BOL: Related items

04- Informatics Approach to Cancer - Interview with Dr. Joel Saltz

Mon, 07 Oct 2013 14:35:43 -0500

For additional information visit http://www.cancerquest.org/joel-saltz-interview. Dr. Joel Saltz is a Professor in the Departments of Pathology, Biostatistics and Bioinformatics, and Mathematics and Computer Science at Emory University. Dr. Saltz's research on bioinformatics spans several disciplines. One project involves applying computer analysis to medical imaging to yield better results for patients. As an example, a computer program may able to help doctors detect small cancers in a CT scan or mammogram. In this interview segment, Dr. Saltz discusses the informatics approach to cancer. To learn more about cancer and watch additional interviews, please visit the CancerQuest website at http://www.cancerquest.org.

Rotifers Lab

Wed, 08 Mar 2023 23:23:14 -0600

For scientists in the MBL’s Gribble Lab, the rotifer (Brachionus manjavacas) is used as a model organism to study evolution, stress responses, the biology of aging, and maternal effects. Rotifers are small, easy to grow in the lab, have a short lifespan, and share many of their genes with humans. That makes them ideal specimens in which to address questions relevant to human health as well as understand basic biological and evolutionary processes. Brachionus rotifers produces eggs that can be completely dried and frozen for decades, then hatch within a day when exposed to water and light.

https://www.mbl.edu/research/research-organisms/rotifer
https://gribblebiolab.org/

Evolution and Cancer

Fri, 27 Sep 2013 11:28:49 -0500

Air date: Wednesday, January 04, 2012, 3:00:00 PM Time displayed is Eastern Time, Washington DC Local Category: Wednesday Afternoon Lectures Description: There is a broad consensus that cancer is the result of somatic cells having serially gained, by a series of mutations, the ability to grow independently, to recruit resources from the circulation and the stroma, to invade local tissues, and to found anatomically distant metastases, ultimately killing the host. From the point of view of the cancer-causing somatic cell population, this is evolution driven by mutation and selection. Genomics has resulted in a parallel consensus that the central functions of all eukaryotes are highly conserved, not only at the level of individual protein functions, but also complex biological pathways and systems. These ideas motivated a comparison between results of molecular genetic studies of experimental evolution in yeast and the molecular genetic phenomena associated with tumorigenesis and tumor progression. We find some very striking similarities, including recurring genomic rearrangements, alterations of the regulation of specific growth-promoting genes, population-genetic features that affect the fitness trajectories of growth rate variants in evolving populations, and physiological and metabolic similarities derived from the conservation of the basic plan of growth and cell multiplication among all eukaryotes. It is hoped that some of the insights from yeast will aid the interpretation of sequence changes found in tumors, especially in the urgent necessity to distinguish 'driver' from 'passenger' mutations." David Botstein's fundamental contributions to modern genetics include the development of genetic methods for understanding biological functions and the discovery of the functions of many yeast and bacterial genes. In 1980, Botstein and three colleagues proposed a method for mapping human genes that laid the groundwork for the Human Genome Project. The basic principle of the mapping scheme was to develop, by recombinant DNA techniques, random single-copy DNA probes capable of detecting DNA sequence polymorphisms when hybridized to restriction digests, or specific fragments, of an individual's DNA. The method was used in subsequent years to identify several human disease genes, such as Huntington's and BRCA1. Variations of this method enabled the sequencing phase of the Human Genome Project. In the 1990s Botstein, having moved to Stanford University School of Medicine, collaborated with Patrick O. Brown of Stanford in exploiting DNA microarrays to study genome-wide gene expression patterns in yeast and in human cancers. This required developing a new statistical method and graphical interface, widely used today to interpret genomic data. Botstein also has helped to create, with Michael Ashburner and Gerald Rubin, a bioinformatics initiative to unify the representation of gene and gene product attributes across all species, called Gene Ontology. He graduated from Harvard College and earned his doctorate from the University of Michigan. He worked at Massachusetts Institute of Technology from 1967 to 1988; served as vice president for science at Genentech from 1988 to 1990; chaired the Department of Genetics at the Stanford University School of Medicine from 1990 to 2003; and joined the Princeton University faculty in 2003. He has sat on numerous editorial boards and was the founding editor of Molecular Biology of the Cell. Among recent major awards, Bostein won the Peter Gruber Foundation Prize in Genetics in 2003, the Apple Science Innovator Award in 2008, and the Albany Medical Center Prize in 2010. The NIH Wednesday Afternoon Lecture Series includes weekly scientific talks by some of the top researchers in the biomedical sciences worldwide. For more information, visit: The NIH Director's Wednesday Afternoon Lecture Series Author: Dr. David Botstein, Princeton University Runtime: 00:59:58 Permanent link: http://videocast.nih.gov/launch.asp?17046

