Add to ORKGThis project uses bioinformatics protocols to explore the impacts of non-synonymous mutations (nsSNPs) in proteins associated with diseases, including germline, rare diseases and somatic diseases such as cancer. New approaches were explored for determining the impacts of disease-associated mutations on protein structure and function. Whilst this work has mainly concentrated on the analysis of cancer mutations, the methods developed are generic and could be applied to analysing other types of disease mutations. Different types of disease-causing mutations have been studied including germline diseases, somatic cancer mutations in oncogenes and tumour-suppressors, along with known activating and inactivating mutations in kinases. The proximity...
Abstract Background Discriminating driver mutations from the ones that play no role in cancer is a s...
Genomics and genome screening are proving central to the study of cancer. However, a good appreciati...
We have investigated the properties of three sets of human missense genetic variations: cancer somat...
We have investigated the properties of three sets of human missense genetic variations: cancer somat...
A major challenge in cancer genomics is uncovering genes with an active role in tumorigenesis from a...
With the advent of Next Generation Sequencing the identification of mutations in the genomes of heal...
Background: Recent advances in sequencing technologies enable the large-scale identification of gene...
Genome sequencing efforts, coupled with technological advances and cost reductions, have led to the ...
Protein kinases are the most common protein domains implicated in cancer, where somatically acquired...
Protein kinases are the most common protein domains implicated in cancer, where somatically acquired...
A central goal of cancer research is to discover and characterize the functional effects of mutated ...
SummaryMost known disease-associated mutations are missense mutations involving changes of amino aci...
Understanding and linking at the molecular level a disease phenotype to a specific genotype often re...
Large-scale tumor sequencing projects enabled the identification of many new cancer gene candidates ...
Genome sequencing efforts, coupled with technological advances and cost reductions, have led to the ...
Abstract Background Discriminating driver mutations from the ones that play no role in cancer is a s...
Genomics and genome screening are proving central to the study of cancer. However, a good appreciati...
We have investigated the properties of three sets of human missense genetic variations: cancer somat...
We have investigated the properties of three sets of human missense genetic variations: cancer somat...
A major challenge in cancer genomics is uncovering genes with an active role in tumorigenesis from a...
With the advent of Next Generation Sequencing the identification of mutations in the genomes of heal...
Background: Recent advances in sequencing technologies enable the large-scale identification of gene...
Genome sequencing efforts, coupled with technological advances and cost reductions, have led to the ...
Protein kinases are the most common protein domains implicated in cancer, where somatically acquired...
Protein kinases are the most common protein domains implicated in cancer, where somatically acquired...
A central goal of cancer research is to discover and characterize the functional effects of mutated ...
SummaryMost known disease-associated mutations are missense mutations involving changes of amino aci...
Understanding and linking at the molecular level a disease phenotype to a specific genotype often re...
Large-scale tumor sequencing projects enabled the identification of many new cancer gene candidates ...
Genome sequencing efforts, coupled with technological advances and cost reductions, have led to the ...
Abstract Background Discriminating driver mutations from the ones that play no role in cancer is a s...
Genomics and genome screening are proving central to the study of cancer. However, a good appreciati...
We have investigated the properties of three sets of human missense genetic variations: cancer somat...