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Summary Lecture Notes Antibody Therapeutics & Diagnostics | Applied Biotechnology | KU Leuven | 2025/26

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Lecture notes from the Applied Biotechnology course at KU Leuven covering antibody therapeutics and diagnostics. The document covers the history of immunity and antibodies, molecular structure of antibodies, the adaptive immune system, therapeutic antibody indications (cancer, infectious diseases, neurology), and diagnostic applications including lateral flow tests and pregnancy tests. Essential for understanding monoclonal antibody development, market dynamics, and clinical applications—ideal for exam preparation and assignments in the Pharmaceutical Sciences program.

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Antibody therapeutics & diagnostics
Introduction

1. Market overview
Therapeutic antibodies
 First antibody in clinic: 1986
 Gaining importance
o Canonical antibodies = most popular
o Other formats: coupled to other drugs, multiple targets,
antibody fragments
 Indications
o Main indication = cancer
o Infectious diseases
o Neurology (difficult to reach the brain over the BBB ->
less approved antibodies but population of patients is
the same as the cancer patients’ population)
 >100 antibodies approved: many hit the same target
o Improvement of earlier versions
 Different administration route
 Lower immunogenicity

Example: adalimumab vs infliximab
Infliximab: approved before adalimumab  IV
Adalimumab: SC = more successful

o Combination therapies with antibodies: better to own
each component
o Lucrative market: “share a piece of the pie”
2. Brief history
Immunity
= state/ quality of being resistant to a particular infectious disease
or pathogen

1) General concept: 18th century
 Smallpox – lady Mary Wortley Montagu
Turkey: pus collected from mild cases  inoculating children
 protected
 Cow pox – Edward Jenner
Diary girls in contact with cow pox  protected
 Tetanus & diphtheria – Emil von Behring
Serum transfer  protected
Hypothesis: receptors that bind antigens + could activate the
complement pathway

, 2) Plasma B-cells involved in antibody generation
3) Clonal selection theory: a B-cell makes a single specific antibody
4) Molecular structure of antibodies
5) Köhler & Milstein (1975)
Method to generate monoclonal antibodies


Antibodies – name
Serum electrophoresis
- Albumin
- ⍺-, β, γ-globulins

Plasma from rabbits
immunized with
ovalbumin

γ-globulins peak decreases after incubation with ovalbumin:
disappearing proteins = immunoglobulins

3. Immune system




Adaptive/ specific immune system:

 Body challenged by foreign pathogen
 Macrophages engulf pathogens non-selectively & break them
down internally
 Proportion of macrophages (dendritic cells) present antigenic
fragments of pathogen to specific lymphocytes: helper T
lymphocytes (TH cells)
o Release cytokines
o Cytokines stimulate B-cells that produce antibodies
specific to antigen to divide and form clones (clonal
selection)
 Most of B-cell clones: short-lived plasma cells that produce
large quantities of specific antibody (2000/second (!))
 Small proportion of clones: differentiate into long-lived
memory B-cells

,Innate/ non-specific immune system:

 First line of defense against infection
 All components are present before the infection
o Function and efficiency does not change with repeated
exposure
o Not specific
 Components
o Physical barriers: e.g.;
- Skin: prevents pathogen penetration
- Bodily fluids (e.g., mucus, tears, saliva, …): collect and
clear pathogens
- Low pH in stomach
o Complement system (collaborates antibodies)
o White blood cells (macrophages, neutrophils, natural killer
cells, dendritic cells, …)
- Dendritic cells: antigen presenting cells: bridge between
innate and adaptive immune system ‘eats’ pathogen +
presents it to T-helper cell

, 1) Dendritic cell ‘eats’ pathogen -> presents it to T-helper cell
2) T-helper cell releases cytokines
3) Cytokines affect the other immune cells

4) B-cells displays antigen+antibody complex
5) The complex is internalized
6) Displayed
7) Recognized by TH cells




Slide 22-23; zie infectieziekten !!!!



Memory cells: long living + produce low levels of circulating antibodies
 Second infection: production of antibodies = faster + higher levels
 Pathogen cannot reproduce sufficient to cause disease
 Individual is said to be immune

Antibodies = most divers class of proteins
Antigen: antibody generators

4. Antibody structure
Y-shaped proteins (but flexible  needed to adapt to pathogen)
Dimers: left and right are identical


Fab domains
Antigen binding
S-S linked
Hinge region
Flexible region that
links CH1 and CH2
Fc domain
Effector function
S-S linked

 Sandwich of 2 β-sheets  each sheet antiparallel
 Loops between β-strands
o Folds = stable; rigid
o Loops = flexible
 Following N- to C-terminus: you jump from
one sheet to another through the loops
between them

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Subido en
11 de junio de 2026
Número de páginas
43
Escrito en
2025/2026
Tipo
RESUMEN

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