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Impacts of Variation in the Human Genome on Gene Regulation

JOURNAL OF MOLECULAR BIOLOGY (2013)

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JOURNAL OF MOLECULAR BIOLOGY

卷 425, 期 21, 页码 3970-3977

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ACADEMIC PRESS LTD- ELSEVIER SCIENCE LTD

DOI: 10.1016/j.jmb.2013.07.015

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Biochemistry & Molecular Biology

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Recent advances in fast and inexpensive DNA sequencing have enabled the extensive study of genomic and transcriptomic variation in humans. Human genomic variation is composed of sequence and structural changes including single-nucleotide and multinucleotide variants, short insertions or deletions (indels), larger copy number variants, and similarly sized copy neutral inversions and translocations. It is now well established that any two genomes differ extensively and that structural changes constitute a prominent source of this variation. There have also been major technological advances in RNA sequencing to globally quantify and describe diversity in transcripts. Large consortia such as the 1000 Genomes Project and the ENCODE (ENCyclopedia Of DNA Elements) Project are producing increasingly comprehensive maps outlining the regions of the human genome containing variants and functional elements, respectively. Integration of genetic variation data and extensive annotation of functional genomic elements, along with the ability to measure global transcription, allow the impacts of genetic variants on gene expression to be resolved. There are several well-established models by which genetic variants affect gene regulation depending on the type, nature, and position of the variant with respect to the affected genes. These effects can be manifested in two ways: changes to transcript sequences and isoforms by coding variants, and changes to transcript abundance by dosage or regulatory variants. Here, we review the current state of how genetic variations impact gene regulation locally and globally in the human genome. (C) 2013 The Authors. Published by Elsevier Ltd. All rights reserved.

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Record, David Reeves, Allyson Ricarte, Ana Rodriguez-Soto, Alexander Ropelewski, Jean Rosario, Morla-Adames Roselkis, David Rowe, Tarun Kanti Roy, Matt Ruffalo, Nancy Ruschman, Angela Sabo, Nina Sachdev, Sinem Saka, Diane Salamon, Pinaki Sarder, Hiroshi Sasaki, Rahul Satija, Diane Saunders, Riley Sawka, Kevin Schey, Heidi Schlehlein, David Scholten, Sarah Schultz, Lauren Schwartz, Melissa Schwenk, Robin Scibek, Ayellet Segre, Matthew Serrata, Walter Shands, Xiaotao Shen, Jay Shendure, Holly Shephard, Lingyan Shi, Tujin Shi, Dong-Guk Shin, Bill Shirey, Max Sibilla, Michal Silber, Jonathan Silverstein, Derek Simmel, Alan Simmons, Dhruv Singhal, Santhosh Sivajothi, Thomas Smits, Francesca Soncin, Qi Song, Valentina Stanley, Tim Stuart, Hanquan Su, Pei Su, Xin Sun, Christine Surrette, Hannah Swahn, Kai Tan, Sarah Teichmann, Abhiroop Tejomay, George Tellides, Kathleen Thomas, Tracey Thomas, Marissa Thompson, Hua Tian, Leonoor Tideman, Cole Trapnell, Albert G. Tsai, Chia-Feng Tsai, Leo Tsai, Elizabeth Tsui, Tina Tsui, Jason Tung, Morgan Turner, Jackie Uranic, Eeshit Dhaval Vaishnav, Sricharan Reddy Varra, Vasyl Vaskivskyi, Dusan Velickovic, Marija Velickovic, Jamie Verheyden, Jessica Waldrip, Douglas Wallace, Xueyi Wan, Allen Wang, Fusheng Wang, Meng Wang, Shuoshuo Wang, Xuefei Wang, Clive Wasserfall, Leonard Wayne, James Webber, Griffin M. Weber, Bei Wei, Jian-Jun Wei, Annika Weimer, Joel Welling, Xingzhao Wen, Zishen Wen, MacKenzie Williams, Seth Winfree, Nicholas Winograd, Abashai Woodard, Devin Wright, Fan Wu, Pei-Hsun Wu, Qiuyang Wu, Xiaodong Wu, Yi Xing, Tiangyang Xu, Manxi Yang, Mingyu Yang, Joseph Yap, Dong Hye Ye, Peng Yin, Zhou Yuan, Chi (Jina) Yun, Ali Zahraei, Kevin Zemaitis, Bo Zhang, Caibin Zhang, Chenyu Zhang, Chi Zhang, Kun Zhang, Shiping Zhang, Ted Zhang, Yida Zhang, Bingqing Zhao, Wenxin Zhao, Jia Wen Zheng, Sheng Zhong, Bokai Zhu, Chenchen Zhu, Diming Zhu, Quan Zhu, Ying Zhu

Summary: The Human Biomolecular Atlas Program (HuBMAP) aims to create a spatial atlas of the healthy human body at single-cell resolution using advanced technologies and disseminating resources to the community. This Perspective introduces the production phase of HuBMAP, which involves generating spatial maps of functional tissue units across organs from diverse populations and creating tools and infrastructure to advance biomedical research.

