Your search keyword '"Hubbard Kyle S"' showing total 16 results

1. Detection of Burkholderia pseudomallei O-antigen serotypes in near-neighbor species

Author

Stone Joshua K, Mayo Mark, Grasso Stephanie A, Ginther Jennifer L, Warrington Stephanie D, Allender Christopher J, Doyle Adina, Georgia Shalamar, Kaestli Mirjam, Broomall Stacey M, Karavis Mark A, Insalaco Joseph M, Hubbard Kyle S, McNew Lauren A, Gibbons Henry S, Currie Bart J, Keim Paul, and Tuanyok Apichai

Subjects

Microbiology, QR1-502

Abstract

Abstract Background Burkholderia pseudomallei is the etiological agent of melioidosis and a CDC category B select agent with no available effective vaccine. Previous immunizations in mice have utilized the lipopolysaccharide (LPS) as a potential vaccine target because it is known as one of the most important antigenic epitopes in B. pseudomallei. Complicating this strategy are the four different B. pseudomallei LPS O-antigen types: A, B, B2, and rough. Sero-crossreactivity is common among O-antigens of Burkholderia species. Here, we identified the presence of multiple B. pseudomallei O-antigen types and sero-crossreactivity in its near-neighbor species. Results PCR screening of O-antigen biosynthesis genes, phenotypic characterization using SDS-PAGE, and immunoblot analysis showed that majority of B. mallei and B. thailandensis strains contained the typical O-antigen type A. In contrast, most of B. ubonensis and B. thailandensis-like strains expressed the atypical O-antigen types B and B2, respectively. Most B. oklahomensis strains expressed a distinct and non-seroreactive O-antigen type, except strain E0147 which expressed O-antigen type A. O-antigen type B2 was also detected in B. thailandensis 82172, B. ubonensis MSMB108, and Burkholderia sp. MSMB175. Interestingly, B. thailandensis-like MSMB43 contained a novel serotype B positive O-antigen. Conclusions This study expands the number of species which express B. pseudomallei O-antigen types. Further work is required to elucidate the full structures and how closely these are to the B. pseudomallei O-antigens, which will ultimately determine the efficacy of the near-neighbor B serotypes for vaccine development.

Published

2012

2. High yield derivation of enriched glutamatergic neurons from suspension-cultured mouse ESCs for neurotoxicology research

Author

Hubbard Kyle S, Gut Ian M, Lyman Megan E, Tuznik Kaylie M, Mesngon Mariano T, and McNutt Patrick M

Subjects

Mouse embryonic stem cells, Neurotoxicity, In vitro modeling, BoNT, LTX, Glutamate, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571, Neurophysiology and neuropsychology, QP351-495

Abstract

Abstract Background Recently, there has been a strong emphasis on identifying an in vitro model for neurotoxicity research that combines the biological relevance of primary neurons with the scalability, reproducibility and genetic tractability of continuous cell lines. Derived neurons should be homotypic, exhibit neuron-specific gene expression and morphology, form functioning synapses and consistently respond to neurotoxins in a fashion indistinguishable from primary neurons. However, efficient methods to produce neuronal populations that are suitable alternatives to primary neurons have not been available. Methods With the objective of developing a more facile, robust and efficient method to generate enriched glutamatergic neuronal cultures, we evaluated the neurogenic capacity of three mouse embryonic stem cell (ESC) lines (R1, C57BL/6 and D3) adapted to feeder-independent suspension culture. Neurogenesis and neuronal maturation were characterized as a function of time in culture using immunological, genomic, morphological and functional metrics. The functional responses of ESNs to neurotropic toxins with distinctly different targets and mechanisms of toxicity, such as glutamate, α-latrotoxin (LTX), and botulinum neurotoxin (BoNT), were also evaluated. Results Suspension-adapted ESCs expressed markers of pluripotency through at least 30 passages, and differentiation produced 97×106 neural progenitor cells (NPCs) per 10-cm dish. Greater than 99% of embryonic stem cell-derived neurons (ESNs) expressed neuron-specific markers by 96 h after plating and rapidly developed complex axodendritic arbors and appropriate compartmentalization of neurotypic proteins. Expression profiling demonstrated the presence of transcripts necessary for neuronal function and confirmed that ESN populations were predominantly glutamatergic. Furthermore, ESNs were functionally receptive to all toxins with sensitivities and responses consistent with primary neurons. Conclusions These findings demonstrate a cost-effective, scalable and flexible method to produce a highly enriched glutamatergic neuron population. The functional characterization of pathophysiological responses to neurotropic toxins and the compatibility with multi-well plating formats were used to demonstrate the suitability of ESNs as a discovery platform for molecular mechanisms of action, moderate-throughput analytical approaches and diagnostic screening. Furthermore, for the first time we demonstrate a cell-based model that is sensitive to all seven BoNT serotypes with EC50 values comparable to those reported in primary neuron populations. These data providing compelling evidence that ESNs offer a neuromimetic platform suitable for the evaluation of molecular mechanisms of neurotoxicity.

