Your search keyword '"Dave KA"' showing total 40 results

1. The experience of using virtual reality for interactive spatial visualisation of environmental data.

Author

Isak de Villiers Bosman, Annique Smith, Kwan Sui Dave Ka, Koos J. W. de Beer, and Jan A Maritz

Published

2023

2. UCHealth’s virtual health center: How Colorado’s largest health system creates and integrates technology into patient care

Author

Elizabeth Goldberg, Dave Kao, Bethany Kwan, Hemali Patel, Amy Hassell, and Richard Zane

Subjects

Computer applications to medicine. Medical informatics, R858-859.7

Abstract

In the face of formidable healthcare challenges, such as staffing shortages and rising costs, technology has emerged as a crucial ally in enhancing patient care. UCHealth, Colorado’s largest health system, has pioneered the integration of technology into patient care through its Virtual Health Center (VHC). In this Comment, we explore UCHealth’s journey in creating a centralized hub that harnesses innovative digital health solutions to address patient care needs across its 12 hospitals, spanning over 600,000 emergency department visits and nearly 150,000 inpatient and observation encounters annually. The VHC has proven to be a transformative force, providing high-quality care at scale, reducing staff burden, and establishing new career pathways in virtual health. The transformation process involved multiple steps: (a) identifying a need, (b) vetting within health system solutions, (c) searching for industry solutions, and scrutinizing these through meetings with our innovations center, (d) piloting the solution, and (e) sustaining the solution by integrating them within the electronic health record (EHR).

Published

2024

3. Returning actionable genetic results to participants in the biobank at the Colorado Center for Personalized Medicine and UCHealth

Author

Jan T. Lowery, Lisen Axell, Lisa Ku, Emily B. Todd, Dave Kao, Nick Rafaels, Matt R.G. Taylor, Elizabeth Kudron, Stephen Wicks, Jean Jirikowic, Elise Shalowitz, and Kristy R. Crooks

Subjects

Array-based genotyping, Biobank, Multi-Ethnic Genotyping Array(MEGA), Personalized medicine, Sanger sequencing, Genetics, QH426-470, Medicine

Abstract

Purpose: To describe our process for returning genetic results to participants in the Colorado Center for Personalized Medicine biobank. Methods: Enrollment in the biobank is open to all adult UCHealth patients. Participants who provided a sample that was genotyped and signed the proper consent were eligible to receive results. Genetic data were generated using a custom genotyping array and confirmed via Sanger sequencing. We used 2 models for returning results and conducted interviews with participants to assess satisfaction with our process, follow-up care, and family communication. Results: As of July 2022, 73,313 participants had provided a sample and proper consent. Of these, 10,489 samples were genotyped, 137 (1.3%) had initial results, and 62 were confirmed and eligible for return. We returned results to 51 participants, 33% for cardiac risk, 31% cancer, 15% familial hypercholesterolemia, and 21% for other conditions (11 participants refused or did not respond). Less than half of participants had a relevant family history. The majority of participants were glad to receive results and satisfied with our process. Conclusion: Although array-based genotyping has known limitations that reduce its accuracy, we were able to identify persons with underlying genetic risk who were previously unaware. It is important to establish a process for returning results that follows clinical guidelines, protects participant autonomy, and is amenable to all participants.

Published

2024

4. Oxygen-dependent hydroxylation by FIH regulates the TRPV3 ion channel

Author

Karttunen, S, Duffield, M, Scrimgeour, NR, Squires, L, Lim, WL, Dallas, ML, Scragg, JL, Chicher, J, Dave, KA, Whitelaw, ML, Peers, C, Gorman, JJ, Gleadle, JM, Rychkov, GY, and Peet, DJ

Abstract

Factor inhibiting HIF (FIH, also known as HIF1AN) is an oxygendependent asparaginyl hydroxylase that regulates the hypoxiainducible factors (HIFs). Several proteins containing ankyrin repeat domains (ARDs) have been characterised as substrates of FIH, although there is little evidence for a functional consequence of hydroxylation on these substrates. This study demonstrates that the transient receptor potential vanilloid 3 (TRPV3) channel is hydroxylated by FIH on asparagine 242 within the cytoplasmic ARD. Hypoxia, FIH inhibitors and mutation of asparagine 242 all potentiated TRPV3-mediated current, without altering TRPV3 protein levels, indicating that oxygen-dependent hydroxylation inhibits TRPV3 activity. This novel mechanism of channel regulation by oxygen-dependent asparaginyl hydroxylation is likely to extend to other ion channels.

Published

2015

5. The macro- and megabenthic fauna on the continental shelf of the eastern Amundsen Sea, Antarctica

Author

Linse, Katrin, Griffiths, Huw J, Barnes, Dave KA, Brandt, Angelika, Davey, Niki, David, Bruno, De Grave, Sammy, d'Udekem d'Acoz, Cédric, Eléaume, Marc, Glover, Adrian G., Hemery, Lenaïg G., Mah, Christopher, Martín-Ledo, Rafael, Munilla, Tomás, O'Loughlin, Mark, Pierrat, Benjamin, Saucède, Thomas, Sands, Chester J, Strugnell, Jan M, Enderlein, Peter, Linse, Katrin, Griffiths, Huw J, Barnes, Dave KA, Brandt, Angelika, Davey, Niki, David, Bruno, De Grave, Sammy, d'Udekem d'Acoz, Cédric, Eléaume, Marc, Glover, Adrian G., Hemery, Lenaïg G., Mah, Christopher, Martín-Ledo, Rafael, Munilla, Tomás, O'Loughlin, Mark, Pierrat, Benjamin, Saucède, Thomas, Sands, Chester J, Strugnell, Jan M, and Enderlein, Peter

Abstract

In 2008 the BIOPEARL II expedition on board of RRS James Clark Ross sailed to the eastern Amundsen Sea Embayment and Pine Island Bay, one of the least studied Antarctic continental shelf regions due to its remoteness and ice cover. A total of 37 Agassiz trawls were deployed at depth transects along the continental and trough slopes. A total of 5,469 specimens, belonging to 32 higher taxonomic groups and more than 270 species, were collected. Species richness per station varied from 1–55. The benthic assemblages were dominated by echinoderms and clearly different to those in the Ross, Scotia and Weddell seas. Here we present the macro- and megafaunal assemblage structure, its species richness and the presence of several undescribed species.

Published

2013

6. The data of the Swedish Malaise Trap Project, a countrywide inventory of Sweden's insect fauna

Author

Dave Karlsson, Mattias Forshage, Kevin Holston, and Fredrik Ronquist

Subjects

Malaise trap, insect fauna, inventory, survey, all, Biology (General), QH301-705.5

Abstract

Despite Sweden's strong entomological tradition, large portions of its insect fauna remain poorly known. As part of the Swedish Taxonomy Initiative, launched in 2002 to document all multi-cellular species occurring in the country, the first taxonomically-broad inventory of the country's insect fauna was initiated, the Swedish Malaise Trap Project (SMTP). In total, 73 Malaise traps were deployed at 55 localities representing a wide range of habitats across the country. Most traps were run continuously from 2003 to 2006 or for a substantial part of that time period. The total catch is estimated to contain 20 million insects, distributed over 1,919 samples (Karlsson et al. 2020). The samples have been sorted into more than 300 taxonomic units, which are made available for expert identification. Thus far, more than 100 taxonomists have been involved in identifying the sorted material, recording the presence of 4,000 species. One third of these had not been recorded from Sweden before and 700 have tentatively been identified as new to science.Here, we describe the SMTP dataset, published through the Global Biodiversity Information Facility (GBIF). Data on the sorted material are available in the "SMTP Collection Inventory" dataset. It currently includes more than 130,000 records of taxonomically-sorted samples. Data on the identified material are published using the Darwin Core standard for sample-based data. That information is divided up into group-specific datasets, as the sample set processed for each group is different and in most cases non-overlapping. The current data are divided into 79 taxonomic datasets, largely corresponding to taxonomic sorting fractions. The orders Diptera and Hymenoptera together comprise about 90% of the specimens in the material and these orders are mainly sorted to family or subfamily. The remaining insect taxa are mostly sorted to the order level. In total, the 79 datasets currently available comprise around 165,000 specimens, that is, about 1% of the total catch. However, the data are now accumulating rapidly and will be published continuously. The SMTP dataset is unique in that it contains a large proportion of data on previously poorly-known taxa in the Diptera and Hymenoptera.

