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KINJAN MEHTA
      Sem.- VII
 What   is IMMUNITY?
 The word immunity is derived from the
  Latin word immunes which means “exempt
  from”.
 Immunity is usually defined as a state of
  relative resistance to an infection.
 Substances capable of stimulating immune
  mechanism are called as antigens.
 Components   of immune system:
 Lymphocytes.
 Cellular immunity.
 Humoral immunity.
 Immunoglobulin.
 Lymph nodes.
 Spleen.
 Thymus.
 There  are 2 types of immunity:
 Active immunity.
 Passive immunity.
 Theimportant components of immune
 system include:
 Granulocytes
 Complement synthesis and antibody
 formation
 Cellular immunity
 Mucocutaneous barriers
 NEUTROPHILS        are synthesized from
  GRANULOCYTES, as the total
  granulocyte count falls below 1000 cells
  /mm3, the rate of bacterial infection
  increases.
 The common org. affecting this are
  E.coli, Pseudomonas
  aeruginosa, Klebsiella, Pneumonia and
  stapylococcus aureus.
 The chances of fungal viral and protozal
  infection is also very high.
 When  the defect in this system is there the
  increase in infection rate is seen.
 Such effects usually occur through the
  chronic treatment with chemotherapeutic
  agents.
 Itprovides protection against fungal
  bacterial, viral and protozal infections.
 Certain drugs, neoplastic diseases and
  organ transplantation procedures
  paralyzes cellular immunity.
 They   prohibit pathogenic organisms to
  take entry into the internal vital organs.
 However these barriers are damaged by a
  no. of medical devices, procedures, or
  chemotherapy.
 This leads to easy access of pathogens to
  the internal organs resulting into infectious
  state.
 (A) ANTI-HISTAMINIC AGENTS:
 Histamine- binding lymphocytes have
  immunosuppressive activities.
 By inhibiting their activation , antihistaminic
  agents improve cell mediated immune
  response.
 IT is the non-narcotic analgesic agent that
  relives pain sensation b inhibiting
  prostaglandin biosynthesis.
 This leads to significant improvement in
  the functioning of t-lymphocytes.
 Useful in coccidiomycosis and
  mycobacterial infections.
 Chemically     it is the complex of inosine and
  an organic salt.
 It enhances t-cell proliferation,
  phagocyotsis and chemo taxis through
  unknown mechanism.
 Initially it was found as an anti-viral agent.
 IT  improves chemotactic responses and
  immune mechanisms in patients with
  diseases associated with
  immunodeficiency.
 It probably acts by inducing the release of
  c-GMP.
 Onlytwo lymphokines known as IL-1, IL-2
 were found to stimulate the patient
 immunity.
 These  are the polypeptides isolated from
  the epithelial cells of thymus gland.
 They induce formation of mature T- cells
  by unknown mechanism.
 This are given usually in saline i.m. in
  doses between 0.5mg/kg and 1.0 mg/kg
  /day for 2-3 weeks and then reduced to 1-3
  doses per week.
 Thisis low molecular weight peptide (m.w.
 less than 6000 Daltons) isolated from
 blood leucocytes of the patient with
 delayed hypersensitivity. it has stimulant
 effect of cell mediated immunity. it may be
 used in treatment of immunodeficiency
 syndrome like chronic mucotaneius
 candidacies, in treatment of recurrent
 herpes simplex conditions
 Various   phases of immune responses
  include:
 (1) antigen reorganisation and/processing.
 (2) amplification.
 (3) antibody formation and
 (4) immune effectors responses.
 Depending   upon the suppressant and
  stimulate effects exerted by these drugs on
  immune system they are categorized as:
 (1) IMMUNOSUPPRESSANTS
 (2) IMMUNO ENHANCERS.
Phases of immune        Suppressants        Enhancers
response

Antigen recognisation   Corticosteriods.    BCG vaccine.
and processing          Cyclophosphamide    C. Parvum
                        cytimun             Tetramisole

Amplification.          L- Asparaginase     Concanavalin A.
                        Corticosteroids.    Tetramisole.
                        Cyclophosphamide.
                        Cytimum.
                        5-fluorouracil

Antibody formation      Corticosteroids.    Lipopolysaccaride.
                        Cyclophosphamide    Tetramisole.
                        Cyclosporin A
                        cytimun
Phases of immune   Suppressants.      enhancers.
response

