Chapter 4: Protein Function Back To Chapter

4.1: Ligand Binding Sites

TABLE OF
CONTENTS

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Chapter 1: DNA, Cells, and Evolution

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1.1: The DNA Helix
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1.2: The Central Dogma
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1.3: Prokaryotic cells
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1.4: Eukaryotic Compartmentalization
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1.5: The Tree of Life - Bacteria, Archaea, Eukaryotes
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1.6: Mutations
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1.7: Gene Evolution - Fast or Slow?
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1.8: Genome Size and the Evolution of New Genes
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1.9: Gene Families
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1.10: Types of Genetic Transfer Between Organisms

Chapter 2: Biochemistry of the Cell

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2.1: The Periodic Table and Organismal Elements
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2.2: Functional Groups
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2.3: Polymers
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2.4: What are Lipids?
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2.5: Structure of Lipids
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2.6: Chemistry of Carbohydrates
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2.7: Nucleic Acids
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2.8: Intermolecular Forces
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2.9: Noncovalent Attractions in Biomolecules
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2.10: pH
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2.11: Hydrolysis of ATP

Chapter 3: Protein Structure

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3.1: What are Proteins?
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3.2: Protein Organization
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3.3: Protein Folding
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3.4: Protein Families
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3.5: Conservation of Protein Domains Over Different Proteins
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3.6: Globular and Fibrous Proteins
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3.7: Intrinsically Disordered Proteins
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3.8: Protein Complex Assembly
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3.9: Conjugated Proteins
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3.10: Amyloid Fibrils
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3.11: Antibody Structure

Chapter 4: Protein Function

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4.1: Ligand Binding Sites
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4.2: Protein-protein Interfaces
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4.3: Conserved Binding Sites
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4.4: The Equilibrium Binding Constant and Binding Strength
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4.5: Cofactors and Coenzymes
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4.6: Allosteric Regulation
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4.7: Ligand Binding and Linkage
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4.8: Allosteric Proteins-ATCase
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4.9: Cooperative Allosteric Transitions
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4.10: Phosphorylation
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4.11: Protein Kinases and Phosphatases
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4.12: GTPases and their Regulation
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4.13: Covalently Linked Protein Regulators
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4.14: Protein Complexes with Interchangeable Parts
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4.15: Mechanical Protein Functions
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4.16: Structural Protein Function
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4.17: Protein Networks

Chapter 5: DNA and Chromosome Structure

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5.1: DNA Packaging
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5.2: DNA as a Genetic Template
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5.3: Organization of Genes
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5.4: Chromosome Structure
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5.5: Chromosome Replication
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5.6: The Nucleosome
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5.7: The Nucleosome Core Particle
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5.8: Nucleosome Remodeling
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5.9: Chromatin Packaging
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5.10: Karyotyping
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5.11: Position-effect Variegation
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5.12: Histone Modification
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5.13: Spreading of Chromatin Modifications
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5.14: Lampbrush Chromosomes
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5.15: Polytene Chromosomes
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5.16: Histone Variants at the Centromere
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5.17: Inheritance of Chromatin Structures
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5.18: Euchromatin
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5.19: Heterochromatin
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5.20: Chromatin Position Affects Gene Expression

Chapter 6: DNA Replication

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6.1: Replication in Prokaryotes
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6.2: Replication in Eukaryotes
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6.3: DNA Base Pairing
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6.4: The DNA Replication Fork
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6.5: Proofreading
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6.6: Lagging Strand Synthesis
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6.7: DNA Helicases
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6.8: Single-Strand DNA Binding Proteins
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6.9: The Replisome
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6.10: Mismatch Repair
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6.11: DNA Topoisomerases
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6.12: Telomeres and Telomerase
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6.13: Non-nuclear Inheritance
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6.14: Animal Mitochondrial Genetics
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6.15: Comparing Mitochondrial, Chloroplast, and Prokaryotic Genomes
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6.16: Export of Mitochondrial and Chloroplast Genes

Chapter 7: DNA Repair and Recombination

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7.1: Overview of DNA Repair
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7.2: Base Excision Repair
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7.3: Long-patch Base Excision Repair
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7.4: Nucleotide Excision Repair
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7.5: Translesion DNA Polymerases
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7.6: Fixing Double-strand Breaks
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7.7: DNA Damage can Stall the Cell Cycle
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7.8: Homologous Recombination
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7.9: Restarting Stalled Replication Forks
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7.10: Gene Conversion
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7.11: Overview of Transposition and Recombination
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7.12: DNA-only Transposons
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7.13: Retroviruses
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7.14: LTR Retrotransposons
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7.15: Non-LTR Retrotransposons
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7.16: Conservative Site-specific Recombination and Phase Variation