Published

2020

7. The Swedish Malaise Trap Project: A 15 Year Retrospective on a Countrywide Insect Inventory

Author

Dave Karlsson, Emily Hartop, Mattias Forshage, Mathias Jaschhof, and Fredrik Ronquist

Subjects

All-taxa biodiversity inventory (ATBI), biota, div, Biology (General), QH301-705.5

Abstract

The Swedish Malaise Trap Project (SMTP) is one of the most ambitious insect inventories ever attempted. The project was designed to target poorly known insect groups across a diverse range of habitats in Sweden. The field campaign involved the deployment of 73 Malaise traps at 55 localities across the country for three years (2003-2006). Over the past 15 years, the collected material has been hand sorted by trained technicians into over 300 taxonomic fractions suitable for expert attention. The resulting collection is a tremendous asset for entomologists around the world, especially as we now face a desperate need for baseline data to evaluate phenomena like insect decline and climate change. Here, we describe the history, organisation, methodology and logistics of the SMTP, focusing on the rationale for the decisions taken and the lessons learned along the way. The SMTP represents one of the early instances of community science applied to large-scale inventory work, with a heavy reliance on volunteers in both the field and the laboratory. We give estimates of both staff effort and volunteer effort involved. The project has been funded by the Swedish Taxonomy Initiative; in total, the inventory has cost less than 30 million SEK (approximately 3.1 million USD). Based on a subset of the samples, we characterise the size and taxonomic composition of the SMTP material. Several different extrapolation methods suggest that the material comprises around 20 million specimens in total. The material is dominated by Diptera (75% of the specimens) and Hymenoptera (15% of specimens). Amongst the Diptera, the dominant groups are Chironomidae (37% of specimens), Sciaridae (15%), Phoridae (13%), Cecidomyiidae (9.5%) and Mycetophilidae (9.4%). Within Hymenoptera, the major groups are Ichneumonidae (44% of specimens), Diaprioidea (19%), Braconidae (9.6%), Platygastroidea (8.5%) and Chalcidoidea (7.9%). The taxonomic composition varies with latitude and season. Several Diptera and Hymenoptera groups are more common in non-summer samples (collected from September to April) and in the North, while others show the opposite pattern. About 1% of the total material has been processed and identified by experts so far. This material represents over 4,000 species. One third of these had not been recorded from Sweden before and almost 700 of them are new to science. These results reveal the large amounts of taxonomic work still needed on Palaearctic insect faunas. Based on the SMTP experiences, we discuss aspects of planning and conducting future large-scale insect inventory projects using mainly traditional approaches in relation to more recent approaches that rely on molecular techniques.

Published

2020

8. Hypothesis: improving literacy about health workforce will improve rural health workforce recruitment, retention and capability

Author

Alexandra Martiniuk, Richard Colbran, Robyn Ramsden, Dave Karlson, Emer O’Callaghan, Estrella Lowe, Michael Edwards, Sharif Bagnulo, Imogene Rothnie, Laura Hardaker, Bernadette Gotch, and Arna Wotherspoon

Subjects

Health, Workforce, Literacy, Rural, Recruitment, Retention, Medicine (General), R5-920, Public aspects of medicine, RA1-1270

Abstract

Abstract Background One of the key barriers to health in rural areas is health workforce. Poor understanding and communication about health workforce across all stakeholder groups (including the broad community) is very common and can negatively affect the health workforce, recruitment, experiences and outcomes. Hypothesis In this paper, we propose the concept of literacy about health workforce. We propose this as a specific, actionable extension of the existing and well accepted health literacy concept. We hypothesise that improving literacy about health workforce will improve, in particular, rural health workforce recruitment, retention and capability. Implications of the hypothesis We propose that literacy about health workforce is important for all members of the health and broader system (e.g. local GP, mayor, workforce agency, health manager, Aboriginal health worker, carers, community health facilitators, patients, schools, local businesses, cultural and recreation groups) because we hypothesise their literacy about health workforce affects their capacity to make informed decisions and take action to manage their health workforce needs in direct synchrony with the community’s health needs. We hypothesise that improving literacy about health workforce will improve the effectiveness and efficiency of attracting, recruiting, training, and retaining a high quality, capable, health workforce, and further, will support the development and acceptance of innovative solutions to health workforce crises such as new models of care. This hypothesis is action orientated, is testable and includes the consideration of methods to engage and improve literacy of those within and external to the health workforce.

Published

2019

9. The macro- and megabenthic fauna on the continental shelf of the eastern Amundsen Sea, Antarctica

Author

Linse, Katrin, primary, Griffiths, Huw J, additional, Barnes, Dave KA, additional, Brandt, Angelika, additional, Davey, Niki, additional, David, Bruno, additional, De Grave, Sammy, additional, d′Udekem d′Acoz, Cédric, additional, Eléaume, Marc, additional, Glover, Adrian G., additional, Hemery, Lenaïg G., additional, Mah, Christopher, additional, Martín-Ledo, Rafael, additional, Munilla, Tomás, additional, O′Loughlin, Mark, additional, Pierrat, Benjamin, additional, Saucède, Thomas, additional, Sands, Chester J, additional, Strugnell, Jan M, additional, and Enderlein, Peter, additional

Published

2013

10. Modified full-face snorkel masks as reusable personal protective equipment for hospital personnel.

Author

Laurel Kroo, Anesta Kothari, Melanie Hannebelle, George Herring, Thibaut Pollina, Ray Chang, Dominic Peralta, Samhita P Banavar, Eliott Flaum, Hazel Soto-Montoya, Hongquan Li, Kyle Combes, Emma Pan, Khang Vu, Kelly Yen, James Dale, Patrick Kolbay, Simon Ellgas, Rebecca Konte, Rozhin Hajian, Grace Zhong, Noah Jacobs, Amit Jain, Filip Kober, Gerry Ayala, Quentin Allinne, Nicholas Cucinelli, Dave Kasper, Luca Borroni, Patrick Gerber, Ross Venook, Peter Baek, Nitin Arora, Philip Wagner, Roberto Miki, Jocelyne Kohn, David Kohn Bitran, John Pearson, Beatriz Arias-Arco, Ricardo Larrainzar-Garijo, Cristián Muñiz Herrera, and Manu Prakash

Subjects

Medicine, Science

Abstract

Here we adapt and evaluate a full-face snorkel mask for use as personal protective equipment (PPE) for health care workers, who lack appropriate alternatives during the COVID-19 crisis in the spring of 2020. The design (referred to as Pneumask) consists of a custom snorkel-specific adapter that couples the snorkel-port of the mask to a rated filter (either a medical-grade ventilator inline filter or an industrial filter). This design has been tested for the sealing capability of the mask, filter performance, CO2 buildup and clinical usability. These tests found the Pneumask capable of forming a seal that exceeds the standards required for half-face respirators or N95 respirators. Filter testing indicates a range of options with varying performance depending on the quality of filter selected, but with typical filter performance exceeding or comparable to the N95 standard. CO2 buildup was found to be roughly equivalent to levels found in half-face elastomeric respirators in literature. Clinical usability tests indicate sufficient visibility and, while speaking is somewhat muffled, this can be addressed via amplification (Bluetooth voice relay to cell phone speakers through an app) in noisy environments. We present guidance on the assembly, usage (donning and doffing) and decontamination protocols. The benefit of the Pneumask as PPE is that it is reusable for longer periods than typical disposable N95 respirators, as the snorkel mask can withstand rigorous decontamination protocols (that are standard to regular elastomeric respirators). With the dire worldwide shortage of PPE for medical personnel, our conclusions on the performance and efficacy of Pneumask as an N95-alternative technology are cautiously optimistic.

Published

2021

11. Capability ... what's in a word? Rural Doctors Network of New South Wales Australia is shifting to focus on the capability of rural health professionals

Author

Alexandra Martiniuk, Richard Colbran, Robyn Ramsden, Mike Edwards, Elizabeth Barrett, Emer O'Callaghan, Ros Bullock, Estrella Lowe, Dave Karlson, John Curnow, Bernadette Gotch, John Kramer, Sharif Bagnulo, Imogene Rothnie, Laura Hardaker, Nicole Turner, Arna Wotherspoon, and Chris Russell

Subjects

access, capability, Capability Approach, capacity, competence, rural health workforce, Special situations and conditions, RC952-1245, Public aspects of medicine, RA1-1270

Abstract

Rural health services, and the workforces that provide those services, are under unprecedented pressure due to insufficient health workforce numbers and distribution of health workforce weighted to urban areas. This creates health service access issues in rural areas, compounding existing health inequalities between rural and urban people. Many approaches to date have aimed to rectify these issues, with moderate success. In this article we present a call to action to pursue a complementary approach: supporting the capability of the rural health workforce. We hypothesise that further exploring what it means to be a 'capable' rural health professional and what processes or conditions support or erode capability may additionally bolster efforts toward strong rural and remote health systems. The Capability Approach is a theory proposed by Amartya Sen, who was awarded the Nobel Memorial Prize in Economic Sciences in 1998 for this work. Although the Capability Approach inspired, for instance, the UN's Human Development Index, it has not been deeply explored in the context of rural health workforce. While still untested, a focus on capability may assist us in taking a broader view, which encompasses functioning and the freedom to pursue different functioning combinations. The feasible freedom and opportunities are paramount to the concept of capability. We posit that competence is static and the responsibility of the practitioner (and their education), but that capability is fluid and multi-dimensional and the responsibility of the practitioner, community and system. Therefore, we hypothesise that a focus on a Capability Approach, which modulates the relation between the contextual factors and outcomes, may provide us with greater understanding and avenues for action when we aim to improve outcomes such as rural health service sustainability. Developing a list of appropriate capabilities and setting strategies to support capability and its more nuanced domains may present unique opportunities for influence, and these may have positive effects on the rural health workforce. Of course it will need to be determined if improving rural primary health professionals' capability has positive impacts upon quality and access to care, and whether supporting capability is sustainable and worthy of investment.