Immune affector    Corticosteroids    C. parvum.
response           Cylcophosphamide   tetramisole
                   Cyclosporin A
                   Cytarabine
                   Cytimun
                   Methotrexate.
 During  organ transplantation, certain
  complex antigens or allograts activate the
  cytotoxic lymphocytes. Their activation
  results to the development of cellular
  immunity rejects organ transplants.
 Immunosuppressive agent beneficial
  effects in such condition suppressing the
  cellular immunity.
 Most  of these agents are primarily used as
  anti- neoplastic agents.
 On the basis of the mechanism of action,
  immunosuppressant can be classified as:
Alkylating
corticosteroids                antimetabolites
                   agents


                               Antibodies and
  antibiotics     enzymes      miscellaneous
                                   agents
                         Examples:


Betamethasone ,
dexamethasone.                                  triamcinolone


                                        Prednisolone,
         hydrocortisone
                                      methylprednisolone




                      paramethasone
 They   all possess anti allergic and anti-
  inflammatory and immunosuppressive
  activities.
 T- lymphocytes are most susceptible to the
  action of corticosteroids resulting into
  lymphopenia.
 They also effect humoral immune
  responses by inhibiting antibody synthesis.
 Adverse  effect:
 High doses cause Osteoporosis,
  hyperglycemia, ulcer formation and
  increased susceptibility for fungal
  infections .
 DOSE: 2-10 mg/kg per day for few weeks.
 Adverse effect can be reduced by usig
  combination of other cytotoxic agents and
  lowering the dose.
 This  kill components of immune response
  of body.
 They give immunosuppressive action to
  the rapidly proliferation cells in the marrow
  and exert cytotoxic effects to the
  lymphocytes by alkylating their nucleic
  acid.
 EXAMPLES:
  CYLCOPHOSPHAMIDE,CYTIMUN.
 CYCLOPHOSPHAMIDE:
 It is a nitrogen mustard and have broad
  spectrum of antineoplastic and immune
  suppressive activities.
 More effective suppressor of humoral
  immune mechanisms.
 It exerts cyotoxic action on both T-cells and
  B-cells.
 DOSE: 2 mg/kg per day.
 Usuallyused in combination with
 corticosteroids in treatment of several
 autoimmune diseases, including
 Wegener’s granulomatosis. Childhood
 nephrosis, idiopathic thrombocytopenia
 purpura and severe rheumatoid arthrititis.
 CYTIMUM:
 It is analog of cylophosphamide having
  better therapeutic index.
 It is specifically effective against B-cells.
 These  drugs act by exerting cyotoxic
  effects on rapidly proliferating cells like
  those of bone marrow, myeloid
  tissues, gonadal tissues and g.i. tract.
 METHOTREXATE, 6-
  MERCAPTOPURINE, AND
  AZATHIOPRINE are extensively studied
  drugs which are more toxic to S-phase
  when DNA synthesis is occurring.
 AZATHIOPRINE:
 It is imidazole derivative of 6-
  mercaptopurine having anti-rheumatic
  activity along with cytotoxic effect.
 It is orally effective and having plasma half
  life of about 16 hours.
 It is the most effective suppressant of
  phase-II of immune responses.
 Xanthine   oxidase enzyme converts much of
  the drug in liver and RBC to 6-thiouric
  acid, thioionisic acid and various other
  metabolized.
 Thioinosic acid competitively inhibit synthesis
  of inosinic acid. This result in inhibition of
  DNA synthesis. thus upon the metabolized
  activation, this suppresses both mediated and
  humoral immune responses and depresses
  antibody proliferative responses.
 AZATHIOPRINE       is used orally in the
  treatment of acute glomerunephritis,
  systemic lupus erythematosus,
  temporalcranial arteritis.
 It is also used in management of organ
  transplantation and delay hypersentizing
  reactions.
 DOSE: 2-5 mg/kg per day.
 METHOTREXATE:
 It is an orally active folic acid analog having anti
  neoplastic and antipsoratic and mild immune
  suppressant activity.
 It has a plasma half-life 7.2-9.0 hours.
 It acts by inhibiting folate metabolism and affects
  phase-II of immune responses.
 It is used to treat severe psorasis,
  dermatomcosotis and rheumatoid arthritis and also
  used in organ transplantation procedure.
 Other drug include chlorambucil, mercaptopurine,
  thioguanine, azarbine, cytarabine.
 CYCLOSPORIN         A is he example for this
  having immunosuppressive. It is the cyclic
  activity and is isolated from the soil fungus,
  Tolypolacadofium inflatum.
 It spefically inhibit generation of effectors
  T-lymphocytes without expressing effect of
  suppressor lymphocytes and B-cells
  activity.
 It impairs proflirative response of T-cells
  of antigens.
 Once   T-cells are stimulated by antigens
  they synthesized interculin -2 that’s start
  growth promoting effects on T-
  lymphocytes.
 Cyclosporine has low activity profile.
 A.E.: gumhypertropy, tremor.
  Neurasthesia, depressive psychosis and
  benign breast tumours'.
 It has plasma half life of 10-27 hours.
 USED    in organ transplantation in patients
  having liver, kidney, pancreas disorder and
  heart transplantation.
 It also expands its effects in the treatment
  of immune diseases of rheumatic arthritis.
 DOSE: adult oral dose is 10-20 mg/kg per
  day.
 i.v. 50 mg diluted intranasal saline may be
  given by slow infusion.
 L-ASPARAGINASE          is the drug of choice
  in treatment of acute lymphoblastic
  leukaemia.
 It has half life of about 11-23 hours.
 this enzyme is usually given i.v. or i.m.
 When combined with methotrexate it
  lowers down the adverse effect and
  intensifies its activity.
EXAMPLE: ANTITHYMOCYTE GLOBULIN (ATG)