Pre- or postdoctoral research fellowship in Structural Bioinformatics in Padova

Wed, 02 Oct 2013 15:12:22 -0500

University of Padova (URL: http://protein.bio.unipd.it/)

A research fellowship is available at the BioComputing Laboratory, University of Padova (URL: http://protein.bio.unipd.it/). A highly motivated and creative candidate is sought to work on structural bioinformatics. Specifically, the project entails the development of novel methods, tools and databases for the analysis of protein structures. The BioComputing Laboratory is a group of a dozen people working on several aspects of prediction of protein structure & function employing techniques at the intersection between biology, medicine, chemistry, physics & computer science. Our aim is to integrate the development of novel methods and their application to biologically relevant problems. We are looking for candidates with a solid Bioinformatics background, programming experience (Python, Perl, C++ and/or Java) and good knowledge of molecular biology (protein structure/function, signalling pathways). Candidates should have a degree with top marks, optionally hold a PhD, and be highly motivated to work on interdisciplinary research. Good knowledge of English, an open-minded spirit, being collaborative and creative are crucial. The fellowship, which should start in late 2013, is initially for one year. It will be commensurate to experience, can be extended depending on performance and may lead to a PhD degree. The successful candidate will be located at the BioComputing Laboratory, University of Padova. Travel support for conferences and/or research visits abroad may be provided. To apply, please send your CV, a brief description of your research background and the names of two (or more) references to Prof. Silvio Tosatto (Email: silvio.tosatto@unipd.it).

Contact Person (Referent): Silvio Tosatto
Ref. E-Mail: silvio.tosatto@unipd.it
Tel: +39 049 827 6269
Fax: +39 049 827 6260
Group Web Page: http://protein.bio.unipd.it/

Postdoctoral Scholar in Bacterial Evolution at Pathogen and Microbiome Institute at Northern Arizona University

Fri, 13 Dec 2024 12:49:16 -0600

We are pleased to announce a Postdoctoral Scholar position to study
bacterial evolution at the Pathogen and Microbiome Institute at
Northern Arizona University with Professor Paul Keim. The scholar
will have the opportunity also work with Professor Sam Sheppard at
The University of Oxford on joint projects. See our recent paper
on interspecific gene flow in Campylobacter. (DOI:
https://doi.org/10.1128/mbio.00581-24)

The job description: "This research position focuses on the science
of bacterial evolution. It will consist of researching theoretical
principles, but could include translational applications. Phylogenomic
and bioinformatic analysis of bacterial populations in nature or
in laboratory experiments will be a key component of the work. Prior
experience is an asset though training will be possible at PMI.
Likewise, laboratory microbiological, molecular, and biochemical
skills are an asset though not essential. Communication and critical
thinking skills are essential for performing the work and for
communicating to the local and international scientific communities.
Participating in team or independent grant writing to obtain research
funding will be required. Student mentoring is a part of the NAU
mission and is a partial expectation."

https://hr.peoplesoft.nau.edu/psp/ph92prta/EMPLOYEE/HRMS/c/HRS_HRAM.HRS_APP_SCHJOB.GBL?Page=HRS_APP_JBPST&Action=U&FOCUS=Applicant&SiteId=1&JobOpeningId=608024&PostingSeq=1

