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MD Pharmacology NMC syllabus ~5 min read Recent advances last updated on 2026-07-02

Screening of Immunomodulatory Drugs

Experimental evaluation of immunomodulatory & antiarthritic drugs — humoral, cell-mediated, reticuloendothelial and arthritis models

Definition, rationale & the immune targets assays probe

  • Definition — Immunomodulator screening is the preclinical bench-and-animal battery that detects whether a test compound suppresses (immunosuppressant) or augments/restores (immunostimulant) an immune response, and grades its potency against reference standards.
  • The immune response is functionally partitioned; each arm has its own validated read-out, and a screening cascade typically samples ≥ 3 arms to profile a compound:
    • Humoral (antibody-mediated) — B-cell/plasma-cell output → plaque-forming-cell (PFC) assay to SRBC; haemagglutination antibody titre.
    • Cell-mediated immunity (CMI) — T-cell effector function → delayed-type-hypersensitivity (DTH) footpad swelling; mitogen-/MLR-driven lymphocyte proliferation; leucocyte-migration-inhibition.
    • Non-specific / innate & reticuloendothelial (RES) — macrophage/neutrophil oxidative burst & phagocytosis → chemiluminescence, carbon-clearance phagocytic index, neutrophil-adhesion.
    • Effector hypersensitivity — mast-cell/IgE-mediated reactions (anaphylaxis, Arthus) as models of drug-modifiable allergic inflammation.
  • Why both tiers — In-vitro assays (enzyme, cell-culture proliferation) allow high-throughput lead selection with tiny compound amounts; whole-animal models test the compound in an intact, cytokine-networked immune system that no single cell assay reproduces.
  • Translation caveat — Mouse models of inflammatory/immune disease correlate poorly with human disease; the trend is toward rat models for superior pain behaviour and surgical tractability.
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Screening Immunomodulatory Drugs

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