Published

2020

12. Completing Linnaeus's inventory of the Swedish insect fauna: Only 5,000 species left?

Author

Fredrik Ronquist, Mattias Forshage, Sibylle Häggqvist, Dave Karlsson, Rasmus Hovmöller, Johannes Bergsten, Kevin Holston, Tom Britton, Johan Abenius, Bengt Andersson, Peter Neerup Buhl, Carl-Cedric Coulianos, Arne Fjellberg, Carl-Axel Gertsson, Sven Hellqvist, Mathias Jaschhof, Jostein Kjærandsen, Seraina Klopfstein, Sverre Kobro, Andrew Liston, Rudolf Meier, Marc Pollet, Matthias Riedel, Jindřich Roháček, Meike Schuppenhauer, Julia Stigenberg, Ingemar Struwe, Andreas Taeger, Sven-Olof Ulefors, Oleksandr Varga, Phil Withers, and Ulf Gärdenfors

Subjects

Medicine, Science

Abstract

Despite more than 250 years of taxonomic research, we still have only a vague idea about the true size and composition of the faunas and floras of the planet. Many biodiversity inventories provide limited insight because they focus on a small taxonomic subsample or a tiny geographic area. Here, we report on the size and composition of the Swedish insect fauna, thought to represent roughly half of the diversity of multicellular life in one of the largest European countries. Our results are based on more than a decade of data from the Swedish Taxonomy Initiative and its massive inventory of the country's insect fauna, the Swedish Malaise Trap Project The fauna is considered one of the best known in the world, but the initiative has nevertheless revealed a surprising amount of hidden diversity: more than 3,000 new species (301 new to science) have been documented so far. Here, we use three independent methods to analyze the true size and composition of the fauna at the family or subfamily level: (1) assessments by experts who have been working on the most poorly known groups in the fauna; (2) estimates based on the proportion of new species discovered in the Malaise trap inventory; and (3) extrapolations based on species abundance and incidence data from the inventory. For the last method, we develop a new estimator, the combined non-parametric estimator, which we show is less sensitive to poor coverage of the species pool than other popular estimators. The three methods converge on similar estimates of the size and composition of the fauna, suggesting that it comprises around 33,000 species. Of those, 8,600 (26%) were unknown at the start of the inventory and 5,000 (15%) still await discovery. We analyze the taxonomic and ecological composition of the estimated fauna, and show that most of the new species belong to Hymenoptera and Diptera groups that are decomposers or parasitoids. Thus, current knowledge of the Swedish insect fauna is strongly biased taxonomically and ecologically, and we show that similar but even stronger biases have distorted our understanding of the fauna in the past. We analyze latitudinal gradients in the size and composition of known European insect faunas and show that several of the patterns contradict the Swedish data, presumably due to similar knowledge biases. Addressing these biases is critical in understanding insect biomes and the ecosystem services they provide. Our results emphasize the need to broaden the taxonomic scope of current insect monitoring efforts, a task that is all the more urgent as recent studies indicate a possible worldwide decline in insect faunas.

Published

2020

13. Darwin wasps: a new name heralds renewed efforts to unravel the evolutionary history of Ichneumonidae

Author

Seraina Klopfstein, Bernardo F. Santos, Mark R. Shaw, Mabel Alvarado, Andrew M.R. Bennett, Davide Dal Pos, Madalene Giannotta, Andres F. Herrera Florez, Dave Karlsson, Andrey I. Khalaim, Alessandro R. Lima, István Mikó, Ilari E. Sääksjärvi, So Shimizu, Tamara Spasojevic, Simon van Noort, Lars Vilhelmsen, and Gavin R. Broad

Subjects

parasitoid wasps, taxonomy, alpha taxonomy, phylogenetics, paleoentomology, fossils, Zoology, QL1-991

Abstract

The parasitoid wasp family Ichneumonidae is arguably one of the groups for which current knowledge lags most strongly behind their enormous diversity. In a five-day meeting in Basel (Switzerland) in June 2019, 22 researchers from 14 countries met to discuss the most important issues in ichneumonid research, including increasing the speed of species discovery, resolving higher-level relationships, and studying the radiation of these parasitoids onto various host groups through time. All agreed that it is time to advertise ichneumonid research more broadly in the scientific community and thereby attract young talents to this group for which specialists are sorely lacking. In order to popularize the group, we here suggest a new name for the family, “Darwin wasps”, to reflect the pivotal role they played in convincing Charles Darwin that not all of creation could have been created by a benevolent god. We hope that the name catches on, and that Darwin wasps start buzzing more loudly across all disciplines of biology.

Published

2019

14. Conducting a large, multi-site survey about patients’ views on broad consent: challenges and solutions

Author

Maureen E. Smith, Saskia C. Sanderson, Kyle B. Brothers, Melanie F. Myers, Jennifer McCormick, Sharon Aufox, Martha J. Shrubsole, Nanibaá A. Garrison, Nathaniel D. Mercaldo, Jonathan S. Schildcrout, Ellen Wright Clayton, Armand H. Matheny Antommaria, Melissa Basford, Murray Brilliant, John J. Connolly, Stephanie M. Fullerton, Carol R. Horowitz, Gail P. Jarvik, Dave Kaufman, Terri Kitchner, Rongling Li, Evette J. Ludman, Catherine McCarty, Valerie McManus, Sarah Stallings, Janet L. Williams, and Ingrid A. Holm

Subjects

Survey, Consent, Multi-site, Genomics, Institutional Review Board, Cognitive interviews, Medicine (General), R5-920

Abstract

Abstract Background As biobanks play an increasing role in the genomic research that will lead to precision medicine, input from diverse and large populations of patients in a variety of health care settings will be important in order to successfully carry out such studies. One important topic is participants’ views towards consent and data sharing, especially since the 2011 Advanced Notice of Proposed Rulemaking (ANPRM), and subsequently the 2015 Notice of Proposed Rulemaking (NPRM) were issued by the Department of Health and Human Services (HHS) and Office of Science and Technology Policy (OSTP). These notices required that participants consent to research uses of their de-identified tissue samples and most clinical data, and allowing such consent be obtained in a one-time, open-ended or “broad” fashion. Conducting a survey across multiple sites provides clear advantages to either a single site survey or using a large online database, and is a potentially powerful way of understanding the views of diverse populations on this topic. Methods A workgroup of the Electronic Medical Records and Genomics (eMERGE) Network, a national consortium of 9 sites (13 separate institutions, 11 clinical centers) supported by the National Human Genome Research Institute (NHGRI) that combines DNA biorepositories with electronic medical record (EMR) systems for large-scale genetic research, conducted a survey to understand patients’ views on consent, sample and data sharing for future research, biobank governance, data protection, and return of research results. Results Working across 9 sites to design and conduct a national survey presented challenges in organization, meeting human subjects guidelines at each institution, and survey development and implementation. The challenges were met through a committee structure to address each aspect of the project with representatives from all sites. Each committee’s output was integrated into the overall survey plan. A number of site-specific issues were successfully managed allowing the survey to be developed and implemented uniformly across 11 clinical centers. Conclusions Conducting a survey across a number of institutions with different cultures and practices is a methodological and logistical challenge. With a clear infrastructure, collaborative attitudes, excellent lines of communication, and the right expertise, this can be accomplished successfully.

Published

2016

15. Review of: Andrew Kolin (2016) Political Economy of Labour Repression in the United States

Author

Dave Kamper

Subjects

Social Sciences

Published

2019

16. Development of an enzyme immunoassay for detection of antibodies against Coccidioides in dogs and other mammalian species.

Author

Nancy A Chow, Mark D Lindsley, Orion Z McCotter, Dave Kangiser, Ron D Wohrle, Wayne R Clifford, Hayley D Yaglom, Laura E Adams, Kenneth Komatsu, Michelle M Durkin, Rocky J Baker, Lisa F Shubitz, Gordana Derado, Tom M Chiller, and Anastasia P Litvintseva

Subjects

Medicine, Science

Abstract

Coccidioides is a soil-dwelling fungus that causes coccidioidomycosis, a disease also known as Valley fever, which affects humans and a variety of animal species. Recent findings of Coccidioides in new, unexpected areas of the United States have demonstrated the need for a better understanding of its geographic distribution. Large serological studies on animals could provide important information on the geographic distribution of this pathogen. To facilitate such studies, we used protein A/G, a recombinant protein that binds IgG antibodies from a variety of mammalian species, to develop an enzyme immunoassay (EIA) that detects IgG antibodies against Coccidioides in a highly sensitive and high-throughput manner. We showed the potential of this assay to be adapted to multiple animal species by testing a collection of serum and/or plasma samples from dogs, mice, and humans with or without confirmed coccidioidomycosis. We then evaluated the performance of the assay in dogs, using sera from dogs residing in a highly endemic area, and found seropositivity rates significantly higher than those in dogs of non-endemic areas. We further evaluated the specificity of the assay in dogs infected with other fungal pathogens known to cross-react with Coccidioides. Finally, we used the assay to perform a cross-sectional serosurvey investigating dogs from Washington, a state in which infection with Coccidioides has recently been documented. In summary, we have developed a Coccidioides EIA for the detection of antibodies in canines that is more sensitive and has higher throughput than currently available methods, and by testing this assay in mice and humans, we have shown a proof of principle of its adaptability for other animal species.