Northern Arizona University is located in Flagstaff, Arizona, a
beautiful mountain town with a surprisingly vibrant restaurant
scene. Located a little over an hour from the Grand Canyon and ~45
min from Sedona, Flagstaff is a hiker's paradise. In fact, the city
of Flagstaff operates more than 50 miles of unpaved trails and there
are, on average, 266 sunny days per year with which to enjoy them.
At 7000 ft in elevation, Flagstaff experiences all four seasons,
but thesummers are mild and, in the winter, you can be on the ski
slopes within 30 min! https://www.flagstaffarizona.org/

As mentioned, joint projects with Professor Sheppard at Oxford
University are possible, including travel to his laboratory in the
United Kingdom. https://www.biology.ox.ac.uk/people/samuel-sheppard

Contact Information:
Paul.Keim@nau.edu

Paul S. Keim, Ph.D.
Regents Professor, &
Cowden Endowed Chair of Microbiology
Northern Arizona University
Flagstaff, AZ 86011-4073

Paul S Keim

Contract Faculty-Bioinformatics at Maulana Azad National Institute of Technology

Thu, 12 Dec 2013 20:46:52 -0600

Contract Faculty-Bioinformatics at Maulana Azad National Institute of Technology

Job Description:F.No.11/10(1)/929 Qualifications: Candidates should have Ph.D. degree. If Ph.D. candidates are not available at least Post Graduate degree with GATE/NET qualification is a must. Walk-in-Interview on 19.12.2013 at 2.30 P.M. to 5.30 P.M .. at Maulana Azad National Institute of Technology: Bhopal For more details,please visit website:http://www.manit.ac.in/manitbhopal/Year2013/Recruitment/Contract_faculty/contract%20faculty%202013-2014.pdf

For more @ http://www.manit.ac.in/manitbhopal/Year2013/Recruitment/Contract_faculty/contract%20faculty%202013-2014.pdf

Web address @ :http://www.manit.ac.in

Yau Group

Tue, 15 Oct 2013 13:05:15 -0500

Yau Group are a new research group based at the Wellcome Trust Centre for Human Genetics and the Department of Statistics at the University of Oxford.

Yau Group develops statistical and computational methods for the analysis of genomic datasets with a particular interest in cancer sequencing applications and the use of Bayesian Statistics.

Yau Group are currently have projects in somatic mutation analysis of heterogeneous cancers, data fusion or integration techniques and single cell genomics.

More @ http://www.well.ox.ac.uk/~cyau/index.html

piRNA and Bioinformatics: Decoding the Guardians of the Genome

LEGE — Sat, 07 Dec 2024 02:15:11 -0600

In the symphony of small RNAs, PIWI-interacting RNAs (piRNAs) stand out as the protectors of genomic integrity. These small, non-coding RNAs play critical roles in silencing transposable elements, regulating gene expression, and maintaining germline stability. The rise of bioinformatics has revolutionized our understanding of piRNAs, enabling researchers to decipher their biogenesis, functions, and evolutionary significance.

What Are piRNAs?

piRNAs are the largest class of small non-coding RNAs, typically 24–32 nucleotides in length. Unlike microRNAs (miRNAs) and small interfering RNAs (siRNAs), piRNAs do not rely on Dicer enzymes for maturation. Instead, they are processed from long single-stranded precursors and associate with PIWI proteins, a subclass of the Argonaute protein family.

The primary functions of piRNAs include:

Silencing Transposable Elements: By targeting transposons, piRNAs prevent genomic instability, particularly in germline cells.
Regulating Gene Expression: piRNAs modulate gene expression at transcriptional and post-transcriptional levels.
Epigenetic Modulation: They guide epigenetic modifications, such as DNA methylation, to specific genomic loci.

Challenges in piRNA Research

Studying piRNAs is fraught with challenges, including:

Short Length: Their small size complicates sequencing and alignment.
Lack of Sequence Conservation: Unlike miRNAs, piRNAs exhibit limited sequence conservation across species.
Complex Biogenesis: The intricate pathways of piRNA generation require sophisticated computational tools to unravel.

Bioinformatics: Illuminating the World of piRNAs

Bioinformatics has emerged as an indispensable tool for studying piRNAs, facilitating their discovery, annotation, and functional analysis. Here's how bioinformatics is transforming piRNA research:

1. Identification and Annotation

The discovery of piRNAs relies on next-generation sequencing (NGS) data. Bioinformatics tools such as piRNApredictor and Piano identify piRNA clusters and predict potential targets. Databases like piRBase and piRNAdb curate information about known piRNAs, their sequences, and associated proteins.

