Your search keyword '"K. Woods"' showing total 135 results

1. P954: ESTABLISHING THE NATIONAL INSTITUTE FOR HEALTH RESEARCH (NIHR) HEALTH INFORMATICS COLLABORATIVE (HIC) MULTIPLE MYELOMA (MM) REGISTRY

Author

S. Tayabali, S. Moore, M. Jenner, F. Djebbari, L. Romao, L. English, R. Rodriguez, B. Briot Ribeyre, G. Roadknight, K. Varnai, S. Little, J. Davies, K. Woods, C. Davis, F. Borca, J. Olza Meneses, H. Phan, W. K. Wong, and R. Popat

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Published

2022

2. Effective Workplace Stress Reduction Strategies in For-Profit Higher Education

Author

Erin K. Woods

Abstract

The idea that business leaders experience stress in the workplace has resulted in a demand for understanding the negative impact stress has on business. Business managers in for-profit higher education lack strategies to reduce employee workplace stress. Grounded in the job demands-resources model, the purpose of this qualitative single case study was to explore how business managers in for-profit higher education in Arizona reduce employee workplace stress. The participants comprised of three business leaders at a for-profit higher education institution in Arizona who have successfully implemented strategies to reduce employee workplace stress. Data were collected from semistructured interviews with three participants via Zoom and a review of company human resource documents on the company website. An inductive approach was applied to analyze the data. Three themes emerged: provide flexible support resources during times of change, establish effective communication, and recognize barriers that need to be addressed to support employees. A key recommendation to mitigate workplace stress is for business leaders in for-profit higher education to develop resources applicable across their university system that account for unanticipated changes in the industry that may affect business growth and student support. The implications for positive social change include the potential to improve employees' health and happiness in the workplace and at home, which may result in lower health care costs for families and the generation of more income and community involvement as individuals live happier and healthier lives. [The dissertation citations contained here are published with the permission of ProQuest LLC. Further reproduction is prohibited without permission. Copies of dissertations may be obtained by Telephone (800) 1-800-521-0600. Web page: http://www.proquest.com/en-US/products/dissertations/individuals.shtml.]

Published

2022

3. Ciprofloxacin and pegylated G-CSF combined therapy mitigates brain hemorrhage and mortality induced by ionizing irradiation

Author

Juliann G. Kiang, Georgetta Cannon, Matthew G. Olson, Min Zhai, Akeylah K. Woods, Feng Xu, Bin Lin, Xianghong Li, Lisa Hull, Suping Jiang, and Mang Xiao

Subjects

mouse, Ciprofloxacin, G-CSF, radiation, platelet, glial fibrillary acidic protein, Public aspects of medicine, RA1-1270

Abstract

IntroductionBrain hemorrhage was found between 13 and 16 days after acute whole-body 9.5 Gy 60Co-γ irradiation (IR). This study tested countermeasures mitigating brain hemorrhage and increasing survival from IR. Previously, we found that pegylated G-CSF therapy (PEG) (i.e., Neulasta®, an FDA-approved drug) improved survival post-IR by 20–40%. This study investigated whether Ciprofloxacin (CIP) could enhance PEG-induced survival and whether IR-induced brain hemorrhage could be mitigated by PEG alone or combined with CIP.MethodsB6D2F1 female mice were exposed to 60Co-γ-radiation. CIP was fed to mice for 21 days. PEG was injected on days 1, 8, and 15. 30-day survival and weight loss were studied in mice treated with vehicles, CIP, PEG, or PEG + CIP. For the early time point study, blood and sternums on days 2, 4, 9, and 15 and brains on day 15 post-IR were collected. Platelet numbers, brain hemorrhage, and histopathology were analyzed. The cerebellum/pons/medulla oblongata were detected with glial fibrillary acidic protein (GFAP), p53, p16, interleukin-18 (IL-18), ICAM1, Claudin 2, ZO-1, and complement protein 3 (C3).ResultsCIP + PEG enhanced survival after IR by 85% vs. the 30% improvement by PEG alone. IR depleted platelets, which was mitigated by PEG or CIP + PEG. Brain hemorrhage, both surface and intracranial, was observed, whereas the sham mice displayed no hemorrhage. CIP or CIP + PEG significantly mitigated brain hemorrhage. IR reduced GFAP levels that were recovered by CIP or CIP + PEG, but not by PEG alone. IR increased IL-18 levels on day 4 only, which was inhibited by CIP alone, PEG alone, or PEG + CIP. IR increased C3 on day 4 and day 15 and that coincided with the occurrence of brain hemorrhage on day 15. IR increased phosphorylated p53 and p53 levels, which was mitigated by CIP, PEG or PEG + CIP. P16, Claudin 2, and ZO-1 were not altered; ICAM1 was increased.DiscussionCIP + PEG enhanced survival post-IR more than PEG alone. The Concurrence of brain hemorrhage, C3 increases and p53 activation post-IR suggests their involvement in the IR-induced brain impairment. CIP + PEG effectively mitigated the brain lesions, suggesting effectiveness of CIP + PEG therapy for treating the IR-induced brain hemorrhage by recovering GFAP and platelets and reducing C3 and p53.

Published

2023

4. Kisspeptin Is Upregulated at the Maternal-Fetal Interface of the Preeclamptic-like BPH/5 Mouse and Normalized after Synchronization of Sex Steroid Hormones

Author

Viviane C. L. Gomes, Ashley K. Woods, Kassandra R. Crissman, Camille A. Landry, Kalie F. Beckers, Bryce M. Gilbert, Lucas R. Ferro, Chin-Chi Liu, Erin L. Oberhaus, and Jenny L. Sones

Subjects

Kiss1/Kiss1r, GPR54, trophoblast, estrogen, progesterone, Reproduction, QH471-489