Published

2012

3. Whole-Genome Sequencing in Microbial Forensic Analysis of Gamma-Irradiated Microbial Materials

Author

Broomall, Stacey M., primary, Ait Ichou, Mohamed, additional, Krepps, Michael D., additional, Johnsky, Lauren A., additional, Karavis, Mark A., additional, Hubbard, Kyle S., additional, Insalaco, Joseph M., additional, Betters, Janet L., additional, Redmond, Brady W., additional, Rivers, Bryan A., additional, Liem, Alvin T., additional, Hill, Jessica M., additional, Fochler, Edward T., additional, Roth, Pierce A., additional, Rosenzweig, C. Nicole, additional, Skowronski, Evan W., additional, and Gibbons, Henry S., additional

Published

2016

4. Pangenome Analysis of Burkholderia pseudomallei: Genome Evolution Preserves Gene Order despite High Recombination Rates

Author

Spring-Pearson, Senanu M., Stone, Joshua K., Doyle, Adina, Allender, Christopher J., Okinaka, Richard T., Mayo, Mark J., Broomall, Stacey M., Hill, Jessica M., Karavis, Mark A., Hubbard, Kyle S., Insalaco, Joseph M., McNew, Lauren A., Rosenzweig, C. Nicole, Gibbons, Henry, Currie, Bart J., Wagner, David, Keim, Paul, Tuanyok, Apichai, Spring-Pearson, Senanu M., Stone, Joshua K., Doyle, Adina, Allender, Christopher J., Okinaka, Richard T., Mayo, Mark J., Broomall, Stacey M., Hill, Jessica M., Karavis, Mark A., Hubbard, Kyle S., Insalaco, Joseph M., McNew, Lauren A., Rosenzweig, C. Nicole, Gibbons, Henry, Currie, Bart J., Wagner, David, Keim, Paul, and Tuanyok, Apichai

Abstract

The pangenomic diversity in Burkholderia pseudomallei is high, with approximately 5.8% of the genome consisting of genomic islands. Genomic islands are known hotspots for recombination driven primarily by site-specific recombination associated with tRNAs. However, recombination rates in other portions of the genome are also high, a feature we expected to disrupt gene order. We analyzed the pangenome of 37 isolates of B. pseudomallei and demonstrate that the pangenome is ‘open’, with approximately 136 new genes identified with each new genome sequenced, and that the global core genome consists of 4568±16 homologs. Genes associated with metabolism were statistically overrepresented in the core genome, and genes associated with mobile elements, disease, and motility were primarily associated with accessory portions of the pangenome. The frequency distribution of genes present in between 1 and 37 of the genomes analyzed matches well with a model of genome evolution in which 96% of the genome has very low recombination rates but 4% of the genome recombines readily. Using homologous genes among pairs of genomes, we found that gene order was highly conserved among strains, despite the high recombination rates previously observed. High rates of gene transfer and recombination are incompatible with retaining gene order unless these processes are either highly localized to specific sites within the genome, or are characterized by symmetrical gene gain and loss. Our results demonstrate that both processes occur: localized recombination introduces many new genes at relatively few sites, and recombination throughout the genome generates the novel multi-locus sequence types previously observed while preserving gene order.

Published

2015

5. Pangenome Analysis of Burkholderia pseudomallei: Genome Evolution Preserves Gene Order despite High Recombination Rates

Author

Spring-Pearson, Senanu M., primary, Stone, Joshua K., additional, Doyle, Adina, additional, Allender, Christopher J., additional, Okinaka, Richard T., additional, Mayo, Mark, additional, Broomall, Stacey M., additional, Hill, Jessica M., additional, Karavis, Mark A., additional, Hubbard, Kyle S., additional, Insalaco, Joseph M., additional, McNew, Lauren A., additional, Rosenzweig, C. Nicole, additional, Gibbons, Henry S., additional, Currie, Bart J., additional, Wagner, David M., additional, Keim, Paul, additional, and Tuanyok, Apichai, additional

