100% de satisfacción garantizada Inmediatamente disponible después del pago Tanto en línea como en PDF No estas atado a nada
logo-home
Buscado previamente por ti
Buscado previamente por ti
logo
Summary Antivirals and Antibacterials $11.65   Añadir al carrito
Navegar rápidamente a
Vista previa
  2.  
  3. GCSE
  4.  
  5. GCSE
  6.  
  7. Biology

Resumen

Summary Antivirals and Antibacterials

1 revisar
 20 vistas  0 compra
  • Grado
  • Biology
  • Institución
  • GCSE

A summary of common types of antibiotics and antivirals

Vista previa 2 fuera de 10  páginas

Información del documento

  • 4 de julio de 2021
  • 10
  • 2020/2021
  • Resumen

Temas

  • antibiotics
  • antivirals
  • biology
  • medicines
  • medicine
  • drug
  • pharmacy
  • pharmacology

Escuela, estudio y materia

  • GCSE
  • GCSE
  • Biology
  • 2
Todos documentos para esta materia (848)

1  revisar

review-writer-avatar

Por: rubana8 • 1 año hace

Vendedor

avatar-seller
anmoll

Comentarios recibidos

Vista previa del contenido

Discovery and Design of Drugs
Choosing a drug target

• Drug targets – agonist, antagonist for receptor or enzyme inhibitor
• The more selective and specific, the better the drug as there’s a less chance of interaction with different
targets (also means less side effects)
• Ideally, enzyme inhibition needs to be specific to a single enzyme

Identifying a bioassay

• The bioassay should be simple, quick and relevant
• In-vitro tests – isolated cells, tissues. This is preferred as it’s cheap and easy to carry out
• In-vivo tests – in animals
• High throughput screening – involves robotics and miniaturisation of in-vitro tests. Many compounds
are automatically tested against different targets. Positive hits have activity in 30μM-1nM but there can
be false positive hits too.

Finding a lead compound

• Natural: sources include plants (salicylic acid, nicotine, galantamine), microorganisms (penicillin,
cephalosporins, aminoglycosides), marine sources (antivirals, anticancer drugs), animals (Botox).
Typically isolated as fermentation broths, plant extracts or animal fluids
• Synthetics: typically, small molecules made from a variety of sources
• Biologics: natural products, recombinant products
• Methods = starting from a natural ligand, combinatorial and parallel synthesis, computer aided design of
leads, serendipity, computerised searching, fragment-based lead discovery

Properties of lead compounds

• Lipinski’s rule of 5 – molecular weight <500amu, <5 HBD groups, <10 HBA groups, calculated logP of <5
(measure of hydrophobicity)
• Typically need to increase the size and hydrophobicity, have more aromatic rings and/or HBAs and lastly
consider ligand binding/efficiency of the lead

Optimising target interactions

• There are various aims for drug design to obtain the final drug – good selectivity, easily synthesised,
chemically stable, non-toxic, pharmacodynamically stable, minimal side effects
• Pharmacodynamic properties optimise the interaction between the drug and target to obtain
• Pharmacokinetic properties to increase the ability to reach the target
• PD and PK properties should have equal priority in influencing drug design strategy

Structure-activity relationships (SARs)

• Aim: to identify which parts of the molecule are essential for activity
• If crystals can be grown of the lead in the binding site, then the x-ray crystallography structure can be
solved

, Drug Discovery Advances
1. Receptor Structure Determination
• X-ray crystallography can determine the 3D structure:
o High-resolution detail (atomic resolution)
o Bond distances, angles, stereochemistry and configuration
o Proteins or protein-drug complexes (if co-crystallised)
• Many receptors are membrane proteins. This means it’s difficult to identify 3D structures as there
are isolation problems since these are found within the membranes

Applications of crystal structure in drug design
1. Priori drug design (aka de novo) – crystal structure of the target is used to create the initial
structurally novel lead compound with the aid of molecular graphics
2. Posteriori analysis – combines existing structure-activity knowledge with the x-ray structure and
proposes design improvements

Example: HIV protease (HIV-1 PR) Inhibitors
• X-ray studies of recombinant expressed HIV-1 PR suggest a substrate binding site (priori).
• The crystal structure of a complex of an inhibitor bound to HIV-1 PR was determined as was a
close contact map detailing hydrogen-bonding interactions.
• Improvements in future inhibitor design (posteriori).
• Currently, there are several HIV protease inhibitors in the market – ritonavir, saquinavir

2. Multi-dimensional NMR
 Disadvantage of x-ray = the structure is not under the biological condition in solution
✓ NMR is conducted in solution and provides fast, structural information

3. Bioinformatics
• Information technology and innovative software is applied to genomics and molecular biology as the
molecules and processes are studied in silico (with computers)

Molecular Modelling
• Software offers techniques beyond traditional graphs.
• The properties of molecules can be visualised:
o Mapped onto the surface of the molecule using colours
o Hydrophobicity can be mapped onto the surface
o Non-physical properties i.e. how highly conserved the residue is or similarity to another
protein can be visualised

Computational Chemistry
• Required for accurate modelling or molecular behaviour.
• Properties should be calculated and assigned and should accurately estimate experiment
• Primary computations = energy (thermodynamics) and kinetics
• Methods for calculations = quantum mechanics or molecular mechanics
o Quantum mechanics – derived from the quantum theory, these calculations are based on
the extended Schrodinger equation that relates the motion of electrons and nucleus to the
potential energy. However, this is time-consuming and resource intensive. Therefore,
approximations are used: semi-empirical methods.
o Molecular mechanics – based on simple empirical approximations, here the focus is on the
motion of the molecules. The energy of the molecule is calculated from the bond angle and
other interatomic interaction energies. The process is fast but less accurate compared to
quantum mechanics.

Los beneficios de comprar resúmenes en Stuvia estan en línea:

Garantiza la calidad de los comentarios

Garantiza la calidad de los comentarios

Compradores de Stuvia evaluaron más de 700.000 resúmenes. Así estas seguro que compras los mejores documentos!

Compra fácil y rápido

Compra fácil y rápido

Puedes pagar rápidamente y en una vez con iDeal, tarjeta de crédito o con tu crédito de Stuvia. Sin tener que hacerte miembro.

Enfócate en lo más importante

Enfócate en lo más importante

Tus compañeros escriben los resúmenes. Por eso tienes la seguridad que tienes un resumen actual y confiable. Así llegas a la conclusión rapidamente!

Preguntas frecuentes

What do I get when I buy this document?

You get a PDF, available immediately after your purchase. The purchased document is accessible anytime, anywhere and indefinitely through your profile.

100% de satisfacción garantizada: ¿Cómo funciona?

Nuestra garantía de satisfacción le asegura que siempre encontrará un documento de estudio a tu medida. Tu rellenas un formulario y nuestro equipo de atención al cliente se encarga del resto.

Who am I buying this summary from?

Stuvia is a marketplace, so you are not buying this document from us, but from seller anmoll. Stuvia facilitates payment to the seller.

Will I be stuck with a subscription?

No, you only buy this summary for $11.65. You're not tied to anything after your purchase.

Can Stuvia be trusted?

4.6 stars on Google & Trustpilot (+1000 reviews)

45,681 summaries were sold in the last 30 days

Founded in 2010, the go-to place to buy summaries for 14 years now

Empieza a vender
$11.65
  • (1)
  Añadir