Abstract

Insufficient invasion of conceptus-derived trophoblast cells in the maternal decidua is a key event in the development of early-onset preeclampsia (PE), a subtype of PE associated with high maternal and fetal morbidity and mortality. Kisspeptins, a family of peptides previously shown to inhibit trophoblast cell invasion, have been implicated in the pathogenesis of early-onset PE. However, a role of kisspeptin signaling during the genesis of this syndrome has not been elucidated. Herein, we used the preeclamptic-like BPH/5 mouse model to investigate kisspeptin expression and potential upstream regulatory mechanisms in a PE-like syndrome. Expression of the kisspeptin encoding gene, Kiss1, and the 10-amino-acid kisspeptide (Kp-10), are upregulated in the non-pregnant uterus of BPH/5 females during diestrus and in the maternal-fetal interface during embryonic implantation and decidualization. Correspondingly, the dysregulation of molecular pathways downstream to kisspeptins also occurs in this mouse model. BPH/5 females have abnormal sex steroid hormone profiles during early gestation. In this study, the normalization of circulating concentrations of 17β-estradiol (E2) and progesterone (P4) in pregnant BPH/5 females not only mitigated Kiss1 upregulation, but also rescued the expression of multiple molecules downstream to kisspeptin and ameliorated adverse fetoplacental outcomes. Those findings suggest that uterine Kiss1 upregulation occurs pre-pregnancy and persists during early gestation in a PE-like mouse model. Moreover, this study highlights the role of sex steroid hormones in uteroplacental Kiss1 dysregulation and the improvement of placentation by normalization of E2, P4 and Kiss1.

Published

2022

5. The role of the anterior insular during targeted helping behavior in male rats

Author

Stewart S. Cox, Angela M. Kearns, Samuel K. Woods, Brogan J. Brown, Samantha J. Brown, and Carmela M. Reichel

Subjects

Medicine, Science

Abstract

Abstract Empathy, the understanding of the emotional state of others, can be examined across species using the Perception Action Model, where shared affect promotes an action by “Observers” to aid a distressed “Target”. The anterior insula (AI) has garnered interest in empathic behavior due to its role integrating sensory and emotional information of self and other. In the following studies, the AI was inhibited pharmacologically and chemogenetically during targeted helping. We demonstrate the insula is active during, and is necessary for the maintenance of, targeted helping. Analysis of ultrasonic vocalizations revealed distress calls from Targets increased when Observers’ helping was attenuated due to insula inhibition. Targets’ elevated distress was directly correlated to Observers’ diminished helping behavior, suggesting emotional transfer between Observer and Target is blunted following Observer AI inhibition. Finally, the AI may selectively blunt targeted helping, as social exploration did not change in a social reward place conditioning task. These studies help further establish the anterior insula as a critical node in the empathic brain during targeted helping, even in the absence of direct social contact.

Published

2022

6. Aortic Remodeling Kinetics in Response to Coarctation-Induced Mechanical Perturbations

Author

Arash Ghorbannia, Mehdi Maadooliat, Ronald K. Woods, Said H. Audi, Brandon J. Tefft, Claudio Chiastra, El Sayed H. Ibrahim, and John F. LaDisa

Subjects

pathological remodeling, arterial adaptation, homeostasis, hypertension, smooth muscle cell proliferation, coarctation of the aorta, Biology (General), QH301-705.5

Abstract

Background: Coarctation of the aorta (CoA; constriction of the proximal descending thoracic aorta) is among the most common congenital cardiovascular defects. Coarctation-induced mechanical perturbations trigger a cycle of mechano-transduction events leading to irreversible precursors of hypertension including arterial thickening, stiffening, and vasoactive dysfunction in proximal conduit arteries. This study sought to identify kinetics of the stress-mediated compensatory response leading to these alterations using a preclinical rabbit model of CoA. Methods: A prior growth and remodeling (G&R) framework was reformulated and fit to empirical measurements from CoA rabbits classified into one control and nine CoA groups of various severities and durations (n = 63, 5–11/group). Empirical measurements included Doppler ultrasound imaging, uniaxial extension testing, catheter-based blood pressure, and wire myography, yielding the time evolution of arterial thickening, stiffening, and vasoactive dysfunction required to fit G&R constitutive parameters. Results: Excellent agreement was observed between model predictions and observed patterns of arterial thickening, stiffening, and dysfunction among all CoA groups. For example, predicted vascular impairment was not significantly different from empirical observations via wire myography (p-value > 0.13). Specifically, 48% and 45% impairment was observed in smooth muscle contraction and endothelial-dependent relaxation, respectively, which were accurately predicted using the G&R model. Conclusions: The resulting G&R model, for the first time, allows for prediction of hypertension precursors at neonatal ages that is currently challenging to examine in preclinical models. These findings provide a validated computational tool for prediction of persistent arterial dysfunction and identification of revised severity–duration thresholds that may ultimately avoid hypertension from CoA.

Published

2023

7. Pharmacological and genetic activation of cAMP synthesis disrupts cholesterol utilization in Mycobacterium tuberculosis.

Author

Kaley M Wilburn, Christine R Montague, Bo Qin, Ashley K Woods, Melissa S Love, Case W McNamara, Peter G Schultz, Teresa L Southard, Lu Huang, H Michael Petrassi, and Brian C VanderVen

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

There is a growing appreciation for the idea that bacterial utilization of host-derived lipids, including cholesterol, supports Mycobacterium tuberculosis (Mtb) pathogenesis. This has generated interest in identifying novel antibiotics that can disrupt cholesterol utilization by Mtb in vivo. Here we identify a novel small molecule agonist (V-59) of the Mtb adenylyl cyclase Rv1625c, which stimulates 3', 5'-cyclic adenosine monophosphate (cAMP) synthesis and inhibits cholesterol utilization by Mtb. Similarly, using a complementary genetic approach that induces bacterial cAMP synthesis independent of Rv1625c, we demonstrate that inducing cAMP synthesis is sufficient to inhibit cholesterol utilization in Mtb. Although the physiological roles of individual adenylyl cyclase enzymes in Mtb are largely unknown, here we demonstrate that the transmembrane region of Rv1625c is required during cholesterol metabolism. Finally, the pharmacokinetic properties of Rv1625c agonists have been optimized, producing an orally-available Rv1625c agonist that impairs Mtb pathogenesis in infected mice. Collectively, this work demonstrates a role for Rv1625c and cAMP signaling in controlling cholesterol metabolism in Mtb and establishes that cAMP signaling can be pharmacologically manipulated for the development of new antibiotic strategies.