 ATG  is used alone or in combination with
  azathioprine and corticosteroids in the
  prevention of the renal allograft rejection in
  the dose of 1-5 mg/kg per day.
 However in some patients , allergic
  reactions has been reported to occur to
  leading to serum sickness and nephritis.
 (A) ADENOSINE DEAMINASE
  INHIBOTORS;
 Examples are erythro-9-(2-hydroxy-3-
  nonyl) adenine hydrochloride and 2-
  deoxy- coformycin.(pentastatin).
 Former one have effect on T-lympohcytes
  while pentastatin is used as antimetabolite.
 (B)  BREDININ:
 It is an imidazole nucleoside having
  antimetabolite antineoplastic activity and is
  used as an immunosuppressant in human
  kidney transplantation.
 (C) CYCLOIMMUNE:
 It is analog of cyclosporine, undergoing
  clinical trials and showing activity for organ
  transplantation.
 (D)   NIRIDAZOLE:
 It is an orally active nitrothiazole derivative
  having anthelmintic activity, anti bacterial
  and immunosuppressive activities.
 It is used to suppress cell- mediated
  immunity response.
 This category of the drugs is used to
  overcome immunodeficiency or
  immunosupreesion arising as a result of
  either inherited or acquired disorders of
  immune system.
 Examples of inherited disorders:
  Agammaglobulinemia and Severe combined
  immune deficiency syndrome (SCIDS).
 Causes: chemotherapy. Radiation or viral
  infection may cause immunosupreesion.
 Examples    of this category include :
 (a) BCG Vaccine:
 It is used as immunological enhancer to
  stimulate intact immune system (i.e. a non-
  specific immunoenhancer.) of the body.
 BCG and its methanol extracted residue
  (MER) contain muramyl dipeptide as an
  active immunostimulant ingredient.
 T-lymphocytes are principle target cells for the action
  of BCG vaccine.
 It causes stimulation of macrophage function,
  phagocytic activity, lysosomal enzyme activity and
  chemotaxis mechanisms .
 It induces the production of lymphocyte-activity factor
  resulting of phase I of immune response.
 Because of its activity against tumour antigen it is
  beneficial in treatment of lung and breast cancer, acute
  lympholytic and myelogeneous leukaemia.
 It is available as unlyophilized, live or killed lyophilized
  form.
 Administration as oral, i.v., i.p., i.d. , intralesional.
 Levamisole is orally active S(-) isomer of
  tetramisole. It is used as immunostimulant in the
  therapy of certain infections, r.a., and
  immunosuppressive conditions
 It mainly acts by raising c-GMP levels through
  interaction with thymopoietien receptor sites. this
  leads to decrease in metabolic inactivation of c-
  GMP accompanied with increased breakdown of c-
  AMP. The increase in c-GMP level induces
  lymphocyte proliferation and augmentation of
  chemotactic responses.
 This reflects into increased antibody
  production, lymphokine production, increased
  phagocytosis.
 Tetramisole  is used in treatment of:
 (1)certain chronic and recurrent bacterial
  infections
 (2) certain diseases with immunodeficiency
  like chronic granulomatous syndrome,
  job’s syndrme etc.
 (3) autoimmune diseases like r.a., crohn’s
  disease, SLE.
 OTHERS    ARE:
 Corynebacterium parvum
 Tilorone
 Inosiplex
 Lipopolysaccharides
 Dialyzable leukocyte extract
Understanding Immunity and Immunosuppressants