2. Mapping and Alignment

piRNAs often originate from repetitive regions, making their alignment challenging. Tools like Bowtie and STAR handle the unique mapping requirements of piRNAs, enabling accurate identification of piRNA clusters in genomes.

3. Functional Analysis

Bioinformatics approaches predict piRNA functions by analyzing their interactions with transposons, genes, and epigenetic marks. Algorithms such as TargetFinder and RIblast explore piRNA-mRNA interactions, shedding light on regulatory networks.

4. Evolutionary Studies

piRNAs are evolutionarily diverse, reflecting their roles in species-specific genomic defense. Comparative genomics tools help trace the evolution of piRNA clusters and their associated PIWI proteins across species.

5. Epigenomic Insights

piRNAs are key players in epigenetic regulation. Bioinformatics pipelines integrate piRNA data with chromatin immunoprecipitation sequencing (ChIP-seq) and DNA methylation data to uncover their role in shaping the epigenome.

Case Study: piRNAs in Germline Integrity

One of the hallmark functions of piRNAs is the suppression of transposable elements in the germline. For example, in Drosophila melanogaster, piRNAs target retrotransposons like gypsy and copia. Bioinformatics analyses revealed that these piRNAs guide PIWI proteins to transposon-derived RNA, ensuring genome stability during gametogenesis.

Clinical Relevance of piRNAs

Recent studies suggest that piRNAs may serve as biomarkers for diseases such as cancer, infertility, and neurodegenerative disorders. For instance:

Cancer: Dysregulated piRNA expression has been linked to tumorigenesis, making them potential targets for cancer therapies.
Infertility: Aberrant piRNA pathways are implicated in male infertility due to their role in spermatogenesis.
Neurodegeneration: piRNAs may regulate neuronal gene expression, highlighting their potential in neurological research.

Future Directions

The integration of bioinformatics with emerging technologies offers exciting opportunities for piRNA research:

Single-Cell Sequencing: Unveiling cell-specific piRNA expression and function.
Machine Learning: Predicting piRNA functions and targets with greater accuracy.
CRISPR-Based Tools: Editing piRNA clusters to explore their roles in vivo.

Conclusion

piRNAs are the unsung guardians of the genome, safeguarding genetic material from transposable elements and contributing to gene regulation and epigenetic programming. Bioinformatics has opened the floodgates of discovery, unraveling the complexities of piRNAs and their myriad roles in biology and disease.

As we continue to decode the piRNA landscape, these small RNAs promise to unveil big secrets about genome stability, evolution, and human health, cementing their place as a fascinating frontier in molecular biology.

Associate Professor - Centre for Bioinformatics at Maharshi Dayanand University, Rohtak

Thu, 12 Dec 2013 20:49:59 -0600

ADVERTISEMENT No. PR-54/2013

No. of Posts and Specialization: 1(UR)

Educational Qualification:

(i) Good academic record with a Ph.D. Degree in the concerned /allied /relevant disciplines.

(ii) The Ph.D. Degree shall be a mandatory qualification for all candidates to be appointed as Associate Professor through direct recruitment.

(iii) A Master‟s Degree with at least 55% marks (or an equivalent grade in a point scale wherever grading system is followed).

(iv) A minimum of eight years of experience of teaching and /or research in an academic /research position equivalent to that of Assistant Professor in a University, College or Accredited Research Institution/Industry excluding the period of Ph.D research with evidence of published work and a minimum of 5 publications as books and /or research papers in refereed journals only/policy papers.

(v) Contribution to educations innovation, design of new curricula and courses and technology-mediated teaching learning process with evidence of having guided doctoral candidates and research students.

(vi) A minimum score as stipulated in the Academic Performance Indicator (API) based performance Based Appraisal System (PBAS), set out in this notification in as mentioned in the advertisement.

Send your application to the A.R (Estt.Teaching), M.D.University, Rohtak on or before December 23, 2013.