Published

2022

8. Mother-Adolescent Neural Concordance in Response to Distress is Related to Greater Mother-Adolescent Concordance of Perceived Adolescent Anxiety

Author

Joshua W. Zollman, Erika E. Forbes, Jill M. Cyranowski, Brittany K. Woods, and Judith K. Morgan

Subjects

Mental healing, RZ400-408

Published

2021

9. ALK Amplification and Rearrangements Are Recurrent Targetable Events in Congenital and Adult Glioblastoma

Author

Anne-Florence Blandin, Ross Giglio, Maya Srikanth Graham, Guadalupe Garcia, Seth Malinowski, Jared K. Woods, Shakti Ramkissoon, Lori Ramkissoon, Frank Dubois, Kathleen Schoolcraft, Jessica Tsai, Dayle Wang, Robert Jones, Jayne Vogelzang, Kristine Pelton, Sarah Becker, Fiona Watkinson, Claire Sinai, Elizabeth F. Cohen, Matthew A. Booker, Michael Y. Tolstorukov, Veerle Haemels, Liliana Goumnerova, Karen Wright, Mark Kieran, Katie Fehnel, David Reardon, Arnault Tauziede-Espariat, Rishi Lulla, Benjamin Carcamo, Stanley Chaleff, Alain Charest, Frederik De Smet, Azra H. Ligon, Adrian Dubuc, Melanie Pages, Pascale Varlet, Patrick Y. Wen, Brian M. Alexander, Susan Chi, Sanda Alexandrescu, Ralf Kittler, Robert Bachoo, Pratiti Bandopadhayay, Rameen Beroukhim, and Keith L. Ligon

Subjects

Cancer Research, Oncology

Abstract

Purpose: Anaplastic lymphoma kinase (ALK) aberrations have been identified in pediatric-type infant gliomas, but their occurrence across age groups, functional effects, and treatment response has not been broadly established. Experimental Design: We performed a comprehensive analysis of ALK expression and genomic aberrations in both newly generated and retrospective data from 371 glioblastomas (156 adult, 205 infant/pediatric, and 10 congenital) with in vitro and in vivo validation of aberrations. Results: ALK aberrations at the protein or genomic level were detected in 12% of gliomas (45/371) in a wide age range (0–80 years). Recurrent as well as novel ALK fusions (LRRFIP1–ALK, DCTN1–ALK, PRKD3–ALK) were present in 50% (5/10) of congenital/infant, 1.4% (3/205) of pediatric, and 1.9% (3/156) of adult GBMs. ALK fusions were present as the only candidate driver in congenital/infant GBMs and were sometimes focally amplified. In contrast, adult ALK fusions co-occurred with other oncogenic drivers. No activating ALK mutations were identified in any age group. Novel and recurrent ALK rearrangements promoted STAT3 and ERK1/2 pathways and transformation in vitro and in vivo. ALK-fused GBM cellular and mouse models were responsive to ALK inhibitors, including in patient cells derived from a congenital GBM. Relevant to the treatment of infant gliomas, we showed that ALK protein appears minimally expressed in the forebrain at perinatal stages, and no gross effects on perinatal brain development were seen in pregnant mice treated with the ALK inhibitor ceritinib. Conclusions: These findings support use of brain-penetrant ALK inhibitors in clinical trials across infant, pediatric, and adult GBMs.

Published

2023

10. <scp>Nano‐RECall</scp> provides an integrated pipeline for <scp>HIV</scp> ‐1 drug resistance testing from Oxford Nanopore sequence data

Author

Kayla Eileen, Delaney, Trevor, Ngobeni, Conan K, Woods, Carli, Gordijn, Mathilda, Claassen, Urvi, Parikh, P Richard, Harrigan, and Gert Uves, van Zyl

Subjects

Infectious Diseases, Public Health, Environmental and Occupational Health, Parasitology

Abstract

Low-capital-layout sequencing options from Oxford Nanopore Technologies (ONT) could assist in expanding HIV drug resistance testing to resource-limited settings. HIV drug resistance mutations often occur as mixtures, but current ONT pipelines provide a consensus sequence only. Moreover, there is no integrated pipeline that provides a drug resistance report from an ONT sequence file without intervention from skilled bioinformaticists. We therefore investigated Nano-RECall, which provides seamless drug resistance interpretation while requiring low-read coverage ONT sequence data from affordable Flongle or MinION flow cells and which provides mutation mixtures similar to Sanger Sequencing.We compared Sanger sequencing to ONT sequencing of the same HIV-1 subtype C polymerase chain reaction (PCR) amplicons, respectively using RECall and the novel Nano-RECall bioinformatics pipelines. Amplicons were from separate assays: (a) Applied Biosystems HIV-1 Genotyping Kit (ThermoFisher) spanning protease (PR) to reverse transcriptase (RT) (PR-RT) (n=46) and (b) homebrew integrase (IN) (n=21). The agreement between Sanger sequences and ONT sequences was assessed at nucleotide level, and at codon level for Stanford HIV drug resistance database mutations at an optimal ONT read depth of 400 reads only.The average sequence similarity between ONT and Sanger sequences was 99.3% (95% CI: 99.1-99.4%) for PR-RT and 99.6% (95% CI: 99.4-99.7%) for INT. Drug resistance mutations did not differ for 21 IN specimens; 8 mutations were detected by both ONT- and Sanger sequencing. For the 46 PR and RT specimens, 245 mutations were detected by either ONT or Sanger, of these 238 (97.1%) were detected by both.The Nano-RECall pipeline, freely available as a downloadable application on a Windows computer, provides Sanger-equivalent HIV drug resistance interpretation. This novel pipeline combined with a simple workflow and multiplexing samples on ONT flow-cells would contribute to making HIV drug resistance sequencing feasible for resource limited settings.

