<![CDATA[BOL: Related items]]> https://bioinformaticsonline.com/related/30440?offset=1010 https://bioinformaticsonline.com/bookmarks/view/20504/chromevol Sun, 25 Jan 2015 00:33:11 -0600 https://bioinformaticsonline.com/bookmarks/view/20504/chromevol <![CDATA[ChromEvol]]> Chromosome number is a remarkably dynamic feature of eukaryotic evolution. Chromosome numbers can change by a duplication of the whole genome (a process termed polyploidy), or by single chromosome changes (ascending dysploidy via, e.g., chromosome fission or descending dysploidy via, e.g., chromosome fusion).
Of the various mechanisms of chromosome number change, polyploidy has received significant attention because of the impact such an event may have on the organism.
ChromEvol implements a series of likelihood models for the evolution of chromosome numbers. By comparing the fit of the different models to biological data, it may be possible to gain insight regarding the pathways by which the evolution of chromosome number proceeds. For each model, the program estimates the rates for the possible transitions assumed by the model, infers the set of ancestral chromosome numbers, and estimates the location along the tree for which polyploidy events (and other chromosome number changes) occurred. For further methodological details, see the publications and manual on the Downloads page.

http://www.tau.ac.il/~itaymay/cp/chromEvol/about.html

Address of the bookmark: http://www.tau.ac.il/~itaymay/cp/chromEvol/downloads.html

]]> Jit https://bioinformaticsonline.com/blog/view/44229/common-steps-for-reads-mapping Thu, 09 Mar 2023 02:48:02 -0600 https://bioinformaticsonline.com/blog/view/44229/common-steps-for-reads-mapping <![CDATA[Common steps for reads mapping !]]>

Mapping reads to a reference genome is an essential step in many types of genomic analysis, such as variant calling and gene expression analysis. Here are some general steps to follow for mapping reads to a genome:

  1. Choose a read mapper: There are many read mappers available, such as BWA, Bowtie, and HISAT2. Choose a mapper that is appropriate for your type of data and research question.

  2. Index the reference genome: Before mapping reads, the reference genome needs to be indexed. This involves creating an index of the genome sequence that allows the mapper to quickly find matches to the reads. Most mappers have their own indexing tools.

  3. Prepare the read data: The reads should be in a format that is compatible with the mapper. Most mappers accept FASTQ or BAM files. Depending on the quality of the data, it may need to be filtered or trimmed before mapping.

  4. Run the mapper: The mapper is run with the command-line interface or using a graphical user interface. The specific command depends on the mapper being used, but typically involves specifying the input data, reference genome, and output file format.

  5. Evaluate the mapping results: After the mapping is complete, the results should be evaluated. This includes assessing the quality of the mapping, such as the mapping rate, the number of mapped reads, and the mapping quality score.

  6. Post-processing: Depending on the analysis being performed, post-processing of the mapped reads may be necessary. This can include filtering reads based on quality, removing duplicate reads, and calling variants.

Overall, mapping reads to a reference genome is a complex process that requires careful consideration of the type of data, the research question, and the specific mapper being used.

]]> BioStar https://bioinformaticsonline.com/opportunity/view/20672/jrfra-structuralcomputational-biology-at-icgeb Thu, 29 Jan 2015 11:52:40 -0600 <![CDATA[JRF/RA Structural/Computational Biology at ICGEB]]> Research Associate and JRF positions in the Structural and Computational Biology Group starting 1st March 2015. Collaborative projects include work on:

a) bioinformatics, systems and computational biology
b) malaria
c) drug discovery
d) genomics
e) microbiology
f) metabolic disorders
g) molecular medicine

Eligibility: Applicants must have one of the following :

1) INSPIRE award for undertakig either PhD or Postdoctoral research;
2) SPM award for PhD;
3) JRF for pursuing PhD from CSIR/DBT/ICMR

Interest and experience in Biochemistry/Bioinformatics/Biophysics/ Chemistry/Genomics/Molecular Biology/ is essential.