Published

2017

17. A hymenopterists’ guide to the Hymenoptera Anatomy Ontology: utility, clarification, and future directions

Author

Katja Seltmann, Matthew Yoder, Istvan Miko, Mattias Forshage, Matthew Bertone, Donat Agosti, Andrew Austin, James Balhoff, Marek Borowiec, Seán Brady, Gavin Broad, Denis Brothers, Roger Burks, Matthew Buffington, Heather Campbell, Kelly Dew, Andrew Ernst, Jose Fernandez-Triana, Michael Gates, Gary Gibson, John Jennings, Norman Johnson, Dave Karlsson, Ricardo Kawada, Lars Krogmann, Robert Kula, Patricia Mullins, Michael Ohl, Claus Rasmussen, Fredrick Ronquist, Susanne Schulmeister, Michael Sharkey, Elijah Talamas, Erika Tucker, Lars Vilhelmsen, Philip S. Ward, Robert Wharton, and Andrew Deans

Subjects

Zoology, QL1-991

Abstract

Hymenoptera exhibit an incredible diversity of phenotypes, the result of ~240 million years of evolution and the primary subject of more than 250 years of research. Here we describe the history, development, and utility of the Hymenoptera Anatomy Ontology (HAO) and its associated applications. These resources are designed to facilitate accessible and extensible research on hymenopteran phenotypes. Outreach with the hymenopterist community is of utmost importance to the HAO project, and this paper is a direct response to questions that arised from project workshops. In a concerted attempt to surmount barriers of understanding, especially regarding the format, utility, and development of the HAO, we discuss the roles of homology, “preferred terms”, and “structural equivalency”. We also outline the use of Universal Resource Identifiers (URIs) and posit that they are a key element necessary for increasing the objectivity and repeatability of science that references hymenopteran anatomy. Pragmatically, we detail a mechanism (the “URI table”) by which authors can use URIs to link their published text to the HAO, and we describe an associated tool (the “Analyzer”) to derive these tables. These tools, and others, are available through the HAO Portal website (http://portal.hymao.org). We conclude by discussing the future of the HAO with respect to digital publication, cross-taxon ontology alignment, the advent of semantic phenotypes, and community-based curation.

Published

2012

18. Impacts of Air Pollution and Climate Change on Forest Ecosystems — Emerging Research Needs

Author

Elena Paoletti, Andrzej Bytnerowicz, Chris Andersen, Algirdas Augustaitis, Marco Ferretti, Nancy Grulke, Madeleine S. Günthardt-Goerg, John Innes, Dale Johnson, Dave Karnosky, Jesada Luangjame, Rainer Matyssek, Steven McNulty, Gerhard Müller-Starck, Robert Musselman, and Kevin Percy

Subjects

Technology, Medicine, Science

Abstract

Outcomes from the 22nd meeting for Specialists in Air Pollution Effects on Forest Ecosystems “Forests under Anthropogenic Pressure Effects of Air Pollution, Climate Change and Urban Development”, September 1016, 2006, Riverside, CA, are summarized. Tropospheric or ground-level ozone (O3) is still the phytotoxic air pollutant of major interest. Challenging issues are how to make O3 standards or critical levels more biologically based and at the same time practical for wide use; quantification of plant detoxification processes in flux modeling; inclusion of multiple environmental stresses in critical load determinations; new concept development for nitrogen saturation; interactions between air pollution, climate, and forest pests; effects of forest fire on air quality; the capacity of forests to sequester carbon under changing climatic conditions and coexposure to elevated levels of air pollutants; enhanced linkage between molecular biology, biochemistry, physiology, and morphological traits.

Published

2007

19. Skeletal morphology of Opius dissitus and Biosteres carbonarius (Hymenoptera: Braconidae), with a discussion of terminology.

Author

Dave Karlsson and Fredrik Ronquist

Subjects

Medicine, Science

Abstract

The Braconidae, a family of parasitic wasps, constitute a major taxonomic challenge with an estimated diversity of 40,000 to 120,000 species worldwide, only 18,000 of which have been described to date. The skeletal morphology of braconids is still not adequately understood and the terminology is partly idiosyncratic, despite the fact that anatomical features form the basis for most taxonomic work on the group. To help address this problem, we describe the external skeletal morphology of Opius dissitus Muesebeck 1963 and Biosteres carbonarius Nees 1834, two diverse representatives of one of the least known and most diverse braconid subfamilies, the Opiinae. We review the terminology used to describe skeletal features in the Ichneumonoidea in general and the Opiinae in particular, and identify a list of recommend terms, which are linked to the online Hymenoptera Anatomy Ontology. The morphology of the studied species is illustrated with SEM-micrographs, photos and line drawings. Based on the examined species, we discuss intraspecific and interspecific morphological variation in the Opiinae and point out character complexes that merit further study.

Published

2012

20. Emergence and impact of oprD mutations in Pseudomonas aeruginosa strains in cystic fibrosis.

Author

Sherrard LJ, Wee BA, Duplancic C, Ramsay KA, Dave KA, Ballard E, Wainwright CE, Grimwood K, Sidjabat HE, Whiley DM, Beatson SA, Kidd TJ, and Bell SC

Subjects

Adolescent, Adult, Australia, Drug Resistance, Bacterial genetics, Female, Humans, Male, Mutation, Pseudomonas aeruginosa, Whole Genome Sequencing, Young Adult, Carbapenems therapeutic use, Cystic Fibrosis microbiology, Porins genetics, Pseudomonas Infections drug therapy, Pseudomonas Infections genetics

Abstract

Background: Antimicrobial resistance in cystic fibrosis (CF) Pseudomonas aeruginosa airway infection is complex and often attributed to chromosomal mutations. How these mutations emerge in specific strains or whether particular gene mutations are clinically informative is unclear. This study focused on oprD, which encodes an outer membrane porin associated with carbapenem resistance when it is downregulated or inactivated., Aim: Determine how mutations in oprD emerge in two prevalent Australian shared CF strains of P. aeruginosa and their clinical relevance., Methods: The two most common shared CF strains in Queensland were investigated using whole genome sequencing and their oprD sequences and antimicrobial resistance phenotypes were established. P. aeruginosa mutants with the most common oprD variants were constructed and characterised. Clinical variables were compared between people with or without evidence of infection with strains harbouring these variants., Results: Frequently found nonsense mutations arising from a 1-base pair substitution in oprD evolved independently in three sub-lineages, and are likely major contributors to the reduced carbapenem susceptibility observed in the clinical isolates. Lower baseline FEV 1 %predicted was identified as a risk factor for infection with a sub-lineage (odds ratio=0.97; 95% confidence interval 0.96-0.99; p<0.001). However, acquiring these sub-lineage strains did not confer an accelerated decline in FEV 1 nor increase the risk of death/lung transplantation., Conclusions: Sub-lineages harbouring specific mutations in oprD have emerged and persisted in the shared strain populations. Infection with the sub-lineages was more likely in people with lower lung function, but this was not predictive of a worse clinical trajectory., Competing Interests: Declaration of Competing Interest The authors declare that they have no conflict of interest., (Copyright © 2021. Published by Elsevier B.V.)

Published

2022

21. Impact of Quantisal ® Oral Fluid Collection Device on Drug Stability.

Author

Riggio M, Dave KA, Koscak B, Blakey M, and Appleton C

Abstract

The stability of drugs can affect drug tests and interpretations. A comprehensive study to verify drug stability in Quantisal ® oral fluid (OF) collection device was undertaken in accordance with Australian standard, AS/NZS 4760:2019 (SAI-Global, 2019). The evaluation was performed for the following drugs: (±) amphetamine, (±) methylamphetamine, (±) 3,4-methylenedioxymethylamphetamine (MDMA), (-)Δ9-tetrahydrocannabinol (THC), cocaine, benzoylecgonine, morphine, codeine, and oxycodone. Stability was assessed at four different storage temperatures over seven time points at ±50% cut-off concentrations (Appendix A, Para A4-4.1, AS/NZS 4760:2019) (SAI-Global, 2019). All drugs were found to be significantly more stable at 4 and -20°C, with stability spanning at least 14 days with percentage change within ±20% from the cut-off concentrations (SAI-Global, 2019). In addition, we report a variation trend with cocaine and benzoylecgonine at elevated temperatures, suggesting hydrolytic decomposition of cocaine and a concomitant increase in benzoylecgonine quantitative values. We confirm the cross-talk by showing that the percentage change in the profile of average cocaine-benzoylecgonine measurement is within the acceptance concentration range of ±20%. This finding highlights the importance of precaution during storage and careful considerations during subsequent interpretation of liquid chromatography-mass spectrometry (LCMS) measurements., Competing Interests: The authors were employed by company Queensland Medical Laboratory (QML) Pathology, under the Healius Pathology Pty Ltd network. QML Pathology has a commercial supplier/customer relationship with Abbott Diagnostics for supply of laboratory reagents, analysers, etc as the laboratory does with many other suppliers. Abbott Diagnostics assisted by providing collection and transportation devices and by recompensing the laboratory for cost of consumables required to perform the validation. This had no influence on the performance of the investigation or the conclusions reached., (Copyright © 2021 Riggio, Dave, Koscak, Blakey and Appleton.)