Published

2023

11. Cardiac Transplantation of the Fontan Patient with a Prior Norwood Procedure

Author

Ronald K. Woods and Michael E. Mitchell

Subjects

Pulmonary and Respiratory Medicine, Surgery, Cardiology and Cardiovascular Medicine

Published

2023

12. Clinical, Experimental, and Computational Validation of a New Doppler-Based Index for Coarctation Severity Assessment

Author

Arash Ghorbannia, Chalani D. Ellepola, Ronald K. Woods, El-Sayed H. Ibrahim, Mehdi Maadooliat, Hilda Martinez Ramirez, and John F. LaDisa

Subjects

Diastole, Systole, Humans, Animals, Reproducibility of Results, Radiology, Nuclear Medicine and imaging, Rabbits, Cardiology and Cardiovascular Medicine, Aortic Coarctation, Echocardiography, Doppler

Abstract

Long-term morbidity including hypertension often persists in coarctation patients despite current guidelines. Coarctation severity can be invasively assessed via peak-to-peak catheter pressure gradient (PPCG), which is estimated noninvasively via simplified Bernoulli equation and conventionally reported as peak instantaneous Doppler gradient (PIDG). However, underlying simplifications of the equation limit diagnostic accuracy. We studied the diagnostic performance of a new Doppler-based diastolic index called the continuous flow pressure gradient (CFPG) versus conventional indices in assessing coarctation severity.In a rabbit model mimicking human aortic coarctation, temporal blood pressure waveforms revealed the diastolic instantaneous pressure gradients and spectral Doppler features impacted by coarctation severity. We therefore hypothesized that CFPG provides superior correlation with coarctation gradients measured invasively. PIDG and CFPG were quantified using color flow echocardiography in humans and rabbits with discrete coarctations. Results were compared with PPCG in rabbits (n = 34) and arm-leg systolic gradients (n = 25) in humans via 1-way analysis of variance, Pearson's correlation, linear regression, and Bland-Altman analysis.A threshold of CFPG ≥ 4.6 mm Hg was identified via the Youden index as representative of PPCG ≥ 20 mm Hg (the current guideline value for coarctation intervention) in rabbits, while a CFPG ≥1.0 mm Hg represented an arm-leg systolic gradient ≥20 mm Hg in humans. Accuracy measures revealed superior correlation of CFPG (R

Published

2022

13. Clinical Variables Associated with Pre-Fontan Aortopulmonary Collateral Burden

Author

David E. Segar, Amy Y. Pan, Daniel I. McLennan, Steven J. Kindel, Stephanie S. Handler, Salil Ginde, Ronald K. Woods, Benjamin H. Goot, and Andrew D. Spearman

Subjects

Pediatrics, Perinatology and Child Health, Cardiology and Cardiovascular Medicine

Published

2022

14. Conal Septal Hypoplasia in Tetralogy of Fallot—Impact on Clinical Course, Treatment Strategies, and Outcomes After Surgical Intervention

Author

Kirsten E. Borsheim, Ronald K. Woods, Evelyn M. Kuhn, and Peter C. Frommelt

Subjects

Pediatrics, Perinatology and Child Health, Cardiology and Cardiovascular Medicine

Published

2022

15. High-LET Radiation Induces Less Injury in the bone marrow of Female Mice than in Male Mice due to Increasing IL-2 and SAA, Maintaining CD27, and Lowering the miR-34a-Regulated Pyroptosis in Female Mice

Author

Scientific Research Department (SRD), AFRRI, Juliann Kiang, Matthew G. Olson, Akeylah K. Woods, Georgetta Cannon, Scientific Research Department (SRD), AFRRI, Juliann Kiang, and Matthew G. Olson, Akeylah K. Woods, Georgetta Cannon

Abstract

High-LET radiation induces less injury in the bone marrow of female mice than in male mice due to increasing IL-2 and SAA, maintaining CD27, and lowering the miR-34a-regulated pyroptosisin female mice RESULTS MATERIALS & METHDS INTRODUCTION ExposurePreviousreportshaveindicatedthatmixed-field(neutron+gamma)irradiationcausessignificantlyincreasedmortality,decreasedsurvivaltimeandlatencyinacuteradiationsyndrome(ARS),andevendelayedhealingofinjuries(woundand/orburn)sufferedincombinationwithradiation[LedneyandElliott2010]comparedwithpurephotonirradiation.Asmechanismsofinjurybylow-LETradiationaredifferentfromthoseofhigh-LETradiation,thismayaffectdoseassessmentandcountermeasureefficacy[MacVittieetal.1991;Ledneyetal.1991and2000;Caryetal.2012].High-LETincreasesC-reactiveprotein(CRP),complementcomponent3(C3),IgMandPGE2incirculation[KiangandLedney,2013].Moreover,reductionofbloodcellcountsandincreasesincirculatingIL-18,G-CSFandGM-CSFafterhigh-LET[Ossetrovaetal.,2018a]aregreaterthanthatobservedafterlow-LET[Ossetrovaetal.,2018b;Kiangetal.,2018].In2018,SusannaRosiandhercolleagues[Krukowskietal.,2018]investigatedforthefirsttimehowcombinedgalacticcosmicradiation(GCR)exposureimpactslong-termbehavioralandcellularresponsesinmaleandfemalemousebrains.TheyfoundthatasingleexposuretosimulatedGCRinducedlong-termcognitiveandbehavioraldeficitsinmalecohorts,includingdiminishedsocialinteraction,increasedanxiety-likephenotypeandimpairedrecognitionmemory.Remarkably,femalecohortsdidnotdisplayanycognitiveorbehavioraldeficitsafterGCRexposure.Theirresultsidentifiedsex-dependentdifferencesinbehavioralandcognitivedomains.Inconcordancewiththesefindings,ourpreviousreports[Kiangetal.,2022]observedthathigh-LETradiationinducedhigherlevelsofmiR-34ainmaleileumcomparedtofemaleileum.Moreover,histologicalexaminationsofsternumsandileumsalongwithassessmentsoftheirtissuecitrullinelevels(biomarkerforentero-epithelialcellproliferation)suggestedorganinjurytobemoresevereinmalesthanfemales.Inthisreport,weinvestigatedbiomo, RITM0041736, Overexposure to ionizing radiation (IR) is life-threatening in nuclear and radiological incidents. IR depletes blood cell sand increases circulating cytokine/chemokine concentrations as well as mortality. It is reported that microglia cells of female mice are less damaged than those in male mice by IR. We have reported that the GI of female mice is more resistant to IR than the GI of male mice mediated by increases in G-CSF which down-regulate the IR-induced elevation of miR-34a and Bax, leading to decreases in both caspase 3-dependent apoptosis and caspase 1-dependent pyroptosis. It is unclear whether sex varied physiopathological responses in bone marrow (BM) and/or how it happened. We exposed B6D2F1 male and female mice to 0,1.5,3,or 6 Gy with radiation containing 67% neutrons and 33% gamma at 0.6 Gy/min. Blood, sternums and femurs were collected on days 1, 4,and 7. On day 7, IR increased adipocytes and depleted BM cells and megakaryocytes in a radiation dose-dependent manner. However, females exhibited less damage in sternum BM histology than males, which was also confirmed with Flt-3 lig and measurements. IR increased cytokines/chemokines in femurs of females and males in a dose-dependent manner, Cytokines and chemokines generally peaked on day 4 and declined on day 7 in femoral BM cells of both males and females. However, IL-2 (a promoter of T reg cells) increased on days 1 and 4 and returned to the baseline on day 7 in females but decreased on days 4 and 7 in males. IR persistently increased serum amyloid A (SAA) and maintained CD 27 (for Ig production) from day 1 to day 7 in females, where as IR decreased both on day 7 in males. MiR-34a is known to trigger gasderm in D-mediated pyroptosis viacaspase-1 activation. IR significantly increased mi R-34a, caspase-1 activation and gasderm in D activation in males but did little in females, suggesting the presence of pyroptosis in males but not females. No apoptosis was found with BM. The results indicate that BM in