Submit curriculum vitae to sb.icgeb@gmail.com by 20 February 2015

]]> https://bioinformaticsonline.com/news/view/34711/1mb-long-dna-with-nanopore-technology Tue, 19 Dec 2017 18:49:28 -0600 https://bioinformaticsonline.com/news/view/34711/1mb-long-dna-with-nanopore-technology <![CDATA[1mb long DNA with Nanopore technology]]> The first continuous DNA read of more than a million bases (>1Mb) has been achieved, using Oxford Nanopore sequencing technology. Congratulations to Martin Smith and collaborators! Read more: http://bit.ly/2j5TNCO

]]> Jit https://bioinformaticsonline.com/opportunity/view/21538/senior-research-fellow-at-all-india-institute-of-medical-sciences-aiims-delhi-delhi-delhi Wed, 11 Mar 2015 03:06:10 -0500 <![CDATA[SENIOR RESEARCH FELLOW at All India Institute of Medical Sciences (AIIMS Delhi) - Delhi, Delhi]]> Applications are invited from eligible candidates for the following temporary post in an ICMR funded Research Project entitle “An Investigation to find out reasons for Phenotypic Heterogeneity/Variability in 22q11.2 Microdeletion Syndrome” in Department of Reproductive Biology, AIIMS, New Delhi PI: Dr. Ashutosh Halder, Professor, Department of Reproductive Biology

Name of the post: Senior Research Fellow (SRF)
Duration: 2 year
Salary: Rs. 28000/- per month + 30% HRA
Eligibility: MSc (life sciences) with 2 years research experience, NET/GATE qualified
Desirable: Experience in the field of Genomics, Epigenomics & Bioinformatics
SELECTION PROCEDURE FOR ALL INDIA INSTITUTE OF MEDICAL SCIENCES (AIIMS DELHI) – SENIOR RESEARCH FELLOW POST:

Candidates can apply on or before 15/03/2015
No Detailed information about the selection process is mentioned in the recruitment notification
HOW TO APPLY FOR SENIOR RESEARCH FELLOW VACANCY IN ALL INDIA INSTITUTE OF MEDICAL SCIENCES (AIIMS DELHI):

Deadline: 15.03.15 Submit your C.V in Room No. 2099 (Molecular Cytogenetics Lab), 2nd floor, Reproductive Biology, All India Institute of Medical Sciences, New Delhi-110029 or Email CV to: ashutoshhalder@gmail.com Your CV should include the details of your work experience & degrees along with two references with e-mail and contact number Only 10 shortlisted (on merit) candidates will be invited for interview. No TA/DA will be applicable for the same

]]> https://bioinformaticsonline.com/bookmarks/view/38535/nanopack-visualizing-and-processing-long-read-sequencing-data Tue, 25 Dec 2018 21:20:50 -0600 https://bioinformaticsonline.com/bookmarks/view/38535/nanopack-visualizing-and-processing-long-read-sequencing-data <![CDATA[NanoPack: visualizing and processing long-read sequencing data]]> Address of the bookmark: https://github.com/wdecoster/nanopack

]]> Jit https://bioinformaticsonline.com/opportunity/view/20959/research-associate-and-jrf-positions-in-the-structural-and-computational-biology-group-at-icgeb Mon, 02 Feb 2015 23:00:37 -0600 <![CDATA[Research Associate and JRF positions in the Structural and Computational Biology Group at ICGEB]]> Research Associate and JRF positions in the Structural and Computational Biology Group starting 1st March 2015. Collaborative projects include work on:

a) bioinformatics, systems and computational biology
b) malaria
c) drug discovery
d) genomics
e) microbiology
f) metabolic disorders
g) molecular medicine

Eligibility: Applicants must have one of the following :

1) INSPIRE award for undertakig either PhD or Postdoctoral research;
2) SPM award for PhD;
3) JRF for pursuing PhD from CSIR/DBT/ICMR

Interest and experience in Biochemistry/Bioinformatics/Biophysics/ Chemistry/Genomics/Molecular Biology/ is essential.

