Tweet
I am a newer for NGS. Recently I got 8 samples of NGS data from the Solid 5500xl. The average depth is about 10x, some maybe deeper. All of the samples are sporadic. People who has this kind of disease will die before they grow up. So lots of evidences make us believe that this kind of disease should be a de novo mutation. Which strategy or strategies should I use that could help me find the right gene? Thank you very much!
-
-
Are the samples from related individuals? -
Is it whole genome, exome, panels? Do you have reads or alignments or variants?Comment
-
They don't have any relationship with each other.Comment
-
We did the whole exon sequence by the solid 5500xl.Comment
-
In brief, align to reference genomes, human, I guess, then call SNPs. Best case, you are looking for a gene where all your samples have SNPs which cause highly deleterious changes to the protein. If your samples are not related, they probably won't all share the exact same mutation.
If you don't have that, you'll have to think a little harder. Maybe there are a few genes mutated in the same pathway? Maybe you have a CNV? It's always possible that your mutation is not even in the exome, in which case, your data won't show it.Comment
-
First of all, thank you very much for your guidance! We have checked the mutations which all 8 samples shared. But we didn't find any reasonable gene for our case. We also checked the CNV before we did the NGS. As you said, maybe there are a few genes mutated in the same pathway, but how could we annotate this? Which software could we use to analysis this ? Thank you again!Comment
-
Let's assume this is a one-or-two-gene disorder, since otherwise, most methodologies just won't work.
It's unreasonable to expect unrelated people to share a mutation. More likely, the related affecteds have a homozygous mutation in the same genes(s), due to inbreeding, which is highly probable for fatal genetic conditions. In this case it is best to sequence related individuals and find genes in which the unaffecteds have heterozygous mutations, but the affecteds have homozygous mutations.
One way to isolate responsible genes is to sequence multiple generations of related individuals (like great-grandparents, grandparent, parents/aunts/uncles, siblings/cousins, etc), and use software to determine inheritance. You don't even need sequencing for most of them; a cheaper SNP array is fine. This will allow you to isolate the genes (or areas) that are unique from the rest of the family (due to crossover events) and thus may be causing problems. Then, armed with the most probable locations, you can examine the affecteds' sequences in detail to determine the problem.Comment
-
At the intersection of cytogenetics and genomics lies the exciting field of cytogenomics. It focuses on studying chromosomes at a molecular scale, involving techniques that analyze either the whole genome or particular DNA sequences to examine variations in structure and behavior at the chromosomal or subchromosomal level. By integrating cytogenetic techniques with genomic analysis, researchers can effectively investigate chromosomal abnormalities related to diseases, particularly...09-26-2023, 06:26 AM -
Cancer research has been transformed through numerous molecular techniques, with RNA sequencing (RNA-seq) playing a crucial role in understanding the complexity of the disease. Maša Ivin, Ph.D., Scientific Writer at Lexogen, and Yvonne Goepel Ph.D., Product Manager at Lexogen, remarked that “The high-throughput nature of RNA-seq allows for rapid profiling and deep exploration of the transcriptome.” They emphasized its indispensable role in cancer research, aiding in biomarker...09-07-2023, 11:15 PM -
Ribonucleic acid (RNA) represents a range of diverse molecules that play a crucial role in many cellular processes. From serving as a protein template to regulating genes, the complex processes involving RNA make it a focal point of study for many scientists. This article will spotlight various methods scientists have developed to investigate different RNA subtypes and the broader transcriptome.
Whole Transcriptome RNA-seq
Whole transcriptome sequencing...08-31-2023, 11:07 AM
Comment