Published

2023

16. A single dose of long acting GM-CSF is a promising mitigator of H-ARS in male and female mice

Author

Scientific Research Department (SRD), AFRRI, Sanchita Ghosh, Gregory Holmes-Hampton, Kaylee Valenzia, Vidya Kumar, Ashely K. Woods, Sean B. Joseph, Scientific Research Department (SRD), AFRRI, Sanchita Ghosh, and Gregory Holmes-Hampton, Kaylee Valenzia, Vidya Kumar, Ashely K. Woods, Sean B. Joseph

Abstract

CBC recovery in male and female mice Disclaimer LA-GM-CSF by Calibr The opinions and assertions expressed herein are those of the author(s) and do not necessarily reflect the official policy or position of the Uniformed Services University or the Department of Defense. None of the AFRRI/USUHS authors or their family members have a financial interest in any commercial product, service, or organization providing financial support for this research. AW and SJ are an employees at Calibr and therefore have a financial interest in the development of the product. The work was supported by NIAID AFRRI Interagency Agreement. Granulocyte-macrophage colony stimulating factor (GM-CSF) is a cytokine that stimulates bone marrow to divide and differentiate into neutrophils and macrophages. Calibr, a division of Scripps Research has developed a product mPDM608 which is a long-acting granulocyte-macrophage colony stimulating factor (LA GM-CSF) construct, which is a mouse specific construct, a fusion of the FDA approved antibody synagis with murine GM-CSF. The major drawback with the FDA approved medical countermeasure, rhuGM-CSF is its short half-life, currently daily dosing is required for recovery from exposure to myelosuppressive doses of radiation. To this end, a push to develop a long acting formulation has emerged. LA GM-CSF is designed for less frequent dosing. In this study, we demonstrate, a single dose of LA-GM-CSF protected mice from lethal dose of radiation, accelerated recovery from radiation-induced peripheral blood cytopenia, as well as attenuated protein biomarkers of hematopoietic acute radiation syndrome (H-ARS). We found that a dose of 10 mg/kg was well tolerated in non-irradiated mice. The compound was tested for its ability to increase survival efficacy in animals, 3.0 mg/kg of LA-GM-CSF was administered once subcutaneously 24 h post-exposure. Efficacy was validated in female cohorts. There was significantly accelerated recovery from radiation-induced p, RITM0041791, Granulocyte-macrophage colony stimulating factor (GM-CSF) is a cytokine that stimulates bone marrow to divide and differentiate into neutrophils and macrophages. Calibr, a division of Scripps Research has developed a product mPDM608 which is a long-acting granulocyte-macrophage colony stimulating factor (LA GM-CSF) construct, which is a mouse specific construct, a fusion of the FDA approved antibody synagis with murine GM-CSF. The major drawback with the FDA approved medical countermeasure, rhuGM-CSF is its short half-life, currently daily dosing is required for recovery from exposure to myelosuppressive doses of radiation. To this end, a push to develop a long acting formulation has emerged. LA GM-CSF is designed for less frequent dosing. In this study, we demonstrate, a single dose of LA-GM-CSF protected mice from lethal dose of radiation, accelerated recovery from radiation-induced peripheral blood cytopenia, as well as attenuated protein biomarkers of hematopoietic acute radiation syndrome (H-ARS). We found that a dose of 10 mg/kg was well tolerated in non-irradiated mice. The compound was tested for its ability to increase survival efficacy in animals, 3.0 mg/kg of LA-GM-CSF was administered once subcutaneously 24 h post-exposure. Efficacy was validated in female cohorts. There was significantly accelerated recovery from radiation-induced peripheral blood cytopenia in males treated with LA-GM-CSF up to day 15 post-TBI, no difference was observed in the CBC counts in females during this period. The drug also increased bone marrow cellularity and megakaryocytes and accelerated multi-lineage hematopoietic recovery. In addition, LA-GM-CSF inhibited radiation-induced hematopoietic biomarkers and inflammatory cytokines. Significant survival benefit with LA-GM-CSF along with hematopoietic recovery suggests that the drug could be developed as a novel radiation countermeasure for personnel who might exposed to lethal dose of irradiation aftermath of a radiation event.

Published

2023

17. Aortic Remodeling Kinetics in Response to Coarctation-Induced Mechanical Perturbations

Author

LaDisa, Arash Ghorbannia, Mehdi Maadooliat, Ronald K. Woods, Said H. Audi, Brandon J. Tefft, Claudio Chiastra, El Sayed H. Ibrahim, and John F.