Chapter 8: Transcription: DNA to RNA

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8.1: What is Gene Expression?
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8.2: RNA Structure
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8.3: RNA Stability
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8.4: Bacterial RNA Polymerase
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8.5: Bacterial Transcription
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8.6: Types of RNA
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8.7: Transcription
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8.8: Transcription Factors
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8.9: Eukaryotic RNA Polymerases
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8.10: Transcription Initiation
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8.11: RNA Polymerase II Accessory Proteins
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8.12: Transcription Elongation Factors
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8.13: Pre-mRNA Processing
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8.14: RNA Splicing
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8.15: Alternative RNA Splicing
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8.16: Chromatin Structure Regulates pre-mRNA Processing
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8.17: Nuclear Export of mRNA
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8.18: Ribosomal RNA Synthesis
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8.19: Transfer RNA Synthesis
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8.20: The Nucleolus
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8.21: Additional Subnuclear Structures

Chapter 9: Translation: RNA to Protein

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9.1: Translation
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9.2: tRNA Activation
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9.3: Ribosomes
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9.4: Improving Translational Accuracy
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9.5: Initiation of Translation
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9.6: Termination of Translation
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9.7: Nonsense-mediated mRNA Decay
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9.8: Molecular Chaperones and Protein Folding
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9.9: The Proteasome
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9.10: Regulated Protein Degradation
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9.11: Proteins: From Genes to Degradation

Chapter 10: Gene Expression

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10.1: Cell-Specific Gene Expression
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10.2: Regulation of Expression Occurs at Multiple Steps
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10.3: Cis-regulatory Sequences
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10.4: Cooperative Binding of Transcription Regulators
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10.5: Prokaryotic Transcriptional Activators and Repressors
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10.6: Operons
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10.7: The Eukaryotic Promoter Region
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10.8: Co-activators and Co-repressors
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10.9: Eukaryotic Transcription Activators
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10.10: Eukaryotic Transcription Inhibitors
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10.11: Combinatorial Gene Control
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10.12: Induced Pluripotent Stem Cells
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10.13: Master Transcription Regulators
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10.14: Epigenetic Regulation
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10.15: Genomic Imprinting and Inheritance

Chapter 11: Additional Roles of RNA

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11.1: Transcription Attenuation in Prokaryotes
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11.2: Riboswitches
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11.3: RNA Editing
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11.4: Regulated mRNA Transport
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11.5: Leaky Scanning
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11.6: mRNA Stability and Gene Expression
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11.7: RNA Interference
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11.8: MicroRNAs
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11.9: siRNA - Small Interfering RNAs
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11.10: piRNA - Piwi-interacting RNAs
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11.11: CRISPR and crRNAs
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11.12: lncRNA - Long Non-coding RNAs
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11.13: Ribozymes
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11.14: Conditions on Early Earth

Chapter 12: Mendelian Genetics

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12.1: Punnett Squares
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12.2: Monohybrid Crosses
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12.3: Dihybrid Crosses
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12.4: Trihybrid Crosses
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12.5: Law of Independent Assortment
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12.6: Chi-square Analysis
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12.7: Pedigree Analysis
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12.8: Incomplete Dominance
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12.9: Lethal Alleles
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12.10: Polygenic Traits
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12.11: Background and Environment Affect Phenotype
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12.12: X and Y Chromosomes
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12.13: The Y Chromosome Determines Maleness
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12.14: The Ratio of X Chromosome to Autosomes
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12.15: X-linked Traits
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12.16: Sex Linked Disorders
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12.17: Dosage Compensation
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12.18: X-inactivation
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12.19: Multiple Allele Traits
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12.20: Blood Types
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12.21: Blood Transfusion and Agglutination

Chapter 13: Genomes and Evolution

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13.1: Evolutionary Relationships through Genome Comparisons
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13.2: Genome Copying Errors
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13.3: Phylogenetic Trees
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13.4: Synteny and Evolution
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13.5: Multi-species Conserved Sequences
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13.6: Gene Duplication and Divergence
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13.7: Exon Recombination
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13.8: Comparing Copy Number Variations and SNPs