Published

2015

6. Novel Application of Stem Cell-Derived Neurons to Evaluate the Time-and Dose-Dependent Progression of Excitotoxic Injury

Author

ARMY MEDICAL RESEARCH INST OF CHEMICAL DEFENSE ABERDEEN PROVING GROUND MD, Gut, Ian M, Beske, Phillip H, Hubbard, Kyle S, Lyman, Megan E, Hamilton, Tracey A, McNutt, Patrick M, ARMY MEDICAL RESEARCH INST OF CHEMICAL DEFENSE ABERDEEN PROVING GROUND MD, Gut, Ian M, Beske, Phillip H, Hubbard, Kyle S, Lyman, Megan E, Hamilton, Tracey A, and McNutt, Patrick M

Abstract

Glutamate receptor (GluR)-mediated neurotoxicity is implicated in a variety of disorders ranging from ischemia to neural degeneration. Under conditions of elevated glutamate, the excessive activation of GluRs causes internalization of pathologic levels of Ca2+, culminating in bioenergetic failure, organelle degradation, and cell death. Efforts to characterize cellular and molecular aspects of excitotoxicity and conduct therapeutic screening for pharmacologic inhibitors of excitogenic progression have been hindered by limitations associated with primary neuron culture. To address this, we evaluated glutamate-induced neurotoxicity in highly enriched glutamatergic neurons (ESNs) derived from murine embryonic stem cells. As of 18 days in vitro (DIV 18), ESNs were synaptically coupled, exhibited spontaneous network activity with neurotypic mEPSCs and expressed NMDARs and AMPARs with physiological current:voltage behaviors. Addition of 0.78 200 mM glutamate evoked reproducible time- and dose-dependent metabolic failure in 6 h, with a calculated EC50 value of 0.44 mM at 24 h. Using a combination of cell viability assays and electrophysiology, we determined that glutamate-induced toxicity was specifically mediated by NMDARs and could be inhibited by addition of NMDAR antagonists, increased extracellular Mg2+ or substitution of Ba2+ for Ca2+. Glutamate treatment evoked neurite fragmentation and focal swelling by both immunocytochemistry and scanning electron microscopy. Presentation of morphological markers of cell death was dose-dependent, with 0.78 200 mM glutamate resulting in apoptosis and 3000 mM glutamate generating a mixture of necrosis and apoptosis. Addition of neuroprotective small molecules reduced glutamate-induced neurotoxicity in a dosedependent fashion., Published in the Journal of PLOS ONE, v8 n5 Article e64423 p1-13, May 2013. The original document contains color images.

Published

2013

7. Morphological and Functional Differentiation in BE (2)-M17 Neuroblastoma Cells by Treatment with Trans-Retinoic Acid

Author

ARMY MEDICAL RESEARCH INST OF CHEMICAL DEFENSE ABERDEEN PROVING GROUND MD, Andres, Devon, Keyser, Brian M, Petrali, John, Benton, Betty, Hubbard, Kyle S, McNutt, Patrick M, Ray, Radharaman, ARMY MEDICAL RESEARCH INST OF CHEMICAL DEFENSE ABERDEEN PROVING GROUND MD, Andres, Devon, Keyser, Brian M, Petrali, John, Benton, Betty, Hubbard, Kyle S, McNutt, Patrick M, and Ray, Radharaman

Abstract

Background: Immortalized neuronal cell lines can be induced to differentiate into more mature neurons by adding specific compounds or growth factors to the culture medium. This property makes neuronal cell lines attractive as in vitro cell models to study neuronal functions and neurotoxicity. The clonal human neuroblastoma BE(2)-M17 cell line is known to differentiate into a more prominent neuronal cell type by treatment with trans-retinoic acid. However, there is a lack of information on the morphological and functional aspects of these differentiated cells. Results: We studied the effects of trans-retinoic acid treatment on (a) some differentiation marker proteins, (b) types of voltage-gated calcium (Ca2+) channels and (c) Ca2+-dependent neurotransmitter ([3H] glycine) release in cultured BE(2)-M17 cells. Cells treated with 10 M trans-retinoic acid (RA) for 72 hrs exhibited marked changes in morphology to include neurite extensions; presence of P/Q, N and T-type voltage-gated Ca2+ channels; and expression of neuron specific enolase (NSE), synaptosomal-associated protein 25 (SNAP-25), nicotinic acetylcholine receptor 7 (nAChR- 7) and other neuronal markers. Moreover, retinoic acid treated cells had a significant increase in evoked Ca2+-dependent neurotransmitter release capacity. In toxicity studies of the toxic gas, phosgene (CG), that differentiation of M17 cells with RA was required to see the changes in intracellular free Ca2+ concentrations following exposure to CG. Conclusion: Taken together, retinoic acid treated cells had improved morphological features as well as neuronal characteristics and functions; thus, these retinoic acid differentiated BE(2)-M17 cells may serve as a better neuronal model to study neurobiology and/or neurotoxicity., The original document contains color images. Published in BMC Neuroscience, v14 n49, 18 Apr 2013. Sponsored in part by NIH, DoE, and USAMRMC.

