BOL: Related items

Figeno: Tool for plotting sequencing data along genomic coordinates.

LEGE — Tue, 17 Sep 2024 02:28:15 -0500

Tool for plotting sequencing data along genomic coordinates.

FIGENO is a
  FIGure
    GENerator
for GENOmics

With figeno, you can plot various types of sequencing data along genomic coordinates. Video overview: https://www.youtube.com/watch?v=h1cBeXoSYTA.

Address of the bookmark: https://github.com/CompEpigen/figeno

Import R Data

Abhimanyu Singh — Wed, 12 Jul 2017 08:30:46 -0500

It is often necessary to import sample textbook data into R before you start working on your homework.

Excel File

Quite frequently, the sample data is in Excel format, and needs to be imported into R prior to use. For this, we can use the function read.xls from the gdata package. It reads from an Excel spreadsheet and returns a data frame. The following shows how to load an Excel spreadsheet named "mydata.xls". This method requires Perl runtime to be present in the system.

> library(gdata)                   # load gdata package
> help(read.xls)                   # documentation
> mydata = read.xls("mydata.xls")  # read from first sheet

Alternatively, we can use the function loadWorkbook from the XLConnect package to read the entire workbook, and then load the worksheets with readWorksheet. The XLConnect package requires Java to be pre-installed.

> library(XLConnect) # load XLConnect package
> wk = loadWorkbook("mydata.xls")
> df = readWorksheet(wk, sheet="Sheet1")

Minitab File

If the data file is in Minitab Portable Worksheet format, it can be opened with the function read.mtp from the foreign package. It returns a list of components in the Minitab worksheet.

> library(foreign)                 # load the foreign package
> help(read.mtp)                   # documentation
> mydata = read.mtp("mydata.mtp")  # read from .mtp file

SPSS File

For the data files in SPSS format, it can be opened with the function read.spss also from the foreign package. There is a "to.data.frame" option for choosing whether a data frame is to be returned. By default, it returns a list of components instead.

> library(foreign) # load the foreign package
> help(read.spss) # documentation
> mydata = read.spss("myfile", to.data.frame=TRUE)

Table File

A data table can resides in a text file. The cells inside the table are separated by blank characters. Here is an example of a table with 4 rows and 3 columns.

100   a1   b1
200   a2   b2
300   a3   b3
400   a4   b4

Now copy and paste the table above in a file named "mydata.txt" with a text editor. Then load the data into the workspace with the function read.table.

> mydata = read.table("mydata.txt")  # read text file
> mydata                             # print data frame
   V1 V2 V3
1 100 a1 b1
2 200 a2 b2
3 300 a3 b3
4 400 a4 b4

For further detail of the function read.table, please consult the R documentation.

> help(read.table)

CSV File

The sample data can also be in comma separated values (CSV) format. Each cell inside such data file is separated by a special character, which usually is a comma, although other characters can be used as well.

The first row of the data file should contain the column names instead of the actual data. Here is a sample of the expected format.

Col1,Col2,Col3
100,a1,b1
200,a2,b2
300,a3,b3

After we copy and paste the data above in a file named "mydata.csv" with a text editor, we can read the data with the function read.csv.

> mydata = read.csv("mydata.csv")  # read csv file
> mydata
  Col1 Col2 Col3
1  100   a1   b1
2  200   a2   b2
3  300   a3   b3

In various European locales, as the comma character serves as the decimal point, the function read.csv2 should be used instead. For further detail of the read.csv and read.csv2 functions, please consult the R documentation.

> help(read.csv)

Working Directory

Finally, the code samples above assume the data files are located in the R working directory, which can be found with the function getwd.

> getwd() # get current working directory

You can select a different working directory with the function setwd(), and thus avoid entering the full path of the data files.

> setwd("") # set working directory

Note that the forward slash should be used as the path separator even on Windows platform.

> setwd("C:/MyDoc")

NCBI to assist in Virus Hunting Data Science Hackathon

BioStar — Thu, 15 Nov 2018 12:55:01 -0600

NCBI Hackathon are pleased to announce the second installment of the SoCal Bioinformatics Hackathon. From January 9-11, 2019, the NCBI will help run a bioinformatics hackathon in Southern California hosted by the Computational Sciences Research Center at San Diego State University!

NCBI Hackathon specifically looking for folks who have experience in computational virus hunting or adjacent fields to identify known, taxonomically-definable and novel viruses from a few hundred thousand metagenomic datasets that we’ll put on cloud infrastructure. This event is for researchers, including students and postdocs, who are already engaged in the use of bioinformatics data or in the development of pipelines for virological analyses from high-throughput experiments. If this describes you, please apply! The event is open to anyone selected for the hackathon and willing to travel to SDSU (see below).

https://ncbiinsights.ncbi.nlm.nih.gov/2018/11/09/ncbi-sdsu-virus-hunting-data-science-hackathon-january-2019/

De novo Genome Assembly for Illumina Data

Rahul Nayak — Mon, 20 Jan 2020 05:13:29 -0600

Written and maintained by Simon Gladman - Melbourne Bioinformatics (formerly VLSCI)

Protocol Overview / Introduction

In this protocol we discuss and outline the process of de novo assembly for small to medium sized genomes.

https://www.melbournebioinformatics.org.au/tutorials/tutorials/assembly/assembly-protocol/

Address of the bookmark: https://www.melbournebioinformatics.org.au/tutorials/tutorials/assembly/assembly-protocol/

BioJupies: Automatically Generates RNA-seq Data Analysis Notebooks

Rahul Nayak — Sun, 20 Dec 2020 11:43:45 -0600

With BioJupies you can produce in seconds a customized, reusable, and interactive report from your own raw or processed RNA-seq data through a simple user interface

BioJupies now supports user accounts! Sign in from the top right corner of the page for access to unlimited private notebooks, RNA-seq datasets and alignment jobs.