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Understanding Immunity and Immunosuppressants

  • 2.  What is IMMUNITY?  The word immunity is derived from the Latin word immunes which means “exempt from”.  Immunity is usually defined as a state of relative resistance to an infection.  Substances capable of stimulating immune mechanism are called as antigens.
  • 3.  Components of immune system:  Lymphocytes.  Cellular immunity.  Humoral immunity.  Immunoglobulin.  Lymph nodes.  Spleen.  Thymus.
  • 4.  There are 2 types of immunity:  Active immunity.  Passive immunity.
  • 5.  Theimportant components of immune system include: Granulocytes Complement synthesis and antibody formation Cellular immunity Mucocutaneous barriers
  • 6.  NEUTROPHILS are synthesized from GRANULOCYTES, as the total granulocyte count falls below 1000 cells /mm3, the rate of bacterial infection increases.  The common org. affecting this are E.coli, Pseudomonas aeruginosa, Klebsiella, Pneumonia and stapylococcus aureus.  The chances of fungal viral and protozal infection is also very high.
  • 7.  When the defect in this system is there the increase in infection rate is seen.  Such effects usually occur through the chronic treatment with chemotherapeutic agents.
  • 8.  Itprovides protection against fungal bacterial, viral and protozal infections.  Certain drugs, neoplastic diseases and organ transplantation procedures paralyzes cellular immunity.
  • 9.  They prohibit pathogenic organisms to take entry into the internal vital organs.  However these barriers are damaged by a no. of medical devices, procedures, or chemotherapy.  This leads to easy access of pathogens to the internal organs resulting into infectious state.
  • 10.  (A) ANTI-HISTAMINIC AGENTS:  Histamine- binding lymphocytes have immunosuppressive activities.  By inhibiting their activation , antihistaminic agents improve cell mediated immune response.
  • 11.  IT is the non-narcotic analgesic agent that relives pain sensation b inhibiting prostaglandin biosynthesis.  This leads to significant improvement in the functioning of t-lymphocytes.  Useful in coccidiomycosis and mycobacterial infections.
  • 12.  Chemically it is the complex of inosine and an organic salt.  It enhances t-cell proliferation, phagocyotsis and chemo taxis through unknown mechanism.  Initially it was found as an anti-viral agent.
  • 13.  IT improves chemotactic responses and immune mechanisms in patients with diseases associated with immunodeficiency.  It probably acts by inducing the release of c-GMP.
  • 14.  Onlytwo lymphokines known as IL-1, IL-2 were found to stimulate the patient immunity.
  • 15.  These are the polypeptides isolated from the epithelial cells of thymus gland.  They induce formation of mature T- cells by unknown mechanism.  This are given usually in saline i.m. in doses between 0.5mg/kg and 1.0 mg/kg /day for 2-3 weeks and then reduced to 1-3 doses per week.
  • 16.  Thisis low molecular weight peptide (m.w. less than 6000 Daltons) isolated from blood leucocytes of the patient with delayed hypersensitivity. it has stimulant effect of cell mediated immunity. it may be used in treatment of immunodeficiency syndrome like chronic mucotaneius candidacies, in treatment of recurrent herpes simplex conditions
  • 17.  Various phases of immune responses include:  (1) antigen reorganisation and/processing.  (2) amplification.  (3) antibody formation and  (4) immune effectors responses.
  • 18.  Depending upon the suppressant and stimulate effects exerted by these drugs on immune system they are categorized as:  (1) IMMUNOSUPPRESSANTS  (2) IMMUNO ENHANCERS.
  • 19. Phases of immune Suppressants Enhancers response Antigen recognisation Corticosteriods. BCG vaccine. and processing Cyclophosphamide C. Parvum cytimun Tetramisole Amplification. L- Asparaginase Concanavalin A. Corticosteroids. Tetramisole. Cyclophosphamide. Cytimum. 5-fluorouracil Antibody formation Corticosteroids. Lipopolysaccaride. Cyclophosphamide Tetramisole. Cyclosporin A cytimun
  • 20. Phases of immune Suppressants. enhancers. response Immune affector Corticosteroids C. parvum. response Cylcophosphamide tetramisole Cyclosporin A Cytarabine Cytimun Methotrexate.