Published

2013

8. Detection of Burkholderia pseudomallei O-antigen serotypes in near-neighbor species

Author

Stone, Joshua K., Mayo, Mark J., Grasso, Stephanie A., Ginther, Jennifer L., Warrington, Stephanie D., Allender, Christopher J., Doyle, Adina, Georgia, Shalamar, Kaestli, Mirjam E., Broomall, Stacey M., Karavis, Mark A., Insalaco, Joseph M., Hubbard, Kyle S., McNew, Lauren A., Gibbons, Henry S., Currie, Bart J., Keim, Paul, Tuanyok, Apichai, Stone, Joshua K., Mayo, Mark J., Grasso, Stephanie A., Ginther, Jennifer L., Warrington, Stephanie D., Allender, Christopher J., Doyle, Adina, Georgia, Shalamar, Kaestli, Mirjam E., Broomall, Stacey M., Karavis, Mark A., Insalaco, Joseph M., Hubbard, Kyle S., McNew, Lauren A., Gibbons, Henry S., Currie, Bart J., Keim, Paul, and Tuanyok, Apichai

Abstract

BackgroundBurkholderia pseudomallei is the etiological agent of melioidosis and a CDC category B select agent with no available effective vaccine. Previous immunizations in mice have utilized the lipopolysaccharide (LPS) as a potential vaccine target because it is known as one of the most important antigenic epitopes in B. pseudomallei. Complicating this strategy are the four different B. pseudomallei LPS O-antigen types: A, B, B2, and rough. Sero-crossreactivity is common among O-antigens of Burkholderia species. Here, we identified the presence of multiple B. pseudomallei O-antigen types and sero-crossreactivity in its near-neighbor species.ResultsPCR screening of O-antigen biosynthesis genes, phenotypic characterization using SDS-PAGE, and immunoblot analysis showed that majority of B. mallei and B. thailandensis strains contained the typical O-antigen type A. In contrast, most of B. ubonensis and B. thailandensis-like strains expressed the atypical O-antigen types B and B2, respectively. Most B. oklahomensis strains expressed a distinct and non-seroreactive O-antigen type, except strain E0147 which expressed O-antigen type A. O-antigen type B2 was also detected in B. thailandensis 82172, B. ubonensis MSMB108, and Burkholderia sp. MSMB175. Interestingly, B. thailandensis-like MSMB43 contained a novel serotype B positive O-antigen.ConclusionsThis study expands the number of species which express B. pseudomallei O-antigen types. Further work is required to elucidate the full structures and how closely these are to the B. pseudomallei O-antigens, which will ultimately determine the efficacy of the near-neighbor B serotypes for vaccine development.

Published

2012

9. Compatibility of SYTO 13 and Hoechst 33342 for Longitudinal Imaging of Neuron Viability and Cell Death

Author

ARMY MEDICAL RESEARCH INST OF CHEMICAL DEFENSE ABERDEEN PROVING GROUND MD, Hubbard, Kyle S, Gut, Ian M, Scheeler, Stephen M, Lyman, Megan E, McNutt, Patrick M, ARMY MEDICAL RESEARCH INST OF CHEMICAL DEFENSE ABERDEEN PROVING GROUND MD, Hubbard, Kyle S, Gut, Ian M, Scheeler, Stephen M, Lyman, Megan E, and McNutt, Patrick M