Address of the bookmark: https://amp.pharm.mssm.edu/biojupies/

Fundamentals of Data Visualization by Claus O. Wilke

Abhi — Sat, 08 Jun 2024 16:07:19 -0500

The book is meant as a guide to making visualizations that accurately reflect the data, tell a story, and look professional. It has grown out of my experience of working with students and postdocs in my laboratory on thousands of data visualizations. Over the years, I have noticed that the same issues arise over and over. I have attempted to collect my accumulated knowledge from these interactions in the form of this book.

The entire book is written in R Markdown, using RStudio as my text editor and the bookdown package to turn a collection of markdown documents into a coherent whole. The book’s source code is hosted on GitHub, at https://github.com/clauswilke/dataviz.

Address of the bookmark: https://clauswilke.com/dataviz/

BIRAC Innovation Fellowships Qualification & Eligibility

Thu, 01 Jun 2017 02:12:37 -0500

BIRAC Innovation Fellowships are highly competitive and prestigious. Under each University Innovation Clusters there are two Post-Doctoral and four Post Masters position.

Stipend / Fellowship (consolidated)
Post-doctoral = Rs 50,000 per month
Post Masters = Rs 30,000 per month.

Duration of Fellowships:
Both Post-Doctoral and Post-Masters fellowships are for two years extendable to one more year depending on the progress of the project and decision of the technical committee.

The University Innovation Clusters established at the five Universities have their broad scientific areas under which BIRAC Innovation Fellows will be selected. The qualification and eligibility of each UIC has been mentioned below.

Who can apply?
BIRAC along with five UICs invites research proposals from:

 Applicants who have completed their Master/ Ph.D. on and after 1st January 2014 for
Post Masters and Post-Doctoral BIRAC Innovation Fellowships

Applicants will have to submit an online application in the prescribed format. Each application will be reviewed by an expert committee at each UIC, which applicant has chosen. Applications will be identified on the identified criteria. Selected applicants will be called for a detailed project presentation and personal interview in front of an expert committee for final selection of the BIRAC Innovation Fellows.

Mere fulfilling the eligibility criterion does not entitle applicants to be called for interview.

More at http://birac.nic.in/webcontent/UIC_Fellowships_Qualification_Eligibility.pdf

SEX-DETector: A Probabilistic Approach to Study Sex Chromosomes in Non-Model Organisms

Surabhi Chaudhary — Wed, 30 May 2018 15:57:31 -0500

SEX-DETector is a probabilistic method that relies on RNAseq data from a cross (parents and progeny of each sex) to infer autosomal and sex-linked genes (genes located on the non recombining part of sex chromosomes).

How does SEX-DETector work?

SEX-DETector does not require prior sequencing of a reference genome: the same sequencing data can be used for the assembly and for the mapping of the reads. A full documentation on the pipeline can be found here.

we recommend Trinity for the assembly.
Trinity components should be merged with cap3. Our code to perform the merging is available here.
We recommend BWA for mapping of the reads.
When the mapping has been perfomed, the individuals need to be genotyped; SEX-DETector takes files produced by Reads2snp (which is available for download on the PopPhyl website) as input.

Address of the bookmark: http://lbbe.univ-lyon1.fr/-SEX-DETector-.html?lang=eg

Mulan: Multiple-sequence local alignment and visualization for studying function and evolution

Jit — Fri, 24 Aug 2018 09:50:01 -0500

Mulan: Multiple-sequence local alignment and visualization for studying function and evolution

Mulan (http://mulan.dcode.org/), a novel method and a network server for comparing multiple draft and finished-quality sequences to identify functional elements conserved over evolutionary time. Mulan brings together several novel algorithms: the TBA multi-aligner program for rapid identification of local sequence conservation, and the multiTF program for detecting evolutionarily conserved transcription factor binding sites in multiple alignments. In addition, Mulan supports two-way communication with the GALA database; alignments of multiple species dynamically generated in GALA can be viewed in Mulan, and conserved transcription factor binding sites identified with Mulan/multiTF can be integrated and overlaid with extensive genome annotation data using GALA.

Address of the bookmark: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC540288/

Orange-Bioinformatics 2.5.34

Robert M Willioms — Mon, 06 Oct 2014 12:51:37 -0500

Orange Bioinformatics extends Orange, a data mining software package, with common functionality for bioinformatics. The provided functionality can be accessed as a Python library or through a visual programming interface (Orange Canvas). The latter is also suitable for non-programmers.

Orange Bioinformatics provides access to publicly available data, like GEO data sets, Biomart, GO, KEGG, Atlas, ArrayExpress, and PIPAx database. As for the analytics, there is gene selection, quality control, scoring distances between experiments with multiple factors. All features can be combined with powerful visualization, network exploration and data mining techniques from the Orange data mining framework.

Address of the bookmark: https://pypi.python.org/pypi/Orange-Bioinformatics/2.5.34