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Lecture notes

L7 - Engineering Antibody Alternatives

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Extensive notes for module 6BBB0333 Protein Structure & Design lecture 7 on engineering antibody alternatives. Notes provide simply written explanations to lecture content, featuring many images to illustrate and break down the complexity of this module. I was awarded a first-class for this module and solely relied on these notes to prepare for my exam.

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Uploaded on
February 19, 2025
Number of pages
14
Written in
2023/2024
Type
Lecture notes
Professor(s)
Mark pfuhl
Contains
All classes

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6BBB0333


L7 – Engineering Antibody Alternatives

Introduction

- Antibodies fulfil numerous roles both in biology - as evolution intended - as well as in
research, medicine and general biotech applications (e.g. measuring protein concentration in
ELISA)
- For a multitude of reasons the search for alternatives is going on for some time leading to an
interesting group of molecules.
- One of the most recent and most promising examples is a group of proteins called ‘Adhirons’
or ‘Affimers’ that tick many boxes expected for such replacements which could make them
very interesting in the future.
- They are a fairly recent development with the first publication from 2014.



An affirmer




- Beta-alpha mixed protein
- 4 beta strands wrapping around a long alpha helix
- Very compact, stable fold (important for design)



Antibody types




- Most popular IgG – used a lot in biotech
- Building blocks are heavy and light chains

, 6BBB0333


o Based on beta sandwich structures
- Combined in a myriad of ways – small IgG, dimerised IgA (additional protein to make dimer),
IgE (extension of constant heavy chain – 3 instead of 2), IgM (5 – can bind 5 antigens in one
go)



Antibody architecture




- Light chains
o Two immunoglobulin-type beta sandwich domains
- Heavy chain (twice the size of LC) – possibly an evolutionary gene duplication event between
the two different chains
- Heavy chain has constant and variable region
- Variable region is very first domain of either heavy or light chain
- It is responsible for antigen binding (occurs at tip of whole structure)
- Very small potion of whole protein is interacting with antigen
o Large size is downside of proteins
- In the native environment (IS) it makes sense to have a large protein:
o While one portion is relevant for antigen binding (tip)…
o the other portion (effector region) is responsible for binding to antigen receptor on
immune cells
o Combination of this triggers immune response so both parts are essential BUT
- If you want to use antibodies outside of cellular/physiological context, this extra (bottom)
portion is not necessary and we can do away with it
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