For more details: http://www.mdurohtak.ac.in/pdf/Notices_Pdf/new_notice/Teaching%20Vacancy%20%28ADVT.%20No.%20PR-54%20of%202013%29.pdf

Last Apply Date: 23 Dec 2013

A Beginner's Guide to Using Kraken for Taxonomic Classification

Neel — Fri, 13 Dec 2024 11:29:03 -0600

Kraken is a popular bioinformatics tool designed for fast and accurate taxonomic classification of metagenomic sequences. Its efficiency and precision make it a go-to resource for analyzing microbial communities, including bacteria, viruses, archaea, and fungi. Whether you're new to bioinformatics or experienced in the field, Kraken is an indispensable tool for taxonomic analysis.

In this blog, we’ll walk through the basics of Kraken, from installation to running an analysis, and highlight its key features and applications.

What is Kraken?

Kraken is a sequence classification tool that assigns taxonomic labels to DNA sequences using exact k-mer matching. It uses a reference database of genomes, dividing sequences into k-mers and identifying matches in a computationally efficient way.

Key Features of Kraken

Speed: Kraken processes data much faster than alignment-based methods.
Accuracy: It uses a precise k-mer matching algorithm for high-resolution taxonomic assignments.
Scalability: It can handle large metagenomic datasets.
Custom Databases: You can build and use custom databases tailored to your research needs.

Installing Kraken

System Requirements
- A Unix-based operating system (Linux/macOS).
- Sufficient computational resources for database building (RAM and disk space).
Installation Steps
- Clone the Kraken repository from GitHub:
  
  git clone https://github.com/DerrickWood/kraken.git cd kraken
- Compile the Kraken binaries:
  
  make
- Add Kraken to your PATH for easy access:
  
  export PATH=$PATH:/path/to/kraken

Preparing a Database

Kraken requires a database of reference genomes. You can use a pre-built database or create a custom one.

Downloading a Pre-built Database
Kraken offers pre-built databases, such as the MiniKraken database, which is lightweight and suitable for smaller datasets. Download it using:

kraken-build --download-library minikraken
Building a Custom Database
To include specific genomes, download FASTA files and build the database:

kraken-build --download-library bacteria --threads 4 --db my_database kraken-build --build --db my_database

This process may take considerable time and resources, depending on the size of the database.

Running Kraken

Once the database is ready, you can classify sequences.

Basic Usage
Use the following command to classify sequences:

kraken --db my_database --threads 4 --fastq-input input_sequences.fastq --output kraken_output.txt

Key options:
- --db: Specifies the database.
- --threads: Number of threads for parallel processing.
- --fastq-input: Indicates input file format (FASTQ/FASTA).
Interpreting Results
Kraken generates an output file with columns for sequence IDs, taxonomic classifications, and the confidence score.

Visualizing Kraken Results

Kraken results can be visualized using tools like Krona or converted to human-readable reports using kraken-report.

Generate a Report

kraken-report --db my_database kraken_output.txt > kraken_report.txt
Krona Visualization
Install Krona and convert Kraken output for visualization:

cut -f2,3 kraken_output.txt | ktImportTaxonomy -o krona_output.html

Open the HTML file in your browser to interactively explore the taxonomic classifications.

Advanced Usage

Confidence Thresholds
Adjust the confidence threshold for classification using the --confidence option. Higher values reduce false positives but may miss some true positives:

kraken --db my_database --confidence 0.1 --fastq-input input.fastq
Paired-End Reads
For paired-end sequencing data, use:

kraken --db my_database --paired reads_1.fastq reads_2.fastq
Customizing K-mers
Kraken allows you to set custom k-mer lengths during database building for specific applications.

Applications of Kraken

Microbial Ecology: Characterizing microbial communities in soil, water, and the human microbiome.
Pathogen Detection: Identifying pathogens in clinical samples.
Fungal Research: Analyzing fungal diversity in metagenomic datasets.
Environmental Monitoring: Tracking microbial populations in diverse habitats.

Conclusion

Kraken is a versatile and efficient tool for taxonomic classification in metagenomics. Its speed, accuracy, and flexibility make it a favorite among bioinformaticians. By following this guide, you can set up and use Kraken to unlock insights into microbial and fungal communities, paving the way for discoveries in ecology, medicine, and biotechnology.