 days, for 5 doses Cyclosporine/Tacrolimus Calcinuerin (inhibit phosphatase activity)
Azathioprine DNA (false nucleotide incorporation)
B. Baciliximab (Simulect®) U4 Inosine monophosphate dehydrogenase
MMF
• 75% human, 25% murine protein (mouse) (inhibits activity)
• used more than Daclizumab IL-2 receptor (block IL-2 mediated T-cell
Diclizumab/Basilizumab
• prevents T-cell proliferation activation)
• Therapeautic use: Protein kinase involved in cell cycle
Sirolimus
o Prophylaxis for acute organ rejection progression (mTOR) (inhibits activity)
o De novo renal transplantation U Memorize table.
• Adverse reactions:
o Well-tolerated F. Other immunosuppressant: Hydroxychloroquine
o Some reports of hypersensitivity • Anti-malarial agent
• Dose: 40mg given in 2doses (20mg each) • Suppresses intracellular antigen processing and loading of
o 1st Dose: 20 mg given 2 hrs before transplant peptides onto MHC class II molecules by increasing the pH
o 2nd Dose: 20 mg given 4 days after transplantRitumixab of lysosomal and endosomal compartments, thereby
• Anti-tumor monoclonal antibodies decreasing T-cell activation
• For CD20 markerks on B cell (anti-B cell) • Indication for SLE: U preventing activation of flares in SLE
• Chimeric mAb patients.
• Mediates cell lysis and depletion
• Therapeutic uses: III. IMMUNOSUPPRESSION IN RENAL
o Refractory non-Hodgkin’s lymphome TRANSPLANTATION
o Post-transplant lymphoproliferative diseases (PTLD) Immunosuppression in Renal Transplantation
o Treatment & prophylaxis of Ab-mediated rejection U We don’t only give one immunosuppressant in kidney
o Limited evidence for kidney transplant transplantation. We usually give a combination and the usual
are the CnI, Steroids, and Anti-metabolites (not yet discussed)
C. Alemtuzumab (CAMPATH 1H) U4 • Cnl/Steroids/ Anti-metabolites (not yet discussed)
• Humanized Mab directed against CD52 receptor on T-cells, • CsA/ MMF/ Steroids
B-cells, monocytes, macrophages, and NK cells >> cell lysis • TAC/ MMF/ Steroids
and long-lasting depletion • CsA/SRL/ Steroids
• Used for induction of immunosuppression and treatment of • TAC /SRL/ Steroids
acute rejection in renal transplantation o 90-95% 1-year graft survival
• NOT for maintenance therapy o 10-20% incidence of acute rejection
• Reports as induction in adult kidney transplant • Antibodies – further decrease incidence of acute rejection
• Anti-tumor monoclonal antibodies
• For CD52 receptor on T-cells, B cells, monocytes,
macrophages, and NK cells

B. IMMUNE CHECKPOINT INHIBITOR MAbs
U Indication: Cancer therapy

Table 11. Immune Checkpoint Inhibitor Mabs

MAbs Target Disease

Ipilimumab CTLA-4 Metastatic melanoma
Nivolumab PD-1 Hodgkin’s
Pembrolizumab Lymphoma, RCC,
Atezolimumab NSCLC, melanoma,
HIV tumors, Bladder
Cancer
Panitumab IgG2 kappa light EGFR expressing
chain Mab metastatic colorectal
Figure 10. One year renal graft survival with different
CA
immunosuppressive agents. Note the advent of immunosuppressive
Pertuzumab IgG1 Mab HER2/neu + breast
agents. There is a decrease in the incidence of acute rejection
CA

Ofatumumab IgG1 against CLL

CD20
IV. MONOCLONAL ANTIBODIES (MAbs)

U DON’T NEED TO KNOW EVERYTHING, DIFFERENT MABS
C. MAbs AND FUSION PROTEINS (USED AS
ARE USED IN DIFFERENT SUBSPECIALTIES. JUST BE IMMUNOMODULATORY AND ANTI-INFLAMMATORY AGENTS)
FAMILIAR WITH THE DRUGS! (AKA DON’T STUDY
U ACCORDING TO MA’AM, NO NEED TO MEMORIZE
ANYMORE. JOKE)
Indication: Psoriasis, Rheumatoid arthritis , SLE, Crohn’s
disease/Inflammatory bowel disease
A. ANTI-TUMOR Mabs