Published

2021

22. Identification of Proteins Deregulated by Platinum-Based Chemotherapy as Novel Biomarkers and Therapeutic Targets in Non-Small Cell Lung Cancer.

Author

Ryan SL, Dave KA, Beard S, Gyimesi M, McTaggart M, Sahin KB, Molloy C, Gandhi NS, Boittier E, O'Leary CG, Shah ET, Bolderson E, Baird AM, Richard DJ, O'Byrne KJ, and Adams MN

Abstract

Platinum-based chemotherapy remains the cornerstone of treatment for most people with non-small cell lung cancer (NSCLC), either as adjuvant therapy in combination with a second cytotoxic agent or in combination with immunotherapy. Resistance to therapy, either in the form of primary refractory disease or evolutionary resistance, remains a significant issue in the treatment of NSCLC. Hence, predictive biomarkers and novel combinational strategies are required to improve the effectiveness and durability of treatment response 6for people with NSCLC. The aim of this study was to identify novel biomarkers and/or druggable proteins from deregulated protein networks within non-oncogene driven disease that are involved in the cellular response to cisplatin. Following exposure of NSCLC cells to cisplatin, in vitro quantitative mass spectrometry was applied to identify altered protein response networks. A total of 65 proteins were significantly deregulated following cisplatin exposure. These proteins were assessed to determine if they are druggable targets using novel machine learning approaches and to identify whether these proteins might serve as prognosticators of platinum therapy. Our data demonstrate novel candidates and drug-like molecules warranting further investigation to improve response to platinum agents in NSCLC., Competing Interests: The authors declare competing financial interests; KO’B and DR are founders of CARP Pharmaceuticals. EB, DR, and KO’B are founders of Carpe Vitae Pharmaceuticals. MA, EB, KO’B, and DR are inventors on patent applications filed by Queensland University of Technology. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Ryan, Dave, Beard, Gyimesi, McTaggart, Sahin, Molloy, Gandhi, Boittier, O’Leary, Shah, Bolderson, Baird, Richard, O’Byrne and Adams.)

Published

2021

23. Ankyrin Repeat Proteins of Orf Virus Influence the Cellular Hypoxia Response Pathway.

Author

Chen DY, Fabrizio JA, Wilkins SE, Dave KA, Gorman JJ, Gleadle JM, Fleming SB, Peet DJ, and Mercer AA

Subjects

Amino Acid Sequence, Animals, Cell Hypoxia, Computational Biology, Escherichia coli genetics, Escherichia coli metabolism, Gene Expression Regulation, HEK293 Cells, HeLa Cells, Host-Pathogen Interactions, Humans, Hydroxylation, Hypoxia-Inducible Factor 1, alpha Subunit metabolism, Leydig Cells, Male, Mixed Function Oxygenases metabolism, Models, Molecular, Orf virus metabolism, Primary Cell Culture, Protein Binding, Protein Domains, Protein Structure, Secondary, Recombinant Proteins genetics, Recombinant Proteins metabolism, Repressor Proteins metabolism, Sheep, Signal Transduction, Ankyrin Repeat, Hypoxia-Inducible Factor 1, alpha Subunit genetics, Mixed Function Oxygenases genetics, Orf virus genetics, Repressor Proteins genetics

Abstract

Hypoxia-inducible factor (HIF) is a transcriptional activator with a central role in regulating cellular responses to hypoxia. It is also emerging as a major target for viral manipulation of the cellular environment. Under normoxic conditions, HIF is tightly suppressed by the activity of oxygen-dependent prolyl and asparaginyl hydroxylases. The asparaginyl hydroxylase active against HIF, factor inhibiting HIF (FIH), has also been shown to hydroxylate some ankyrin repeat (ANK) proteins. Using bioinformatic analysis, we identified the five ANK proteins of the parapoxvirus orf virus (ORFV) as potential substrates of FIH. Consistent with this prediction, coimmunoprecipitation of FIH was detected with each of the ORFV ANK proteins, and for one representative ORFV ANK protein, the interaction was shown to be dependent on the ANK domain. Immunofluorescence studies revealed colocalization of FIH and the viral ANK proteins. In addition, mass spectrometry confirmed that three of the five ORFV ANK proteins are efficiently hydroxylated by FIH in vitro While FIH levels were unaffected by ORFV infection, transient expression of each of the ORFV ANK proteins resulted in derepression of HIF-1α activity in reporter gene assays. Furthermore, ORFV-infected cells showed upregulated HIF target gene expression. Our data suggest that sequestration of FIH by ORFV ANK proteins leads to derepression of HIF activity. These findings reveal a previously unknown mechanism of viral activation of HIF that may extend to other members of the poxvirus family., Importance: The protein-protein binding motif formed from multiple repeats of the ankyrin motif is common among chordopoxviruses. However, information on the roles of these poxviral ankyrin repeat (ANK) proteins remains limited. Our data indicate that the parapoxvirus orf virus (ORFV) is able to upregulate hypoxia-inducible factor (HIF) target gene expression. This response is mediated by the viral ANK proteins, which sequester the HIF regulator FIH (factor inhibiting HIF). This is the first demonstration of any viral protein interacting directly with FIH. Our data reveal a new mechanism by which viruses reprogram HIF, a master regulator of cellular metabolism, and also show a new role for the ANK family of poxvirus proteins., (Copyright © 2016 American Society for Microbiology.)

Published

2016

24. Proteoform-Specific Insights into Cellular Proteome Regulation.

Author

Norris EL, Headlam MJ, Dave KA, Smith DD, Bukreyev A, Singh T, Jayakody BA, Chappell KJ, Collins PL, and Gorman JJ

Subjects

A549 Cells metabolism, Chromatography, Liquid methods, Gene Expression Regulation, Humans, Phosphorylation, Proteolysis, Tandem Mass Spectrometry methods, A549 Cells virology, Proteome metabolism, Proteomics methods, Respiratory Syncytial Virus, Human physiology

Abstract

Knowledge regarding compositions of proteomes at the proteoform level enhances insights into cellular phenotypes. A strategy is described herein for discovery of proteoform-specific information about cellular proteomes. This strategy involved analysis of data obtained by bottom-up mass spectrometry of multiple protein OGE separations on a fraction by fraction basis. The strategy was exemplified using five matched sets of lysates of uninfected and human respiratory syncytial virus-infected A549 cells. Template matching demonstrated that 67.3% of 10475 protein profiles identified focused to narrow pI windows indicative of efficacious focusing. Furthermore, correlation between experimental and theoretical pI gradients indicated reproducible focusing. Based on these observations a proteoform profiling strategy was developed to identify proteoforms, detect proteoform diversity and discover potential proteoform regulation. One component of this strategy involved examination of the focusing profiles for protein groups. A novel concordance analysis facilitated differentiation between proteoforms, including proteoforms generated by alternate splicing and proteolysis. Evaluation of focusing profiles and concordance analysis were applicable to cells from a single and/or multiple biological states. Statistical analyses identified proteoform variation between biological states. Regulation relevant to cellular responses to human respiratory syncytial virus was revealed. Western blotting and Protomap analyses validated the proteoform regulation. Discovery of STAT1, WARS, MX1, and HSPB1 proteoform regulation by human respiratory syncytial virus highlighted the impact of the profiling strategy. Novel truncated proteoforms of MX1 were identified in infected cells and phosphorylation driven regulation of HSPB1 proteoforms was correlated with infection. The proteoform profiling strategy is generally applicable to investigating interactions between viruses and host cells and the analysis of other biological systems., (© 2016 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2016

25. Proteomic changes occurring in the malaria mosquitoes Anopheles gambiae and Anopheles stephensi during aging.

Author

Sikulu MT, Monkman J, Dave KA, Hastie ML, Dale PE, Kitching RL, Killeen GF, Kay BH, Gorman JJ, and Hugo LE

Subjects

Animals, Anopheles parasitology, Malaria transmission, Plasmodium, Aging physiology, Anopheles metabolism, Gene Expression Regulation physiology, Insect Proteins biosynthesis, Proteomics

Abstract

The age of mosquitoes is a crucial determinant of their ability to transmit pathogens and their resistance to insecticides. We investigated changes to the abundance of proteins found in heads and thoraces of the malaria mosquitoes Anopheles gambiae and Anopheles stephensi as they aged. Protein expression changes were assessed using two-dimensional difference gel electrophoresis and the identity of differentially expressed proteins was determined by using either matrix-assisted laser desorption ionization tandem time-of-flight mass spectrometry or capillary high-pressure liquid chromatography coupled with a linear ion-trap (LTQ)-Orbitrap XL hybrid mass spectrometer. Protein biomarkers were validated by semi quantitative Western blot analysis. Nineteen and nine age dependent protein spots were identified for A. stephensi and A. gambiae, respectively. Among the proteins down-regulated with age were homologs of ADF/Cofilin, cytochome c1, heat shock protein-70 and eukaryotic translation initiation factor 5A (eIF5a). Proteins up-regulated with age included probable methylmalonate-semialdehyde dehydrogenase, voltage-dependent anion-selective channel and fructose bisphosphate aldolase. Semi quantitative Western blot analysis confirmed expression patterns observed by 2-D DIGE for eIF5a and ADF/Cofilin. Further work is recommended to determine whether these biomarkers are robust to infection, blood feeding and insecticide resistance. Robust biomarkers could then be incorporated into rapid diagnostic assays for ecological and epidemiological studies., Biological Significance: In this study, we have identified several proteins with characteristic changes in abundance in both A. gambiae and A. stephensi during their aging process. These changes may highlight underlying mechanisms beneath the relationship between mosquito age and factors affecting Plasmodium transmission and mosquito control. The similarity of changes in protein abundance between these species and the primary dengue vector Aedes aegypti, has revealed conserved patterns of aging-specific protein regulation., (Copyright © 2015 Elsevier B.V. All rights reserved.)