Chapter 14: Cell Signaling Pathways

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14.1: What is Cell Signaling?
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14.2: Autocrine Signaling
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14.3: Paracrine Signaling
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14.4: Endocrine Signaling
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14.5: Intracellular Signaling Cascades
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14.6: Notch Signaling Pathway
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14.7: Canonical Wnt Signaling Pathway
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14.8: Non-Canonical Wnt Signaling Pathways
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14.9: Hedgehog Signaling Pathway
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14.10: NF-κB-dependent Signaling Pathway
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14.11: Internal Receptors
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14.12: Circadian Rhythms and Gene Regulation
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14.13: G-protein Coupled Receptors
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14.14: What are Second Messengers?
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14.15: Enzyme-linked Receptors

Chapter 15: Studying DNA and RNA

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15.1: Recombinant DNA
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15.2: DNA Isolation
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15.3: Restriction Enzymes
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15.4: DNA Agarose Gel Electrophoresis
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15.5: Labeling DNA Probes
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15.6: Southern Blot
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15.7: DNA Microarrays
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15.8: Complementary DNA
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15.9: FISH - Fluorescent In-situ Hybridization
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15.10: PCR - Polymerase Chain Reaction
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15.11: Real Time RT-PCR
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15.12: RACE - Rapid Amplification of cDNA Ends
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15.13: Sanger Sequencing
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15.14: Maxam-Gilbert Sequencing
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15.15: Next-generation Sequencing
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15.16: RNA-seq
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15.17: Genome Annotation and Assembly

Chapter 16: Analyzing Gene Expression and Function

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16.1: In vitro Mutagenesis
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16.2: Genetic Screens
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16.3: Test Cross
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16.4: Complementation Tests
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16.5: Epistasis Analysis
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16.6: Single Nucleotide Polymorphisms-SNPs
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16.7: Genome-wide Association Studies-GWAS
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16.8: Bacterial Transformation
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16.9: Transgenic Organisms
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16.10: Reproductive Cloning
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16.11: CRISPR
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16.12: Experimental RNAi
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16.13: Reporter Genes
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16.14: In-situ Hybridization
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16.15: Chromatin Immunoprecipitation- ChIP
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16.16: Synthetic Biology
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16.17: Ribosome Profiling
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16.18: Transgenic Plants
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16.19: Gene Therapy

Chapter 17: Cell Proliferation

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17.1: What is the Cell Cycle?
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17.2: Interphase
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17.3: The Cell Cycle Control System
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17.4: Positive Regulator Molecules
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17.5: Inhibition of Cdk Activity
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17.6: S-Cdk Initiates DNA Replication
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17.7: M-Cdk Drives Transition Into Mitosis
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17.8: Mitogens and the Cell Cycle
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17.9: Replicative Cell Senescence
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17.10: Abnormal Proliferation
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17.11: Cells Coordinate Growth and Proliferation

Chapter 18: Cell Division

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18.1: Mitosis and Cytokinesis
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18.2: Duplication of Chromatin Structure
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18.3: Cohesins
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18.4: Condensins
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18.5: The Mitotic Spindle
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18.6: Centrosome Duplication
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18.7: Microtubule Instability
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18.8: Spindle Assembly
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18.9: Attachment of Sister Chromatids
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18.10: Forces Acting on Chromosomes
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18.11: Separation of Sister Chromatids
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18.12: The Spindle Assembly Checkpoint
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18.13: Anaphase A and B
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18.14: Anaphase Promoting Complex
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18.15: The Contractile Ring
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18.16: Determining the Plane of Cell Division
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18.17: The Phragmoplast
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18.18: Distribution of Cytoplasmic Content

Chapter 19: Meiosis

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19.1: What is Meiosis?
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19.2: Meiosis I
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19.3: Meiosis II
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19.4: Meiosis vs. Mitosis
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19.5: Crossing over
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19.6: Nondisjunction

Chapter 20: Cancer

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20.1: What is Cancer?
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20.2: Cancers Originate from Somatic Mutations in a Single Cell
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20.3: Tumor Progression
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20.4: Adaptive Mechanisms in Cancer Cells
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20.5: The Tumor Microenvironment
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20.6: Metastasis
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20.7: Cancer-Critical Genes I: Proto-oncogenes
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20.8: Cancer-Critical Genes II: Tumor Suppressor Genes
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20.9: Loss of Tumor Suppressor Gene Functions
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20.10: The Retinoblastoma Gene
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20.11: The Ras Gene
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20.12: mTOR Signaling and Cancer Progression
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20.13: Mechanisms of Retrovirus-induced Cancers
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20.14: Rous Sarcoma Virus (RSV) and Cancer
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20.15: Cancer Stem Cells and Tumor Maintenance
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20.16: Mouse Models of Cancer Study
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20.17: Cancer Prevention
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20.18: Cancer Therapies
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20.19: Targeted Cancer Therapies
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20.20: Treatment Resistant Cancers
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20.21: Combination Therapies and Personalized Medicine

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Ligand Binding Sites

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4.2: Protein-protein Interfaces

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TRANSCRIPT

Activities of most proteins depend on their interactions with other molecules or ions, known as ligands. Although ligands are able to bind to proteins, not every ligand binds to every protein.