& KATZUNG Table 12. Mabs and Fusion Proteins (used as Immunomodulatory and
1. Alemtuzumab Anti-inflammatory Agents)
2. Bevacizumab MAbs Target Disease
3. Cetximab
4. Ofatumumab Adalimumab TNF a Rheumatoid arthritis
5. Panitumumab Certolizumab Psoriatic arthritis
6. Rituximab pegol Ankylosing spondylitis
7. Trastuzumab Etanercept Crohn’s diseases
8. Eculizumab (Recombinant Humanized Mab) Golimumab Ulcerative colitis
• humanized IgG monoclonal antibody that binds the infliximab
C5 complement component, inhibiting its cleavage Abatacept CTLA-4 RA
into C5a and C5b thereby inhibiting the terminal pore- KT
forming lytic activity of complement. & Anakinra IL-1 RA
Rilonacept IL-1R1
• Approved for patients with paroxysmal nocturnal
Ixekizumab IL-17 Plaque psoriasis
hemoglobinuria (PNH) and atypical hemolytic uremic
Secukinumab
syndrome (aHUS).
Brodalimab
• Reduces the need for red blood cell transfusions. & Reslizumab IL-5 Severe eosinophilic
Mepolizumab asthma
Table 10. Anti-Tumor Mabs 4& Siltuxomab IL-6 Casilieman’s disease
Drug Description Use (HIV )
Tocilizumab Humanized IgG1
Bevacizumab Anti-VEGF (anti Metastatic CA IL-6
vascular endothelial Basiliximab CD25 (IL2 receptor KT
growth factor) a)
Ranibizumab VEGF-A antagonist Age-related macular Belimumab B cell activating SLE
degeneration factor
Pegaptanib RNA aptamer Macular Canakinumab IL-1b CAPS (cryopyrin
directed against degeneration associated periodic
VEGF-165 syndromes)
Cetuximab Anti EGFR Metastatic wild type Natalizumab Humanized IgG1 MS
Kras colon cancer binds to a4 subunit Crohn’s disease
Gemtuzumab Anti CD33;; AML of a4 b1 of
withdrawn due to leucocytes
deaths Omalizumab Anti-IgE Allergic asthma
Panitumumab Anti CD20 Lymphoma,
leukemia, transplant
rejection,
autoimmune
disorders
Trastuzumab Anti-HER-2/neu HER 2+ breast CA


V. OVERVIEW OF THE MECHANISMS OF Peripheral neuropathy, constipation, rash, fatigue
o
PHARMACOLOGIC IMMUNOSUPPRESION Hypothyroidism
o
Increased risk for DVT (deep vein thrombosis)
o
IMids (immunomodulatory drugs) analogue: Lenalidomide,
o
Pomalidomide

C. Bacillus Calmette-Guerin (BCG)
• Live attenuated culture of Mycobacterium bovis
• Induces a granulomatous reaction at site of administration
• Indications:
o CA in situ of urinary bladder
o Prophylaxis of primary and recurrent papillary tumors
after transurethral resection

D. Recombinant Cytokines
1. Hematopoietic growth factors
• Erythropoietin
o Hormone produced by the kidneys that
stimulate bone marrow for RBC production
o Therapeutic use: Iatrogenic anemia
• G-CSF, GM-CSF
o Glycoprotein produced by recombinant DNA
technology
o Increase WBCs of patient with cytopenia due to
chemotherapy
o Therapeutic use: leukopenia
• U After chemotherapy, when all the blood cells are down
and low, these drugs can be given to increase the count.

Figure 11. Sites of immunosuppressant action
2. Interferon
1. Nuclear Region • Consists of recombinant DNA products that are
o Inhibition of gene expression to mediate available for IM, SQ, IV, and intralesional route
inflammatory response. MRNA transcription • Biologic activity: Mimics those of the naturally
o U Corticosteroids occurring endogenous molecules that are produced
2. Clonal expansion of cells and secreted by WBC in response to viral infections and
o Depletion of expanding lymphocyte population for immunologic activation
o Hallmark of immune response 4 • Three forms: INF-α2b, INF-β, INF-γ
o U Corticosteroids, CnI • Adverse effects:
3. CnI (location of CnI >> orange arrow) o Common: (First dose effect) fever, transient
a. U CnI will inactivate NFAT. Therefore, forward skin rash, flu-like symptoms, bone marrow
action in nucleus will not anymore proceed. suppression
4. Release of cytokines o Rare: Urticaria, angioedema,
a. Corticosteroids bronchoconstriction, anaphylaxis
5. Different cell surface receptors o Neuropsychiatric symptoms and depression
a. U MAbs (30%)

VI. IMMUNOMODULATORS Table 13. Differences between IFN-α-2b and β-1a
• It boost our immune systemU IFN-α-2b IFN-β-1a
• Agents that stimulate hematopoietic recovery in patients
suffering from cytopenia resulting from disease of therapy • Obtained from E. coli
• Has antiviral and
• Indications: Chronic
immunomodulatory effect
A. Levamisole Hepatitis B and C, Melanoma,
• Indication: Multiple Sclerosis
Follicular lymphoma and
• Originally synthesized as anti-helminthic Kaposi’s sarcoma