Abstract

Simultaneous use of cell-permeant and impermeant fluorescent nuclear dyes is a common method to study cell viability and cell death progression. Although these assays are usually conducted as end-point studies, time-lapse imaging offers a powerful technique to distinguish temporal changes in cell viability at single-cell resolution. SYTO 13 and Hoechst 33342 are two commonly used cell-permeant nuclear dyes; however their suitability for live imaging has not been well characterized. We compare end-point assays with time-lapse imaging studies over a 6 h period to evaluate the compatibility of these two dyes with longitudinal imaging, using both control neurons and an apoptotic neuron model. In longitudinal assays of untreated neurons, SYTO 13 addition caused acute necrosis within 3 h, whereas neurons imaged with Hoechst remained viable for at least 6 h. In a staurosporine-induced apoptotic model of neurotoxicity, determinations of the mode of cell death and measurements of nuclear size were identical between longitudinal studies using Hoechst and end-point assays. Alternatively, longitudinal studies using 500 nM or 5 nM SYTO 13 were not consistent with end-point assays. SYTO 13 is acutely neurotoxic and when used in longitudinal studies, masked end-stage morphologic evidence of apoptotic cell death. In contrast, a single application of Hoechst evoked no evidence of toxicity over a 6 h period, and was consistent with end-point characterizations of cell viability and nuclear morphology. For longitudinal characterization of acute cell death, Hoechst is a superior option., Published in the Journal of BMC Research Notes, v5 n437 p1-5, 2012. The original document contains color images.

Published

2012

10. High Yield Derivation of Enriched Glutamatergic Neurons from Suspension-Cultured Mouse ESCs for Neurotoxicology Research

Author

ARMY MEDICAL RESEARCH INST OF CHEMICAL DEFENSE ABERDEEN PROVING GROUND MD, Hubbard, Kyle S, Gut, Ian M, Lyman, Megan E, Tuznik, Kaylie M, Mesngon, Mariano T, McNutt, Patrick M, ARMY MEDICAL RESEARCH INST OF CHEMICAL DEFENSE ABERDEEN PROVING GROUND MD, Hubbard, Kyle S, Gut, Ian M, Lyman, Megan E, Tuznik, Kaylie M, Mesngon, Mariano T, and McNutt, Patrick M

Abstract

Recently, there has been a strong emphasis on identifying an in vitro model for neurotoxicity research that combines the biological relevance of primary neurons with the scalability, reproducibility and genetic tractability of continuous cell lines. Derived neurons should be homotypic, exhibit neuron-specific gene expression and morphology, form functioning synapses and consistently respond to neurotoxins in a fashion indistinguishable from primary neurons. However, efficient methods to produce neuronal populations that are suitable alternatives to primary neurons have not been available. With the objective of developing a more facile, robust and efficient method to generate enriched glutamatergic neuronal cultures, we evaluated the neurogenic capacity of three mouse embryonic stem cell (ESC) lines (R1, C57BL/6 and D3) adapted to feeder-independent suspension culture. Neurogenesis and neuronal maturation were characterized as a function of time in culture using immunological, genomic, morphological and functional metrics. The functional responses of ESNs to neurotropic toxins with distinctly different targets and mechanisms of toxicity, such as glutamate, alpha-latrotoxin (LTX), and botulinum neurotoxin (BoNT), were also evaluated. Suspension-adapted ESCs expressed markers of pluripotency through at least 30 passages, and differentiation produced 97 10(6) neural progenitor cells (NPCs) per 10-cm dish. Greater than 99% of embryonic stem cell-derived neurons (ESNs) expressed neuron-specific markers by 96 h after plating and rapidly developed complex axodendritic arbors and appropriate compartmentalization of neurotypic proteins. Expression profiling demonstrated the presence of transcripts necessary for neuronal function and confirmed that ESN populations were predominantly glutamatergic. Furthermore, ESNs were functionally receptive to all toxins with sensitivities and responses consistent with primary neurons., Published in the Journal of BMC Neuroscience, v13 n127 p1-15, 2012. The original document contains color images.

Published

2012

11. Novel Application of Stem Cell-Derived Neurons to Evaluate the Time- and Dose-Dependent Progression of Excitotoxic Injury

Author

Gut, Ian M., primary, Beske, Phillip H., additional, Hubbard, Kyle S., additional, Lyman, Megan E., additional, Hamilton, Tracey A., additional, and McNutt, Patrick M., additional

Published

2013

12. Morphological and functional differentiation in BE(2)-M17 human neuroblastoma cells by treatment with Trans-retinoic acid

Author

Andres, Devon, primary, Keyser, Brian M, additional, Petrali, John, additional, Benton, Betty, additional, Hubbard, Kyle S, additional, McNutt, Patrick M, additional, and Ray, Radharaman, additional

Published

2013

13. Longitudinal RNA sequencing of the deep transcriptome during neurogenesis of cortical glutamatergic neurons from murine ESCs

Author

Hubbard, Kyle S, primary, Gut, Ian M, additional, Lyman, Megan E, additional, and McNutt, Patrick M, additional

Published

2013

14. Compatibility of SYTO 13 and Hoechst 33342 for longitudinal imaging of neuron viability and cell death

Author

Hubbard, Kyle S, primary, Gut, Ian M, additional, Scheeler, Stephen M, additional, Lyman, Megan E, additional, and McNutt, Patrick M, additional

Published

2012

15. Morphological and functional differentiation in BE (2)-M17 human neuroblastoma cells by treatment with Trans-retinoic acid.