Published

2015

26. Mass spectrometry identification of age-associated proteins from the malaria mosquitoes Anopheles gambiae s.s. and Anopheles stephensi.

Author

Sikulu MT, Monkman J, Dave KA, Hastie ML, Dale PE, Kitching RL, Killeen GF, Kay BH, Gorman JJ, and Hugo LE

Abstract

This study investigated proteomic changes occurring in Anopheles gambiae and Anopheles stephensi during adult mosquito aging. These changes were evaluated using two-dimensional difference gel electrophoresis (2D-DIGE) and the identities of aging related proteins were determined using capillary high-pressure liquid chromatography (capHPLC) coupled with a linear ion-trap (LTQ)-Orbitrap XL hybrid mass spectrometry (MS). Here, we have described the techniques used to determine age associated proteomic changes occurring in heads and thoraces across three age groups; 1, 9 and 17 d old A. gambiae and 4 age groups; 1, 9, 17 and 34 d old A. stephensi. We have provided normalised spot volume raw data for all protein spots that were visible on 2D-DIGE images for both species and processed Orbitrap mass spectrometry data. For public access, mass spectrometry raw data are available via ProteomeXchange with identifier PXD002153. A detailed description of this study has been described elsewhere [1].

Published

2015

27. Oxygen-dependent hydroxylation by FIH regulates the TRPV3 ion channel.

Author

Karttunen S, Duffield M, Scrimgeour NR, Squires L, Lim WL, Dallas ML, Scragg JL, Chicher J, Dave KA, Whitelaw ML, Peers C, Gorman JJ, Gleadle JM, Rychkov GY, and Peet DJ

Subjects

Amino Acid Sequence, Ankyrin Repeat genetics, HEK293 Cells, Humans, Hydroxylation genetics, Hypoxia-Inducible Factor 1, alpha Subunit genetics, Mixed Function Oxygenases antagonists & inhibitors, Mixed Function Oxygenases genetics, Mutation, Oxygen metabolism, Protein Binding, Repressor Proteins antagonists & inhibitors, Repressor Proteins genetics, TRPV Cation Channels genetics, Cell Hypoxia genetics, Hypoxia-Inducible Factor 1, alpha Subunit metabolism, Mixed Function Oxygenases metabolism, Repressor Proteins metabolism, TRPV Cation Channels metabolism

Abstract

Factor inhibiting HIF (FIH, also known as HIF1AN) is an oxygen-dependent asparaginyl hydroxylase that regulates the hypoxia-inducible factors (HIFs). Several proteins containing ankyrin repeat domains (ARDs) have been characterised as substrates of FIH, although there is little evidence for a functional consequence of hydroxylation on these substrates. This study demonstrates that the transient receptor potential vanilloid 3 (TRPV3) channel is hydroxylated by FIH on asparagine 242 within the cytoplasmic ARD. Hypoxia, FIH inhibitors and mutation of asparagine 242 all potentiated TRPV3-mediated current, without altering TRPV3 protein levels, indicating that oxygen-dependent hydroxylation inhibits TRPV3 activity. This novel mechanism of channel regulation by oxygen-dependent asparaginyl hydroxylation is likely to extend to other ion channels., (© 2015. Published by The Company of Biologists Ltd.)

Published

2015

28. A comprehensive proteomic view of responses of A549 type II alveolar epithelial cells to human respiratory syncytial virus infection.

Author

Dave KA, Norris EL, Bukreyev AA, Headlam MJ, Buchholz UJ, Singh T, Collins PL, and Gorman JJ

Subjects

Cell Extracts chemistry, Cell Line, Chromatography, High Pressure Liquid, Epithelial Cells metabolism, Epithelial Cells virology, Gene Expression Regulation, Host-Pathogen Interactions genetics, Humans, Interferons genetics, Interferons immunology, Interferons metabolism, NF-kappa B p52 Subunit genetics, NF-kappa B p52 Subunit immunology, NF-kappa B p52 Subunit metabolism, Peptide Fragments analysis, Proteolysis, Proteome genetics, Proteome metabolism, Respiratory Mucosa metabolism, Respiratory Mucosa virology, Respiratory Syncytial Virus, Human metabolism, Signal Transduction, Tandem Mass Spectrometry, Tumor Necrosis Factor-alpha genetics, Tumor Necrosis Factor-alpha immunology, Tumor Necrosis Factor-alpha metabolism, Viral Proteins genetics, Viral Proteins immunology, Viral Proteins metabolism, Epithelial Cells immunology, Host-Pathogen Interactions immunology, Proteome immunology, Respiratory Mucosa immunology, Respiratory Syncytial Virus, Human immunology

Abstract

Human respiratory syncytial virus is a major respiratory pathogen for which there are no suitable antivirals or vaccines. A better understanding of the host cell response to this virus may redress this problem. The present report concerns analysis of multiple independent biological replicates of control and 24 h infected lysates of A549 cells by two different proteomic workflows. One workflow involved fractionation of lysates by in-solution protein IEF and individual fractions were digested using trypsin prior to capillary HPLC-LTQ-OrbitrapXL-MS/MS. A second workflow involved digestion of whole cell lysates and analysis by nanoUltraHPLC-LTQ-OrbitrapElite-MS/MS. Both workflows resulted in the quantification of viral proteins exclusively in lysates of infected cells in the relative abundances anticipated from previous studies. Unprecedented numbers (3247 - 5010) of host cell protein groups were also quantified and the infection-specific regulation of a large number (191) of these protein groups was evident based on a stringent false discovery rate cut-off (<1%). Bioinformatic analyses revealed that most of the regulated proteins were potentially regulated by type I, II, and III interferon, TNF-α and noncanonical NF-κB2 mediated antiviral response pathways. Regulation of specific protein groups by infection was validated by quantitative Western blotting and the cytokine-/key regulator-specific nature of their regulation was confirmed by comparable analyses of cytokine treated A549 cells. Overall, it is evident that the workflows described herein have produced the most comprehensive proteomic characterization of host cell responses to human respiratory syncytial virus published to date. These workflows will form the basis for analysis of the impacts of specific genes of human respiratory syncytial virus responses of A549 and other cell lines using a gene-deleted version of the virus. They should also prove valuable for the analysis of the impact of other infectious agents on host cells., (© 2014 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2014

29. Bovine ephemeral fever rhabdovirus α1 protein has viroporin-like properties and binds importin β1 and importin 7.

Author

Joubert DA, Blasdell KR, Audsley MD, Trinidad L, Monaghan P, Dave KA, Lieu KG, Amos-Ritchie R, Jans DA, Moseley GW, Gorman JJ, and Walker PJ

Subjects

Amino Acid Motifs, Animals, Cattle, Cell Nucleus genetics, Cell Nucleus metabolism, Ephemeral Fever genetics, Ephemeral Fever virology, Ephemeral Fever Virus, Bovine chemistry, Ephemeral Fever Virus, Bovine genetics, Karyopherins genetics, Nuclear Localization Signals, Protein Binding, Protein Transport, Viral Proteins chemistry, Viral Proteins genetics, beta Karyopherins genetics, Ephemeral Fever metabolism, Ephemeral Fever Virus, Bovine metabolism, Karyopherins metabolism, Viral Proteins metabolism, beta Karyopherins metabolism

Abstract

Bovine ephemeral fever virus (BEFV) is an arthropod-borne rhabdovirus that is classified as the type species of the genus Ephemerovirus. In addition to the five canonical rhabdovirus structural proteins (N, P, M, G, and L), the large and complex BEFV genome contains several open reading frames (ORFs) between the G and L genes (α1, α2/α3, β, and γ) encoding proteins of unknown function. We show that the 10.5-kDa BEFV α1 protein is expressed in infected cells and, consistent with previous predictions based on its structure, has the properties of a viroporin. Expression of a BEFV α1-maltose binding protein (MBP) fusion protein in Escherichia coli was observed to inhibit cell growth and increase membrane permeability to hygromycin B. Increased membrane permeability was also observed in BEFV-infected mammalian cells (but not cells infected with an α1-deficient BEFV strain) and in cells expressing a BEFV α1-green fluorescent protein (GFP) fusion protein, which was shown by confocal microscopy to localize to the Golgi complex. Furthermore, the predicted C-terminal cytoplasmic domain of α1, which contains a strong nuclear localization signal (NLS), was translocated to the nucleus when expressed independently, and in an affinity chromatography assay employing a GFP trap, the full-length α1 was observed to interact specifically with importin β1 and importin 7 but not with importin α3. These data suggest that, in addition to its function as a viroporin, BEFV α1 may modulate components of nuclear trafficking pathways, but the specific role thereof remains unclear. Although rhabdovirus accessory genes occur commonly among arthropod-borne rhabdoviruses, little is known of their functions. Here, we demonstrate that the BEFV α1 ORF encodes a protein which has the structural and functional characteristics of a viroporin. We show that α1 localizes in the Golgi complex and increases cellular permeability. We also show that BEFV α1 binds importin β1 and importin 7, suggesting that it may have a yet unknown role in modulating nuclear trafficking. This is the first functional analysis of an ephemerovirus accessory protein and of a rhabdovirus viroporin.