Submit curriculum vitae to sb.icgeb@gmail.com by 20 February 2015

]]> https://bioinformaticsonline.com/bookmarks/view/40754/understanding-your-reads-and-mapping Wed, 29 Jan 2020 06:29:55 -0600 https://bioinformaticsonline.com/bookmarks/view/40754/understanding-your-reads-and-mapping <![CDATA[Understanding your reads and mapping !]]> One of the best tutorial for beginners ...

https://bioinformatics-core-shared-training.github.io/cruk-summer-school-2017/Day1/Session4-seqIntro.html

Address of the bookmark: https://bioinformatics-core-shared-training.github.io/cruk-summer-school-2017/Day1/Session4-seqIntro.html

]]> Neel https://bioinformaticsonline.com/opportunity/view/21064/jrf-project-assistant-recruitment-at-shillong-%E2%80%93-bioinformatics-centre-dic Sat, 07 Feb 2015 06:00:23 -0600 <![CDATA[JRF / Project Assistant Recruitment at Shillong – Bioinformatics Centre (DIC)]]> 3 Vacancies at Bioinformatics Centre (DIC) For M.Tech/M.Sc. Degree Candidates. Apply Before 15th February,2015

Bioinformatics Centre (DIC) invites applications for the following posts:

Job Number: 01
Job Designation: Junior Research Fellow (JRF)
Number of Vacancy: 02 (Two)
Educational Qualification:
M.Tech/M.Sc. in Life Sciences/Botany/Zoology/Biochemistry/Biotechnology/Bioinformatics.
Desirable Qualification:
Aptitude for Bioinformatics and Computer Programming/Next generation sequencing data analysis.

Job Number: 02
Job Designation: Project Assistant
Number of Vacancy: 01 (One)
Educational Qualification:
Graduation in Science.
Desirable Qualification:
Experience of working in a Life Science/Plant Biotechnology Lab.

Place of Work: Shillong

How To Apply For Opening:
The applications through email bicnehu@gmail.com or post must reach the undersigned within 15 days from the date of publication of this advertisement.

Last Date To Apply: 15th February,2015

Contact Address: Bioinformatics Centre (DIC),Shillong-793022

Advertisement Details: Employment News (31 January – 6 February) Page 28

]]> https://bioinformaticsonline.com/pages/view/17843/pathway-analysis Fri, 03 Oct 2014 08:51:13 -0500 https://bioinformaticsonline.com/pages/view/17843/pathway-analysis <![CDATA[Pathway Analysis]]> Pathway Analysis is usually performed with aim to enrich the genes with their functional information and reveal the underlying biological mechanisms pursue by genes. Pathway Analysis is not only limited to what biological pathways a particular set of expressed genes follow but also to disclose the relationships between these genes. With availability of more genomics, transcriptomics and proteomics data, interactions between genes involve in multiple pathways become more clear and also relationships between the genes, their transcripts, and their gene products. However, existing tools and dbs mainly based on knowledge driven approach in which pathways will be identified by finding the correlation between the information in one of the pathway knowledge databases (KEGG,Reactome,Panther,BioCarta, Panther,GO,NCI,WikiPathways,etc) and gene expression result for a specific conditions for instance tumor, obesity , cold resistant crops/plants, etc.

Introductory Articles/ppt/sources:

http://www.ploscompbiol.org/article/info%3Adoi%2F10.1371%2Fjournal.pcbi.1002375

http://bioinformatics.mdanderson.org/MicroarrayCourse/Lectures09/Pathway%20Analysis.pdf

http://gettinggeneticsdone.blogspot.de/2012/03/pathway-analysis-for-high-throughput.html

http://davetang.org/muse/tag/pathway/

https://www.biostars.org/p/42219/

http://bioinformatics.ca//files/public/Pathways_2014_Module4_v2.pdf

http://bioinformatics.ca//files/public/Pathways_2014_Module2.pdf

Impotant Database and Tools:

GeneMANIA, Cytoscape, IPA and Metacore (Commerical ), Pathway Commons, Reactome ,Panther, BioCyc, WikiPathways, Pathvisio, KEGG, NCI, Stringdb, Amigo, WebGestalt ,ConsensusPathDB ,GSEA,Blast2go

Popular R based tools:

Reactome.db, ReactomePA, ClusterProfiler, Gage, SPIA, topGO, Pathview,DOSE,GOStat

More:

http://www.bioconductor.org/help/search/index.html?q=Enrichment+analysis+

 

]]> Rahul Agarwal