Author

Andres, Devon, Keyser, Brian M., Petrali, John, Benton, Betty, Hubbard, Kyle S., McNutt, Patrick M., and Ray, Radharaman

Subjects

TRETINOIN, NERVOUS system tumors, NEUROBLASTOMA, CELL culture, NEUROTOXICOLOGY

Abstract

Background: Immortalized neuronal cell lines can be induced to differentiate into more mature neurons by adding specific compounds or growth factors to the culture medium. This property makes neuronal cell lines attractive as in vitro cell models to study neuronal functions and neurotoxicity. The clonal human neuroblastoma BE(2)-M17 cell line is known to differentiate into a more prominent neuronal cell type by treatment with trans-retinoic acid. However, there is a lack of information on the morphological and functional aspects of these differentiated cells. Results: We studied the effects of trans-retinoic acid treatment on (a) some differentiation marker proteins, (b) types of voltage-gated calcium (Ca2+) channels and (c) Ca2+-dependent neurotransmitter ([3H] glycine) release in cultured BE(2)-M17 cells. Cells treated with 10 μM trans-retinoic acid (RA) for 72 hrs exhibited marked changes in morphology to include neurite extensions; presence of P/Q, N and T-type voltage-gated Ca2+ channels; and expression of neuron specific enolase (NSE), synaptosomal-associated protein 25 (SNAP-25), nicotinic acetylcholine receptor α7 (nAChR-α7) and other neuronal markers. Moreover, retinoic acid treated cells had a significant increase in evoked Ca2+-dependent neurotransmitter release capacity. In toxicity studies of the toxic gas, phosgene (CG), that differentiation of M17 cells with RA was required to see the changes in intracellular free Ca2+ concentrations following exposure to CG. Conclusion: Taken together, retinoic acid treated cells had improved morphological features as well as neuronal characteristics and functions; thus, these retinoic acid differentiated BE(2)-M17 cells may serve as a better neuronal model to study neurobiology and/or neurotoxicity. [ABSTRACT FROM AUTHOR]

Published

2013

16. Whole-Genome Sequencing in Microbial Forensic Analysis of Gamma-Irradiated Microbial Materials.

Author

Broomall SM, Ait Ichou M, Krepps MD, Johnsky LA, Karavis MA, Hubbard KS, Insalaco JM, Betters JL, Redmond BW, Rivers BA, Liem AT, Hill JM, Fochler ET, Roth PA, Rosenzweig CN, Skowronski EW, and Gibbons HS

Subjects

Bacteria genetics, Bacteria growth & development, Forensic Sciences, Gamma Rays, Sequence Analysis, DNA, Bacteria radiation effects, Biological Warfare Agents, Genome, Bacterial radiation effects

Abstract

Effective microbial forensic analysis of materials used in a potential biological attack requires robust methods of morphological and genetic characterization of the attack materials in order to enable the attribution of the materials to potential sources and to exclude other potential sources. The genetic homogeneity and potential intersample variability of many of the category A to C bioterrorism agents offer a particular challenge to the generation of attributive signatures, potentially requiring whole-genome or proteomic approaches to be utilized. Currently, irradiation of mail is standard practice at several government facilities judged to be at particularly high risk. Thus, initial forensic signatures would need to be recovered from inactivated (nonviable) material. In the study described in this report, we determined the effects of high-dose gamma irradiation on forensic markers of bacterial biothreat agent surrogate organisms with a particular emphasis on the suitability of genomic DNA (gDNA) recovered from such sources as a template for whole-genome analysis. While irradiation of spores and vegetative cells affected the retention of Gram and spore stains and sheared gDNA into small fragments, we found that irradiated material could be utilized to generate accurate whole-genome sequence data on the Illumina and Roche 454 sequencing platforms., (Copyright © 2016, American Society for Microbiology. All Rights Reserved.)

Published

2015