• Restores depressed immune function of B- lymphocytes, T-
lymphocytes, monocytes and macrophages
• Indication: Colon CA Duke’s Stage C, adjuvant 5-FU 3. Interleukin-2
• T-cell growth factor in 1976
B. Thalidomide • Stimulates growth of T-lymphocytes from normal human
• Known for severe, life threatening birth defects BM
o Banned before, for use as an abortifacient • Indications: Metastatic renal cell CA
• Inhibits TNF-α, reduces phagocytosis by neutrophils, • Adverse effects:
increases production of IL-10, alters adhesion molecule o Hypotension
expression and enhances cell-mediated immunity o Major organ failure
• Indication: o Fatal systemic capillary leak
o Erythema Nodosum leprosum • Others: U GOOD TO KNOW
o Multiple myeloma o Dimethyl fumarate (DMF) – flushing
o Rheumatoid arthritis o Glatiramer acetate – skin hypersensitivity
o Lupus o Fingolimod hydrochloride (FH) – cardiac toxicity
• Adverse effects: o Approved for treatment of relapsing-remitting
o Teratogenesis (phocomelia) multiple sclerosis

o Respiratory Syncitial Virus (RSV)
4. Therapeutic antibodies immuneglobulin (IV)
a. Intravenous Immunoglobulin (IVIG) (Polyclonal)
• Prepared by cold ethanol fractionation of
plasma from multiple donors (10,000 to 60,000
donors) followed by processes that remove Ab
aggregates and inactivate potential viral
pathogens
• Supplied as 5% or 10% Protein solution
• 95-99% of IVIG is IgG with traces of IgA, IgM
• MOA:
o Reduction of T-helper cells Figure 12. Balance on immunosupression
o Increase of regulatory T cells
o Decreased spontaneous IgG Ex: U Organ Transplantation
production o Reduced immunosuppressant, there will be rejection.
o Fc receptor blockade o Increase immunosuppressant too much, then infections
o Increased Ab catabolism will come out.
o Idiotypic-anti-idiotypic interaction with U “BALANCED IMMUNOSUPPRESSION IS THE GOAL TO
pathologic antibodies ATTAIN DESIRED AFFECT FREE FROM SIDE EFFECTS!”
• Uses:
o U Useful for neurologic symptoms, TEST YOUR KNOWLEDGE
even in immunodeficient patients
§ Encephalitis 1. The correct immunosuppressant and intracellular
§ Multiple sclerosis mediators/receptors combination is:
o U Immune replacement for primary A. Cyclosporine: Calcineurin
immunodeficiency diseases B. Sirolimus: mTOR
o U Immunomodulation for: C. Tacrolimus: FKBP12
§ Autoimmune TTP D. Evermolimus: Cyclophilin
(thrombotic
thrombocytopenic purpura) 2. Which of the following biologicals is correctly matched with its
§ Toxic epidermal necrolysis target antigen?
§ Kawasaki disease to prevent
formation of cardiac A. Daclizumab - CD 20
aneurysm B. Rituximab - CD 52
§ HIV, bone marrow transplant C. Alemtuzumab - CD 25
• Adverse effects: D. Eculizumab - C5
o Infections
o Formation of immune complexes 3. The attending medical doctor of Tara decided to give her
o Flushing something to boost her immune system as treatment for her
o Headache hepatitis B infection. Which of the following drugs should be
o Nausea and vomiting given?
o Myalgias A. Rabbit anti-thymocyte globulin
o Aseptic meningitis (rare) B. Interferon
o Pre-treatment: Aspirin, C. Mycophenolate mofetil
Acetaminophen, Diphenhydramine, D. Prednisone
Hydrocortisone (U Given in order to
prevent reactions to IVIG) 4. A 25-year old post kidney transplant patient on follow-up
presented with decreased WBC and platelet counts. Which of
b. Polyclonal antibody (directed against cells) the following drugs is most likely causing these?
• RhD Immunoglobulin
o Human IgG globulin solution A. Prednisone
containing an enriched fraction of Ab B. Mycophenolate mofetil
against the D blood group Ag C. Tacrolimus
o Given after first pregnancy of Rh (-) D. Cyclosporine A
mother within 72 hours of birth of an
Rh (+) baby 5. Increased susceptibility to infection in patients on prolonged
steroid use is mainly due to this pharmacologic effect:
c. Hyperimmune globulins (Polyclonal and
monoclonal) for infectious disease A. Regulation of transcription of genes
• Specific immuneglobulins also called B. Lysis and redistribution of induced lymphocytes
“hyperimmune globulins” C. Poor chemotaxis of neutrophils and macrophages
• Prepared from select donors who have high D. Inhibition of cytotoxic T-cell activation
titers of the desired Ab, either naturally
acquired or simulated through immunization REFERENCES

• Hyperimmune globulins:
1. Lecture Presentation
o Hep B immunoglobulin
2. Notes
o Rabies immunoglobulin
3. 2020 Trans
o Tetanus immunoglobulin
4. Katzung
o Varicella immunoglobulin

o Cytomegalovirus (CMV) Answers: 1) C 2)D 3)B 4)B 5)C (2020A Anek)
immuneglobulin (IV)


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Dr. Angeles D. Marbella | October 18, 2018

Remember Lecturer Book Prev. Trans Notes

A. MECHANISM OF ACTION

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