Published

2014

30. Proteomic biomarkers for ageing the mosquito Aedes aegypti to determine risk of pathogen transmission.

Author

Hugo LE, Monkman J, Dave KA, Wockner LF, Birrell GW, Norris EL, Kienzle VJ, Sikulu MT, Ryan PA, Gorman JJ, and Kay BH

Subjects

Animals, Biomarkers metabolism, Female, Proteomics, Aedes metabolism, Aging, Insect Vectors metabolism, Proteome

Abstract

Biomarkers of the age of mosquitoes are required to determine the risk of transmission of various pathogens as each pathogen undergoes a period of extrinsic incubation in the mosquito host. Using the 2-D Difference Gel Electrophoresis (2-D DIGE) procedure, we investigated the abundance of up to 898 proteins from the Yellow Fever and dengue virus vector, Aedes aegypti, during ageing. By applying a mixed-effects model of protein expression, we identified five common patterns of abundance change during ageing and demonstrated an age-related decrease in variance for four of these. This supported a search for specific proteins with abundance changes that remain tightly associated with ageing for use as ageing biomarkers. Using MALDI-TOF/TOF mass spectrometry we identified ten candidate proteins that satisfied strict biomarker discovery criteria (identified in two out of three multivariate analysis procedures and in two cohorts of mosquitoes). We validated the abundances of the four most suitable candidates (Actin depolymerising factor; ADF, Eukaryotic initiation factor 5A; eIF5A, insect cuticle protein Q17LN8, and Anterior fat body protein; AFP) using semi-quantitative Western analysis of individual mosquitoes of six ages. The redox-response protein Manganese superoxide dismutase (SOD2) and electron shuttling protein Electron transfer oxidoreductase (ETO) were subject to post-translational modifications affecting their charge states with potential effects on function. For the four candidates we show remarkably consistent decreases in abundance during ageing, validating initial selections. In particular, the abundance of AFP is an ideal biomarker candidate for whether a female mosquito has lived long enough to be capable of dengue virus transmission. We have demonstrated proteins to be a suitable class of ageing biomarkers in mosquitoes and have identified candidates for epidemiological studies of dengue and the evaluation of new disease reduction projects targeting mosquito longevity.

Published

2013

31. The human respiratory syncytial virus nonstructural protein 1 regulates type I and type II interferon pathways.

Author

Hastie ML, Headlam MJ, Patel NB, Bukreyev AA, Buchholz UJ, Dave KA, Norris EL, Wright CL, Spann KM, Collins PL, and Gorman JJ

Subjects

Animals, Catalase genetics, Catalase metabolism, Cell Line, Tumor, Chlorocebus aethiops, Cluster Analysis, Gene Expression Regulation, Host-Pathogen Interactions, Humans, Interferon Type I genetics, Interferon Type I physiology, Interferon-gamma genetics, Interferon-gamma physiology, Intracellular Signaling Peptides and Proteins genetics, Intracellular Signaling Peptides and Proteins metabolism, Oxidative Stress, Proteome genetics, Proteome metabolism, STAT1 Transcription Factor metabolism, STAT2 Transcription Factor metabolism, Signal Transduction, Superoxide Dismutase genetics, Superoxide Dismutase metabolism, Transcription, Genetic, Two-Dimensional Difference Gel Electrophoresis, Vero Cells, Interferon Type I metabolism, Interferon-gamma metabolism, Respiratory Syncytial Virus, Human physiology, Viral Nonstructural Proteins physiology

Abstract

Respiratory syncytial viruses encode a nonstructural protein (NS1) that interferes with type I and III interferon and other antiviral responses. Proteomic studies were conducted on human A549 type II alveolar epithelial cells and type I interferon-deficient Vero cells (African green monkey kidney cells) infected with wild-type and NS1-deficient clones of human respiratory syncytial virus to identify other potential pathway and molecular targets of NS1 interference. These analyses included two-dimensional differential gel electrophoresis and quantitative Western blotting. Surprisingly, NS1 was found to suppress the induction of manganese superoxide dismutase (SOD2) expression in A549 cells and to a much lesser degree Vero cells in response to infection. Because SOD2 is not directly inducible by type I interferons, it served as a marker to probe the impact of NS1 on signaling of other cytokines known to induce SOD2 expression and/or indirect effects of type I interferon signaling. Deductive analysis of results obtained from cell infection and cytokine stimulation studies indicated that interferon-γ signaling was a potential target of NS1, possibly as a result of modulation of STAT1 levels. However, this was not sufficient to explain the magnitude of the impact of NS1 on SOD2 induction in A549 cells. Vero cell infection experiments indicated that NS1 targeted a component of the type I interferon response that does not directly induce SOD2 expression but is required to induce another initiator of SOD2 expression. STAT2 was ruled out as a target of NS1 interference using quantitative Western blot analysis of infected A549 cells, but data were obtained to indicate that STAT1 was one of a number of potential targets of NS1. A label-free mass spectrometry-based quantitative approach is proposed as a means of more definitive identification of NS1 targets.

Published

2012

32. Preparation and analysis of proteins and peptides using MALDI TOF/TOF mass spectrometry.

Author

Dave KA, Headlam MJ, Wallis TP, and Gorman JJ

Subjects

Chromatography, High Pressure Liquid instrumentation, Chromatography, High Pressure Liquid methods, Coumaric Acids chemistry, Databases, Protein, Electrophoresis, Gel, Two-Dimensional instrumentation, Electrophoresis, Gel, Two-Dimensional methods, Trypsin metabolism, Peptides analysis, Proteins analysis, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization instrumentation, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization methods, Tandem Mass Spectrometry instrumentation, Tandem Mass Spectrometry methods

Abstract

Matrix-assisted laser desorption/ionization time-of-flight/time-of-flight mass spectrometry (MALDI-TOF/TOF-MS) is a valuable tool for the analysis of peptides and proteins. Particularly useful features include high sensitivity, fast data acquisition, ease of use, and robust instrumentation. Although MALDI is relatively tolerant to buffers and other impurities, substantial sensitivity enhancement can be achieved through removal of non-analyte components of samples. Therefore, sample processing to remove buffers and impurities can greatly improve the quality of results obtained by MALDI experiments. This unit describes optimized procedures for enzymatic digestion, preparation of MALDI target plates, thin layer matrix preparation, on-target sample cleanup, and capillary HPLC-MALDI co-spotting of analyte and matrix. Procedures are also described for analysis of on-membrane proteins by MALDI-TOF/TOF-MS before tryptic digestion. Some of these procedures are also applicable to protein spots from two-dimensional (2-D) gels. Guidance is also provided for acquisition and interpretation of MS and MS/MS spectra., (© 2011 by John Wiley & Sons, Inc.)

Published

2011

33. Building the preBötzinger complex.

Author

Dave KA

Subjects

Animals, Membrane Proteins metabolism, Mice, Nerve Tissue Proteins metabolism, Neural Pathways embryology, Neural Pathways physiology, Neurogenesis physiology, Periodicity, Receptors, Cell Surface, Receptors, Neurokinin-1 metabolism, Respiration, Somatostatin metabolism, Glutamic Acid metabolism, Homeodomain Proteins metabolism, Interneurons physiology, Medulla Oblongata embryology, Medulla Oblongata physiology, Stem Cells physiology

Published

2010

34. Prostaglandin E2 induces glutamate release from subventricular zone astrocytes.

Author

Dave KA, Platel JC, Huang F, Tian D, Stamboulian-Platel S, and Bordey A

Subjects

Animals, Calcium metabolism, Electroporation, Enzyme-Linked Immunosorbent Assay, Immunohistochemistry, Mice, Neural Stem Cells metabolism, Patch-Clamp Techniques, Receptors, Glutamate metabolism, Receptors, N-Methyl-D-Aspartate metabolism, Astrocytes metabolism, Dinoprostone metabolism, Glutamic Acid metabolism, Neural Stem Cells cytology, Neurogenesis physiology

Abstract

It was recently reported that in one of the adult neurogenetic zones, the subventricular zone (SVZ), astrocyte-like cells release glutamate upon intracellular Ca2+ increases. However, the signals that control Ca2+ activity and glutamate release from SVZ astrocytes are not known. Here, we examined whether prostaglandin E2 (PGE2), which induces glutamate release from mature astrocytes, is such a signal. Using the gramicidin-perforated patch-clamp technique, we show that the activity of N-Methyl-D-Aspartate receptor (NMDAR) channel in neuroblasts is a high fidelity sensor of ambient glutamate levels. Using such sensors, we found that application of PGE2 led to increased ambient glutamate levels in the SVZ. In parallel experiments, PGE2 induced an increase in intracellular Ca2+ levels in SVZ cells, in particular astrocyte-like cells, as shown using Ca2+ imaging. Finally, a PGE2 enzyme immunoassay showed that the choroid plexus of the lateral ventricle and to a lesser extent the SVZ (ten-fold less) released PGE2. These findings suggest that PGE2 is a physiological signal for inducing glutamate release from SVZ astrocytes that is important for controlling neuroblast survival and proliferation. This signal may be accentuated following ischemia or injury-induced PGE2 release and may contribute to the injury-associated increased neurogenesis.