Subjects

pathological remodeling, arterial adaptation, homeostasis, hypertension, smooth muscle cell proliferation, coarctation of the aorta

Abstract

Background: Coarctation of the aorta (CoA; constriction of the proximal descending thoracic aorta) is among the most common congenital cardiovascular defects. Coarctation-induced mechanical perturbations trigger a cycle of mechano-transduction events leading to irreversible precursors of hypertension including arterial thickening, stiffening, and vasoactive dysfunction in proximal conduit arteries. This study sought to identify kinetics of the stress-mediated compensatory response leading to these alterations using a preclinical rabbit model of CoA. Methods: A prior growth and remodeling (G&R) framework was reformulated and fit to empirical measurements from CoA rabbits classified into one control and nine CoA groups of various severities and durations (n = 63, 5–11/group). Empirical measurements included Doppler ultrasound imaging, uniaxial extension testing, catheter-based blood pressure, and wire myography, yielding the time evolution of arterial thickening, stiffening, and vasoactive dysfunction required to fit G&R constitutive parameters. Results: Excellent agreement was observed between model predictions and observed patterns of arterial thickening, stiffening, and dysfunction among all CoA groups. For example, predicted vascular impairment was not significantly different from empirical observations via wire myography (p-value > 0.13). Specifically, 48% and 45% impairment was observed in smooth muscle contraction and endothelial-dependent relaxation, respectively, which were accurately predicted using the G&R model. Conclusions: The resulting G&R model, for the first time, allows for prediction of hypertension precursors at neonatal ages that is currently challenging to examine in preclinical models. These findings provide a validated computational tool for prediction of persistent arterial dysfunction and identification of revised severity–duration thresholds that may ultimately avoid hypertension from CoA.

Published

2023

18. Commentary: Double Inlet Ventricle – Septate, Fenestrate, and Be Prepared to Reoperate

Author

Tracy R. Geoffrion and Ronald K. Woods

Subjects

Pulmonary and Respiratory Medicine, Surgery, Cardiology and Cardiovascular Medicine

Published

2023

19. SMA blade twist system: from the requirements to the demonstration in relevant environment

Author

Salvatore Ameduri, Monica Ciminello, Antonio Concilio, Ignazio Dimino, Bernardino Galasso, Mariano Guida, Johannes Riemenschneider, and Benjamin K. Woods

Published

2023

20. Supplementary Figure 3 from ALK Amplification and Rearrangements Are Recurrent Targetable Events in Congenital and Adult Glioblastoma

Author

Keith L. Ligon, Rameen Beroukhim, Pratiti Bandopadhayay, Robert Bachoo, Ralf Kittler, Sanda Alexandrescu, Susan Chi, Brian M. Alexander, Patrick Y. Wen, Pascale Varlet, Melanie Pages, Adrian Dubuc, Azra H. Ligon, Frederik De Smet, Alain Charest, Stanley Chaleff, Benjamin Carcamo, Rishi Lulla, Arnault Tauziede-Espariat, David Reardon, Katie Fehnel, Mark Kieran, Karen Wright, Liliana Goumnerova, Veerle Haemels, Michael Y. Tolstorukov, Matthew A. Booker, Elizabeth F. Cohen, Claire Sinai, Fiona Watkinson, Sarah Becker, Kristine Pelton, Jayne Vogelzang, Robert Jones, Dayle Wang, Jessica Tsai, Kathleen Schoolcraft, Frank Dubois, Lori Ramkissoon, Shakti Ramkissoon, Jared K. Woods, Seth Malinowski, Guadalupe Garcia, Maya Srikanth Graham, Ross Giglio, and Anne-Florence Blandin

Abstract

Supplementary Figure 3: PPP1CB-ALK fusion is oncogenic and sensitive to targeted therapy. A. Immunoblot analysis of ALK downstream signaling proteins in cortical mNSC (CTX#6) and brainstem mNSC (BS#3) expressing PPP1CB-ALK. Cells were treated for 4 hours with ceritinib and lorlatinib at the indicated concentrations.B. Left panel: Soft agar colony-forming assay using stable mNSC PPP1CB-ALK demonstrated colony formation with dose-dependent inhibition by ceritinib. mNSC KRAS did not respond to ceritinib validating the drug specificity. Right panel: Quantification of colony formation under targeted drug inhibition using CellProfiler. Values represent colony counts relative to the untreated group ± s.d. The mean of three independent replicates is shown. Significance between treatments determined by the Mann-Whitney test. *P < 0.05, **P < 0.01.C. Cell viability of ceritinib-treated PPP1CB-ALK NIH-3T3 relative to eGFP-positive cells by CellTiterGlo.D. Relative viability of the ALK wild-type GBM line (BT164) and BT1857 lorlatinib-treated cells versus DMSO control.E. Relative viability of BT164 and BT1857 ceritinib-treated cells versus DMSO control.F. Relative viability of BT164 and BT1857 cells treated with an EGFR tyrosine kinase inhibitor neratinib.G. Pharmacodynamic analysis of NIH 3T3-PPP1CB-ALK s.c. tumors treated with vehicle or ceritinib at 30mg/kg for 5 days. Representative H&E stain, ALK, pSTAT3, pAKT S473 and Ki-67 IHC.H. Quantification of Ki-67-positive cells in vehicle and ceritinib-treated tumors using CellProfiler software. Error bars show standard error of the mean. *P < 0.05.I. Quantification of pSTAT3-positive cells in vehicle and ceritinib-treated tumors using CellProfiler software. Error bars show standard error of the mean. *P < 0.05.J. Tumor growth following subcutaneous implantation of PPP1CB-ALK and eGFP-expressing fibroblasts.K. Kaplan-Meier survival curves of SCID mice injected subcutaneously with mNSC CTX-PPP1CB-ALK (red, n = 5) or mNSC CTX-eGFP (black, n = 4) and treated with ceritinib at 30mg/kg/d for 15 days. Mice were euthanized at endpoint (tumor volume of 2000mm3). The grey area represents the treatment period.L. Vehicle or ceritinib-treated mouse weights at start and end of treatment.