Instead, a ligand binds only to a specific region on a protein’s surface called the binding site. But how do ligand binding sites ensure selectivity when proteins sit in a mixed ligand soup?

The particular arrangement of amino acids in a protein forms a complementary binding site on its surface for a specific ligand. However, complementary shapes are not enough for ligand binding.

Chemical interactions hold the ligand and the protein together. Generally, these interactions are non-covalent, reversible, and weak. Therefore, many of these interactions need to occur simultaneously during ligand binding.

For example, the larger the surface area of interaction, the more Van der Waals interactions can happen. These forces work best for large ligands. For others, the specific conformation of the binding site enables hydrogen bonding or electrostatic interactions.

But if the ligand binding site can form hydrogen bonds, why doesn’t it form hydrogen bonds with the water in its surroundings? The answer lies in the shape of the ligand binding site.

As an example, in this protein, the orientation of the amino acids forms a cavity, which restricts the access of water molecules. For individual water molecules, entering the cavity is energetically unfavorable as they have to break their hydrogen bonds with other water molecules.

Yet, the ligand will readily form hydrogen bonds with the polar amino acids in the binding site because the specific protein-ligand interactions are energetically more favorable than their interactions with water molecules.

Polar amino acids also form electrostatic interactions with a ligand. For instance, the negatively-charged glutamate in this binding site attracts the positively-charged ligand. A mutation in this sequence that turns this negatively charged glutamate into a positively charged lysine eliminates ligand binding.

Taken together, the exact sequence and orientation of the amino acids relative to each other determine the chemical reactivity and selectivity of the ligand binding site.

4.1: Ligand Binding Sites

Proteins are dynamic macromolecules that carry out a wide variety of essential processes; however, the activities of most proteins depend on their interactions with other molecules or ions, known as ligands.

Protein-ligand interactions are quite specific; even though numerous potential ligands surround a cellular protein at any given time, only a particular ligand can bind to that protein. Moreover, a ligand binds only to a dedicated area on the surface of the protein, known as the ligand-binding site. The specificity of a protein’s ligand-binding site is determined by the arrangement of its amino acid chain which gives the area its shape and chemical reactivity. Hence, a ligand-binding site provides a complementary shape to its ligand and keeps the ligand in place via chemical interactions. These chemical interactions are often noncovalent; however, since these interactions are reversible and weak, many of these interactions need to occur simultaneously to hold the protein and the ligand together.

Research that elucidates interaction mechanisms at ligand binding sites generally involves in silico modeling and in vitro approaches. In silico modeling uses computers to compare previously known protein structures and evolutionary data to make predictions to determine the optimal binding shape and energy state of the protein-ligand complex. In vitro approaches compliment in silico predictions by providing evidence for ligand binding through binding and kinetic assays in the laboratory. Ligand binding research is important for understanding the functions of proteins and how they perform specific cellular processes in both healthy, as well as in diseased conditions. For instance, certain genetic conditions and cancers can alter the sequence of a protein, ultimately affecting its ability to bind a ligand. In addition, this research also allows scientists to design drugs with specific interactions and minimal side effects by targeting the ligand-binding site of an implicated protein.

Suggested Reading

Chapter 1: DNA, Cells, and Evolution

Chapter 2: Biochemistry of the Cell

Chapter 3: Protein Structure

Chapter 4: Protein Function

Chapter 5: DNA and Chromosome Structure

Chapter 6: DNA Replication

Chapter 7: DNA Repair and Recombination

Chapter 8: Transcription: DNA to RNA

Chapter 9: Translation: RNA to Protein

Chapter 10: Gene Expression

Chapter 11: Additional Roles of RNA

Chapter 12: Mendelian Genetics

Chapter 13: Genomes and Evolution

Chapter 14: Cell Signaling Pathways

Chapter 15: Studying DNA and RNA

Chapter 16: Analyzing Gene Expression and Function

Chapter 17: Cell Proliferation

Chapter 18: Cell Division

Chapter 19: Meiosis

Chapter 20: Cancer

4.1: Ligand Binding Sites

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