  • 21.  During organ transplantation, certain complex antigens or allograts activate the cytotoxic lymphocytes. Their activation results to the development of cellular immunity rejects organ transplants.  Immunosuppressive agent beneficial effects in such condition suppressing the cellular immunity.
  • 22.  Most of these agents are primarily used as anti- neoplastic agents.  On the basis of the mechanism of action, immunosuppressant can be classified as:
  • 23. Alkylating corticosteroids antimetabolites agents Antibodies and antibiotics enzymes miscellaneous agents
  • 24. Examples: Betamethasone , dexamethasone. triamcinolone Prednisolone, hydrocortisone methylprednisolone paramethasone
  • 25.  They all possess anti allergic and anti- inflammatory and immunosuppressive activities.  T- lymphocytes are most susceptible to the action of corticosteroids resulting into lymphopenia.  They also effect humoral immune responses by inhibiting antibody synthesis.
  • 26.  Adverse effect:  High doses cause Osteoporosis, hyperglycemia, ulcer formation and increased susceptibility for fungal infections .  DOSE: 2-10 mg/kg per day for few weeks.  Adverse effect can be reduced by usig combination of other cytotoxic agents and lowering the dose.
  • 27.  This kill components of immune response of body.  They give immunosuppressive action to the rapidly proliferation cells in the marrow and exert cytotoxic effects to the lymphocytes by alkylating their nucleic acid.  EXAMPLES: CYLCOPHOSPHAMIDE,CYTIMUN.
  • 28.  CYCLOPHOSPHAMIDE:  It is a nitrogen mustard and have broad spectrum of antineoplastic and immune suppressive activities.  More effective suppressor of humoral immune mechanisms.  It exerts cyotoxic action on both T-cells and B-cells.  DOSE: 2 mg/kg per day.
  • 29.  Usuallyused in combination with corticosteroids in treatment of several autoimmune diseases, including Wegener’s granulomatosis. Childhood nephrosis, idiopathic thrombocytopenia purpura and severe rheumatoid arthrititis.
  • 30.  CYTIMUM:  It is analog of cylophosphamide having better therapeutic index.  It is specifically effective against B-cells.
  • 31.  These drugs act by exerting cyotoxic effects on rapidly proliferating cells like those of bone marrow, myeloid tissues, gonadal tissues and g.i. tract.  METHOTREXATE, 6- MERCAPTOPURINE, AND AZATHIOPRINE are extensively studied drugs which are more toxic to S-phase when DNA synthesis is occurring.
  • 32.  AZATHIOPRINE:  It is imidazole derivative of 6- mercaptopurine having anti-rheumatic activity along with cytotoxic effect.  It is orally effective and having plasma half life of about 16 hours.  It is the most effective suppressant of phase-II of immune responses.
  • 33.  Xanthine oxidase enzyme converts much of the drug in liver and RBC to 6-thiouric acid, thioionisic acid and various other metabolized.  Thioinosic acid competitively inhibit synthesis of inosinic acid. This result in inhibition of DNA synthesis. thus upon the metabolized activation, this suppresses both mediated and humoral immune responses and depresses antibody proliferative responses.
  • 34.  AZATHIOPRINE is used orally in the treatment of acute glomerunephritis, systemic lupus erythematosus, temporalcranial arteritis.  It is also used in management of organ transplantation and delay hypersentizing reactions.  DOSE: 2-5 mg/kg per day.
  • 35.  METHOTREXATE:  It is an orally active folic acid analog having anti neoplastic and antipsoratic and mild immune suppressant activity.  It has a plasma half-life 7.2-9.0 hours.  It acts by inhibiting folate metabolism and affects phase-II of immune responses.  It is used to treat severe psorasis, dermatomcosotis and rheumatoid arthritis and also used in organ transplantation procedure.  Other drug include chlorambucil, mercaptopurine, thioguanine, azarbine, cytarabine.
  • 36.  CYCLOSPORIN A is he example for this having immunosuppressive. It is the cyclic activity and is isolated from the soil fungus, Tolypolacadofium inflatum.  It spefically inhibit generation of effectors T-lymphocytes without expressing effect of suppressor lymphocytes and B-cells activity.  It impairs proflirative response of T-cells of antigens.