Published

2023

21. Supplementary Figure 5 from ALK Amplification and Rearrangements Are Recurrent Targetable Events in Congenital and Adult Glioblastoma

Author

Keith L. Ligon, Rameen Beroukhim, Pratiti Bandopadhayay, Robert Bachoo, Ralf Kittler, Sanda Alexandrescu, Susan Chi, Brian M. Alexander, Patrick Y. Wen, Pascale Varlet, Melanie Pages, Adrian Dubuc, Azra H. Ligon, Frederik De Smet, Alain Charest, Stanley Chaleff, Benjamin Carcamo, Rishi Lulla, Arnault Tauziede-Espariat, David Reardon, Katie Fehnel, Mark Kieran, Karen Wright, Liliana Goumnerova, Veerle Haemels, Michael Y. Tolstorukov, Matthew A. Booker, Elizabeth F. Cohen, Claire Sinai, Fiona Watkinson, Sarah Becker, Kristine Pelton, Jayne Vogelzang, Robert Jones, Dayle Wang, Jessica Tsai, Kathleen Schoolcraft, Frank Dubois, Lori Ramkissoon, Shakti Ramkissoon, Jared K. Woods, Seth Malinowski, Guadalupe Garcia, Maya Srikanth Graham, Ross Giglio, and Anne-Florence Blandin

Abstract

Supplementary Figure 5: Single-cell RNA Sequencing and IHC examination of ALK in human neural development and immature neural cells. A. 2D representation of human brain cell subtypes (48 samples) during cortex development using a single cell RNA-seq atlas (cortex-dev.cells.ucsc.edu) shows that ALK transcript appears to be enriched in a certain cell type. Color-coded by ALK gene expression (beige to red) and age in weeks (rainbow).B. ALK-stained sagittal section of normal human cerebellum at 15 postconceptional weeks (pcw).C. ALK-stained sagittal section of human fetal neural stem cell pellets at 13 postconceptional weeks (pcw).D. ALK-stained sagittal section of human fetal neural stem cell pellets at 15 postconceptional weeks (pcw).

Published

2023

22. Data from ALK Amplification and Rearrangements Are Recurrent Targetable Events in Congenital and Adult Glioblastoma

Author

Keith L. Ligon, Rameen Beroukhim, Pratiti Bandopadhayay, Robert Bachoo, Ralf Kittler, Sanda Alexandrescu, Susan Chi, Brian M. Alexander, Patrick Y. Wen, Pascale Varlet, Melanie Pages, Adrian Dubuc, Azra H. Ligon, Frederik De Smet, Alain Charest, Stanley Chaleff, Benjamin Carcamo, Rishi Lulla, Arnault Tauziede-Espariat, David Reardon, Katie Fehnel, Mark Kieran, Karen Wright, Liliana Goumnerova, Veerle Haemels, Michael Y. Tolstorukov, Matthew A. Booker, Elizabeth F. Cohen, Claire Sinai, Fiona Watkinson, Sarah Becker, Kristine Pelton, Jayne Vogelzang, Robert Jones, Dayle Wang, Jessica Tsai, Kathleen Schoolcraft, Frank Dubois, Lori Ramkissoon, Shakti Ramkissoon, Jared K. Woods, Seth Malinowski, Guadalupe Garcia, Maya Srikanth Graham, Ross Giglio, and Anne-Florence Blandin

Abstract

Purpose:Anaplastic lymphoma kinase (ALK) aberrations have been identified in pediatric-type infant gliomas, but their occurrence across age groups, functional effects, and treatment response has not been broadly established.Experimental Design:We performed a comprehensive analysis of ALK expression and genomic aberrations in both newly generated and retrospective data from 371 glioblastomas (156 adult, 205 infant/pediatric, and 10 congenital) with in vitro and in vivo validation of aberrations.Results:ALK aberrations at the protein or genomic level were detected in 12% of gliomas (45/371) in a wide age range (0–80 years). Recurrent as well as novel ALK fusions (LRRFIP1–ALK, DCTN1–ALK, PRKD3–ALK) were present in 50% (5/10) of congenital/infant, 1.4% (3/205) of pediatric, and 1.9% (3/156) of adult GBMs. ALK fusions were present as the only candidate driver in congenital/infant GBMs and were sometimes focally amplified. In contrast, adult ALK fusions co-occurred with other oncogenic drivers. No activating ALK mutations were identified in any age group. Novel and recurrent ALK rearrangements promoted STAT3 and ERK1/2 pathways and transformation in vitro and in vivo. ALK-fused GBM cellular and mouse models were responsive to ALK inhibitors, including in patient cells derived from a congenital GBM. Relevant to the treatment of infant gliomas, we showed that ALK protein appears minimally expressed in the forebrain at perinatal stages, and no gross effects on perinatal brain development were seen in pregnant mice treated with the ALK inhibitor ceritinib.Conclusions:These findings support use of brain-penetrant ALK inhibitors in clinical trials across infant, pediatric, and adult GBMs.

Published

2023

23. Supplementary Figure 6 from ALK Amplification and Rearrangements Are Recurrent Targetable Events in Congenital and Adult Glioblastoma

Author

Keith L. Ligon, Rameen Beroukhim, Pratiti Bandopadhayay, Robert Bachoo, Ralf Kittler, Sanda Alexandrescu, Susan Chi, Brian M. Alexander, Patrick Y. Wen, Pascale Varlet, Melanie Pages, Adrian Dubuc, Azra H. Ligon, Frederik De Smet, Alain Charest, Stanley Chaleff, Benjamin Carcamo, Rishi Lulla, Arnault Tauziede-Espariat, David Reardon, Katie Fehnel, Mark Kieran, Karen Wright, Liliana Goumnerova, Veerle Haemels, Michael Y. Tolstorukov, Matthew A. Booker, Elizabeth F. Cohen, Claire Sinai, Fiona Watkinson, Sarah Becker, Kristine Pelton, Jayne Vogelzang, Robert Jones, Dayle Wang, Jessica Tsai, Kathleen Schoolcraft, Frank Dubois, Lori Ramkissoon, Shakti Ramkissoon, Jared K. Woods, Seth Malinowski, Guadalupe Garcia, Maya Srikanth Graham, Ross Giglio, and Anne-Florence Blandin

Abstract

Supplementary Figure 6: Single cell RNA sequencing comparison of ALK expression and other infant/pediatric glioma kinase drivers in developing human and mouse brain. A. 2D representation of human brain cell subtypes (48 samples) during cortex development using a single cell RNA-seq atlas (http://cells.ucsc.edu/?ds=cortex-dev) shows that ALK positive cells make up less than 1% of all cells in the dataset and aren't localized within a specific cluster.B. Cluster-level summary of the human scRNA dataset shows that ALK expression (TPM) is decreased compared to EGFR, NTRK2, and NTRK3, and ALK positive cells make up a much lower percentage of each cluster compared to those 3 genes.C. 2D representation of developmental mouse forebrain (E12.5 – P6) in a single cell RNA-seq atlas (http://cc-shiny-01.functionalgenomics.ca/braindex/clusters) shows similar results as seen in the human scRNA Nowakowski dataset.D. Cluster-level summary of the mouse scRNA dataset corroborates results seen in the Nowkowski scRNA dataset; that Alk expression (log-normalized) is decreased, and less prevalent than EGFR, NTRK2, and NTRK3.E. 2D representation of RNA sequencing data for NTRK1-3 genes in the Nowakowski developing human cortex dataset. Compared to ALK expression, the NTRK genes have increased expression levels, increased prevalence in the dataset, and show increased localization to specific cluster.F. Similar to (E), the 2D representation of Ntrk genes in the developing mouse scRNA dataset shows increased expression and prevalence compared to Alk.