Published

2010

35. Regulating brain size.

Author

Dave KA

Subjects

1-Alkyl-2-acetylglycerophosphocholine Esterase metabolism, Animals, Humans, Mice, Microtubule-Associated Proteins metabolism, Mitosis genetics, Organ Size genetics, Brain anatomy & histology, Nuclear Proteins genetics, Stem Cells physiology

Published

2010

36. NMDA receptors activated by subventricular zone astrocytic glutamate are critical for neuroblast survival prior to entering a synaptic network.

Author

Platel JC, Dave KA, Gordon V, Lacar B, Rubio ME, and Bordey A

Subjects

Animals, Animals, Newborn, Cell Differentiation physiology, Cell Movement physiology, Cell Survival physiology, Cerebral Ventricles cytology, Cerebral Ventricles metabolism, Gene Knockout Techniques, Mice, Mice, Transgenic, Nerve Net cytology, Nerve Net metabolism, Neurons cytology, Olfactory Bulb cytology, Olfactory Bulb metabolism, Astrocytes metabolism, Glutamic Acid metabolism, Neurogenesis physiology, Neurons metabolism, Receptors, N-Methyl-D-Aspartate metabolism, Synapses metabolism

Abstract

Even before integrating into existing circuitry, adult-born neurons express receptors for neurotransmitters, but the intercellular mechanisms and their impact on neurogenesis remain largely unexplored. Here, we show that neuroblasts born in the postnatal subventricular zone (SVZ) acquire NMDA receptors (NMDARs) during their migration to the olfactory bulb. Along their route, neuroblasts are ensheathed by astrocyte-like cells expressing vesicular glutamate release machinery. Increasing calcium in these specialized astrocytes induced NMDAR activity in neuroblasts, and blocking astrocytic vesicular release eliminated spontaneous NMDAR activity. Single-cell knockout of NMDARs using neonatal electroporation resulted in neuroblast apoptosis at the time of NMDAR acquisition. This cumulated in a 40% loss of neuroblasts along their migratory route, demonstrating that NMDAR acquisition is critical for neuroblast survival prior to entering a synaptic network. In addition, our findings suggest an unexpected mechanism wherein SVZ astrocytes use glutamate signaling through NMDARs to control the number of adult-born neurons reaching their final destination., ((c) 2010 Elsevier Inc. All rights reserved.)

Published

2010

37. GABA increases Ca2+ in cerebellar granule cell precursors via depolarization: implications for proliferation.

Author

Dave KA and Bordey A

Subjects

Calcium metabolism, Cell Proliferation drug effects, Cells, Cultured, Cerebellum cytology, Cerebellum growth & development, Glutamic Acid pharmacology, Humans, gamma-Aminobutyric Acid pharmacology, Cerebellar Neoplasms metabolism, Cerebellum metabolism, Glutamic Acid metabolism, Medulloblastoma metabolism, Receptors, GABA-A metabolism, Signal Transduction physiology, gamma-Aminobutyric Acid metabolism

Abstract

The amino acids glutamate and gamma-aminobutyric acid (GABA) have primarily been characterized as the most prevalent excitatory and inhibitory, respectively, neurotransmitters in the vertebrate central nervous system. However, the role of these signaling molecules extends far beyond the synapse. GABA, glutamate, and their complement of receptors are essential signaling molecules that regulate developmental processes in both embryonic and young adult mammals. In this review, we describe the current knowledge on the role of GABA and glutamate in development, focusing on the perinatal cerebellum. We will then present novel data suggesting that GABA depolarizes granule cell precursors via GABA(A) receptors, which leads to calcium increases in these cells. Finally, we will consider the role of GABA and glutamate signaling on cell proliferation and perhaps neural cancers. From our review of the literature and these data, we hypothesize that GABA(A) receptors and metabotropic glutamate receptors may be a novel target for the pharmacological regulation of the cerebellar tumors, medulloblastomas.

Published

2009

38. Sulfonation and phosphorylation of regions of the dioxin receptor susceptible to methionine modifications.

Author

Dave KA, Whelan F, Bindloss C, Furness SG, Chapman-Smith A, Whitelaw ML, and Gorman JJ

Subjects

Amino Acid Sequence, Animals, Cell Line, Chromatography, High Pressure Liquid, Humans, Mice, Molecular Sequence Data, Mutant Proteins chemistry, Mutant Proteins metabolism, Peptides chemistry, Phosphates metabolism, Phosphoprotein Phosphatases metabolism, Phosphorylation, Phosphoserine metabolism, Receptors, Aryl Hydrocarbon chemistry, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Trypsin metabolism, Methionine metabolism, Protein Processing, Post-Translational, Receptors, Aryl Hydrocarbon metabolism, Sulfur metabolism

Abstract

Tagged murine dioxin receptor was purified from mammalian cells, digested with trypsin, and analyzed by capillary HPLC-MALDI-TOF/TOF-MS and -MS/MS. Several chromatographically distinct semitryptic peptides matching two regions spanning residues Glu(409)-Arg(424) and Ser(547)-Arg(555) of the dioxin receptor were revealed by de novo sequencing. Methionine residues at 418 and 548 were detected in these peptides as either unmodified or modified by moieties of 16 (oxidation) or 57 amu (S-carboxamidomethylation) or in a form corresponding to degradative removal of 105 amu from the S-carboxamidomethylated methionine. MS/MS spectra revealed that the peptides containing modified methionine residues also existed in forms with a modification of +80 amu on serine residues 411, 415, and 547. The MS/MS spectra of these peptide ions also revealed diagnostic neutral loss fragment ions of 64, 98, and/or 80 amu, and in some instances combinations of these neutral losses were apparent. Taken together, these data indicated that serines 411 and 547 of the dioxin receptor were sulfonated and serine 415 was phosphorylated. Separate digests of the dioxin receptor were prepared in H(2)(16)O and H(2)(18)O, and enzymatic dephosphorylation was subsequently performed on the H(2)(16)O digest only. The digests were mixed in equal proportions and analyzed by capillary HPLC-MALDI-TOF/TOF-MS and -MS/MS. This strategy confirmed assignment of sulfonation as the cause of the +80-amu modifications on serines 411 and 547 and phosphorylation as the predominant cause of the +80-amu modification of serine 415. The relative quantitation of phosphorylation and sulfonation enabled by this differential phosphatase strategy also suggested the presence of sulfonation on a serine other than residue 411 within the sequence spanning Glu(409)-Arg(424). This represents the first description of post-translational sulfonation sites and identification of a new phosphorylation site of the latent dioxin receptor. Furthermore this is only the second report of serine sulfonation of eukaryotic proteins. Mutagenesis studies are underway to assess the functional consequences of these modifications.

Published

2009

39. Control of neuroblast production and migration by converging GABA and glutamate signals in the postnatal forebrain.

Author

Platel JC, Dave KA, and Bordey A

Subjects

Adult, Cell Differentiation, Cell Movement, Cell Proliferation, Humans, Neurotransmitter Agents metabolism, Prosencephalon cytology, Adult Stem Cells cytology, Adult Stem Cells physiology, Glutamic Acid metabolism, Neurons cytology, Neurons physiology, Prosencephalon metabolism, gamma-Aminobutyric Acid metabolism

Abstract

The production of adult-born neurons is an ongoing process accounting for > 10,000 immature neurons migrating to the olfactory bulb every day. This high turnover rate necessitates profound control mechanisms converging onto neural stem cells and neuroblasts to achieve adequate adult-born neuron production. Here, we elaborate on a novel epigenetic control of adult neurogenesis via highly coordinated, non-synaptic, intercellular signalling. This communication engages the neurotransmitters GABA and glutamate, whose extracellular concentrations depend on neuroblast number and high affinity uptake systems in stem cells. Previous studies show that neuroblasts release GABA providing a negative feedback control of stem cell proliferation. Recent findings show an unexpected mosaic expression of glutamate receptors leading to calcium elevations in migrating neuroblasts. We speculate that stem cells release glutamate that activates glutamate receptors on migrating neuroblasts providing them with migratory and survival cues. In addition, we propose that the timing of neurotransmitter release and their spatial diffusion will determine the convergent coactivation of neuroblasts and stem cells, and provide a steady-state level of neuroblast production. Upon external impact or injury this signalling may adjust to a new steady-state level, thus providing non-synaptic scaling of neuroblast production.

Published

2008

40. Neural networking: Yale and Hebb at the 37th annual meeting of the Society for Neuroscience.

Author

Dave KA

Subjects

Neural Networks, Computer, Societies, Scientific

Published

2008