  • 37.  Once T-cells are stimulated by antigens they synthesized interculin -2 that’s start growth promoting effects on T- lymphocytes.  Cyclosporine has low activity profile.  A.E.: gumhypertropy, tremor. Neurasthesia, depressive psychosis and benign breast tumours'.  It has plasma half life of 10-27 hours.
  • 38.  USED in organ transplantation in patients having liver, kidney, pancreas disorder and heart transplantation.  It also expands its effects in the treatment of immune diseases of rheumatic arthritis.  DOSE: adult oral dose is 10-20 mg/kg per day.  i.v. 50 mg diluted intranasal saline may be given by slow infusion.
  • 39.  L-ASPARAGINASE is the drug of choice in treatment of acute lymphoblastic leukaemia.  It has half life of about 11-23 hours.  this enzyme is usually given i.v. or i.m.  When combined with methotrexate it lowers down the adverse effect and intensifies its activity.
  • 40. EXAMPLE: ANTITHYMOCYTE GLOBULIN (ATG)  ATG is used alone or in combination with azathioprine and corticosteroids in the prevention of the renal allograft rejection in the dose of 1-5 mg/kg per day.  However in some patients , allergic reactions has been reported to occur to leading to serum sickness and nephritis.
  • 41.  (A) ADENOSINE DEAMINASE INHIBOTORS;  Examples are erythro-9-(2-hydroxy-3- nonyl) adenine hydrochloride and 2- deoxy- coformycin.(pentastatin).  Former one have effect on T-lympohcytes while pentastatin is used as antimetabolite.
  • 42.  (B) BREDININ:  It is an imidazole nucleoside having antimetabolite antineoplastic activity and is used as an immunosuppressant in human kidney transplantation.  (C) CYCLOIMMUNE:  It is analog of cyclosporine, undergoing clinical trials and showing activity for organ transplantation.
  • 43.  (D) NIRIDAZOLE:  It is an orally active nitrothiazole derivative having anthelmintic activity, anti bacterial and immunosuppressive activities.  It is used to suppress cell- mediated immunity response.
  • 44.  This category of the drugs is used to overcome immunodeficiency or immunosupreesion arising as a result of either inherited or acquired disorders of immune system.  Examples of inherited disorders: Agammaglobulinemia and Severe combined immune deficiency syndrome (SCIDS).  Causes: chemotherapy. Radiation or viral infection may cause immunosupreesion.
  • 45.  Examples of this category include :  (a) BCG Vaccine:  It is used as immunological enhancer to stimulate intact immune system (i.e. a non- specific immunoenhancer.) of the body.  BCG and its methanol extracted residue (MER) contain muramyl dipeptide as an active immunostimulant ingredient.
  • 46.  T-lymphocytes are principle target cells for the action of BCG vaccine.  It causes stimulation of macrophage function, phagocytic activity, lysosomal enzyme activity and chemotaxis mechanisms .  It induces the production of lymphocyte-activity factor resulting of phase I of immune response.  Because of its activity against tumour antigen it is beneficial in treatment of lung and breast cancer, acute lympholytic and myelogeneous leukaemia.  It is available as unlyophilized, live or killed lyophilized form.  Administration as oral, i.v., i.p., i.d. , intralesional.
  • 47.  Levamisole is orally active S(-) isomer of tetramisole. It is used as immunostimulant in the therapy of certain infections, r.a., and immunosuppressive conditions  It mainly acts by raising c-GMP levels through interaction with thymopoietien receptor sites. this leads to decrease in metabolic inactivation of c- GMP accompanied with increased breakdown of c- AMP. The increase in c-GMP level induces lymphocyte proliferation and augmentation of chemotactic responses.  This reflects into increased antibody production, lymphokine production, increased phagocytosis.
  • 48.  Tetramisole is used in treatment of:  (1)certain chronic and recurrent bacterial infections  (2) certain diseases with immunodeficiency like chronic granulomatous syndrome, job’s syndrme etc.  (3) autoimmune diseases like r.a., crohn’s disease, SLE.
  • 49.  OTHERS ARE:  Corynebacterium parvum  Tilorone  Inosiplex  Lipopolysaccharides  Dialyzable leukocyte extract