Hi everyone,

I just started my PhD in bioinformatics and specifically alternative splicing using RNA-seq, my background is computer science. I have two big issues at the moment:

1. Understanding specific graphs and results in papers
2. There are way many gene, isoform, function, cancer names ...

It's really hard to understand papers at the moment and I need to google many things ... I appreciate if you tell me how I can resolve those issues. I have some very basic questions like:

What is novel isoform?

What's the difference between novel transcripts and reference like transcripts?

cheers

DavidP

"Googling stuff" is pretty much standard operating procedure for everyone starting something new :P

A "novel isoform" is a transcript for a gene that hadn't been previously reported. A "reference transcript" is a transcript that has enough evidence supporting its existence to end up in a reference database, which are typically maintained by large groups such as Ensembl or Gencode.

Simple genomics courses in Coursera & EdX would be a great help to you. Of course, googling always helps. But the idea is that once you know the basics of genomics, pop. genetics then some nomenclature would be clear to you and then you would need to google only some terminologies.

Some courses: 1. https://www.coursera.org/specializations/computational-biology
2. https://www.coursera.org/specializations/data-structures-algorithms

As for question 2, check this Biostars post that gives you an updated list of courses in the field. The Ensembl help & documentation page, including our glossary could be a good place specially if you start using the Ensembl Gene Set, which is pretty thorough in annotating alternatively spliced transcripts, whether coding or otherwise. Once you have those concepts clearer, it may be easier to understand the graphs and results in the papers you read. You can also contact the authors of those papers you are not too sure about for further clarification. You can either email the corresponding author directly or better still tweet them. The latter will probably be more impactful as it's open and public to the community.

I was looking at a paper which compares some tools like MATS, they talk about factors like AUC and FDR. I know what they are but am confused how to relate it back to the tools!!!

thanks a lot guys.

I have another question. What is replicate data? paired or unpaired?

Many thanks everyone for all help so far.

I'm looking for some tools to first determine alternative splicing and then the event(s) such as: 1. Skipped exon (SE) 2. Alternate 3’ splice site (A3SS) 3. Alternate 5’ splice site (A5SS) 4. Mutually exclusive (MXE) 5. Intron retention (IR)

Lots of people have given excellent answers and suggestions for online resources. I would also highly recommend taking some appropriate courses at your institution. Most PhD programs require at least a few courses for you to take, usually determined by your committee and department. If your background is in CS and you are now in a department or group that is primarily biology, you should take some appropriate courses. Or even just audit some courses. The biology of what is happening informs many of the design decisions of experiments, which carries on downstream into how those results are analysed. It's very common for people without biology backgrounds to analyse these sorts of datasets badly because they don't understand what is happening in those datasets.

I think I need to read more about Probability and Statistics, things like negative binomial (NB) distribution, generalized linear model (GLM) and Normalizing for composition biases. I need lots of ground work there, is there a good course or web resource?

hey guys, which bioconducter you reckon for analyzing different types of alternative splicing?