NATURE CELL BIOLOGY (2023)

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Correction Cell Biology

Lipid droplets and peroxisomes are co-regulated to drive lifespan extension in response to mono-unsaturated fatty acids (vol 25, pg 672, 2023)

Katharina Papsdorf, Jason W. Miklas, Amir Hosseini, Matias Cabruja, Christopher S. Morrow, Marzia Savini, Yong Yu, Carlos G. Silva-Garcia, Nicole R. Haseley, Luke Meraz Murphy, Pallas Yao, Elisa de Launoit, Scott J. Dixon, Michael P. Snyder, Meng C. Wang, William B. Mair, Anne Brunet

NATURE CELL BIOLOGY (2023)

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Article Biochemical Research Methods

Organ Mapping Antibody Panels: a community resource for standardized multiplexed tissue imaging

Ellen M. Quardokus, Diane C. Saunders, Elizabeth McDonough, John W. Hickey, Christopher Werlein, Christine Surrette, Presha Rajbhandari, Anna Martinez Casals, Hua Tian, Lisa Lowery, Elizabeth K. Neumann, Frida Bjoerklund, Taruna V. Neelakantan, Josh Croteau, Anne E. Wiblin, Jeremy Fisher, April J. Livengood, Karen G. Dowell, Jonathan C. Silverstein, Jeffrey M. Spraggins, Gloria S. Pryhuber, Gail Deutsch, Fiona Ginty, Garry P. Nolan, Simon Melov, Danny Jonigk, Michael A. Caldwell, Ioannis S. Vlachos, Werner Muller, Nils Gehlenborg, Brent R. Stockwell, Emma Lundberg, Michael P. Snyder, Ronald N. Germain, Jeannie M. Camarillo, Neil L. Kelleher, Katy Boerner, Andrea J. Radtke

Summary: Organ Mapping Antibody Panels are standardized antibody panels created by the community for multiplexed spatial imaging. This imaging technique allows detailed characterization of molecular and cellular organization in tissues. Although high-parameter data collection is now possible (>60 targets), constructing the necessary antibody panels requires expertise and capital. Organ Mapping Antibody Panels are community-validated resources that save time and money, enhance reproducibility, expedite discovery, and support the creation of a Human Reference Atlas.

NATURE METHODS (2023)

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Article Endocrinology & Metabolism

Dynamic lipidome alterations associated with human health, disease and ageing

Daniel Hornburg, Si Wu, Mahdi Moqri, Xin Zhou, Kevin Contrepois, Nasim Bararpour, Gavin M. Traber, Baolong Su, Ahmed A. Metwally, Monica Avina, Wenyu Zhou, Jessalyn M. Ubellacker, Tejaswini Mishra, Sophia Miryam Schussler-Fiorenza Rose, Paula B. Kavathas, Kevin J. Williams, Michael P. Snyder

Summary: This study reports over 800 lipid species and their roles in health-to-disease transitions, such as in diabetes, ageing, and inflammation. Longitudinal lipidomic profiling of plasma samples from 112 participants revealed dynamic changes in the plasma lipidome during respiratory viral infection, insulin resistance, and ageing, highlighting the potential roles of lipids in immune homoeostasis and inflammation regulation.

NATURE METABOLISM (2023)

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Article Biochemistry & Molecular Biology

Mycobacterium tuberculosis Ku Stimulates Multi-round DNA Unwinding by UvrD1 Monomers

Ankita Chadda, Alexander G. Kozlov, Binh Nguyen, Timothy M. Lohman, Eric A. Galburt

Summary: In this study, it was found that the DNA damage response in Mycobacterium tuberculosis differs from well-studied model bacteria. The DNA repair helicase UvrD1 in Mtb is activated through a redox-dependent process and is closely associated with the homo-dimeric Ku protein. Additionally, Ku protein is shown to stimulate the helicase activity of UvrD1.

JOURNAL OF MOLECULAR BIOLOGY (2024)

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