Published

2023

24. Supplementary Figure 2 from ALK Amplification and Rearrangements Are Recurrent Targetable Events in Congenital and Adult Glioblastoma

Author

Keith L. Ligon, Rameen Beroukhim, Pratiti Bandopadhayay, Robert Bachoo, Ralf Kittler, Sanda Alexandrescu, Susan Chi, Brian M. Alexander, Patrick Y. Wen, Pascale Varlet, Melanie Pages, Adrian Dubuc, Azra H. Ligon, Frederik De Smet, Alain Charest, Stanley Chaleff, Benjamin Carcamo, Rishi Lulla, Arnault Tauziede-Espariat, David Reardon, Katie Fehnel, Mark Kieran, Karen Wright, Liliana Goumnerova, Veerle Haemels, Michael Y. Tolstorukov, Matthew A. Booker, Elizabeth F. Cohen, Claire Sinai, Fiona Watkinson, Sarah Becker, Kristine Pelton, Jayne Vogelzang, Robert Jones, Dayle Wang, Jessica Tsai, Kathleen Schoolcraft, Frank Dubois, Lori Ramkissoon, Shakti Ramkissoon, Jared K. Woods, Seth Malinowski, Guadalupe Garcia, Maya Srikanth Graham, Ross Giglio, and Anne-Florence Blandin

Abstract

Supplementary Figure 2: T1 post-contrast axial and sagittal images of ALK-fused and non ALK-altered GBMs and ALK staining in ALK-fused congenital GBMs. A. Example images from patients with ALK aberrations (76, 89, 116, 197)B. In contrast to those without ALK aberrations (right columns). Contrast is gadolinium for those where applicable and show enhancement within both the tumor categories.C. Representative H&E and ALK IHCs of congenital GBM harboring an ALK fusion.

Published

2023

25. Supplementary Figure 4 from ALK Amplification and Rearrangements Are Recurrent Targetable Events in Congenital and Adult Glioblastoma

Author

Keith L. Ligon, Rameen Beroukhim, Pratiti Bandopadhayay, Robert Bachoo, Ralf Kittler, Sanda Alexandrescu, Susan Chi, Brian M. Alexander, Patrick Y. Wen, Pascale Varlet, Melanie Pages, Adrian Dubuc, Azra H. Ligon, Frederik De Smet, Alain Charest, Stanley Chaleff, Benjamin Carcamo, Rishi Lulla, Arnault Tauziede-Espariat, David Reardon, Katie Fehnel, Mark Kieran, Karen Wright, Liliana Goumnerova, Veerle Haemels, Michael Y. Tolstorukov, Matthew A. Booker, Elizabeth F. Cohen, Claire Sinai, Fiona Watkinson, Sarah Becker, Kristine Pelton, Jayne Vogelzang, Robert Jones, Dayle Wang, Jessica Tsai, Kathleen Schoolcraft, Frank Dubois, Lori Ramkissoon, Shakti Ramkissoon, Jared K. Woods, Seth Malinowski, Guadalupe Garcia, Maya Srikanth Graham, Ross Giglio, and Anne-Florence Blandin

Abstract

Supplementary Figure 4: Characterization of the lung cancer recurrent DCTN1-ALK fusion identified in cGBM (case ALK.232). A. Integrative Genomic Viewer (IGV) screenshot of the DCTN1-ALK variant.B. Predicted sequence of DCTN1-ALK fusion (DCTN1 exon 1-26, ALK exon 20-29 conserved).C. PDX DCTN1-ALK sub-renal capsule engraftment confimed by IHC.C. Relative viability of the ALK wild-type GBM line (BT164) and BT1857 ceritinib-treated cells versus DMSO control.D. Relative viability of BT164 and BT1857 lorlatinib-treated cells versus DMSO control.E. Relative viability of BT164 and BT1857 cells treated with an EGFR tyrosine kinase inhibitor neratinib.F. PDX DCTN1-ALK sub-renal capsule engraftment confirmed by IHC.

Published

2023

26. Supplementary Figure 1 from ALK Amplification and Rearrangements Are Recurrent Targetable Events in Congenital and Adult Glioblastoma

Author

Keith L. Ligon, Rameen Beroukhim, Pratiti Bandopadhayay, Robert Bachoo, Ralf Kittler, Sanda Alexandrescu, Susan Chi, Brian M. Alexander, Patrick Y. Wen, Pascale Varlet, Melanie Pages, Adrian Dubuc, Azra H. Ligon, Frederik De Smet, Alain Charest, Stanley Chaleff, Benjamin Carcamo, Rishi Lulla, Arnault Tauziede-Espariat, David Reardon, Katie Fehnel, Mark Kieran, Karen Wright, Liliana Goumnerova, Veerle Haemels, Michael Y. Tolstorukov, Matthew A. Booker, Elizabeth F. Cohen, Claire Sinai, Fiona Watkinson, Sarah Becker, Kristine Pelton, Jayne Vogelzang, Robert Jones, Dayle Wang, Jessica Tsai, Kathleen Schoolcraft, Frank Dubois, Lori Ramkissoon, Shakti Ramkissoon, Jared K. Woods, Seth Malinowski, Guadalupe Garcia, Maya Srikanth Graham, Ross Giglio, and Anne-Florence Blandin

Abstract

Supplementary Figure 1: Characterization of the novel LRRFIP1-ALK fusion (case ALK.223) A. Visualization of the read coverage at the fusion sites in ALK and LRRFIP1 genes using Integrative Genomic Viewer.B. Pile-up plot generated by SvABA using whole-genome sequencing data shows the breakpoint coordinates.C. Copy number ratio profile by WGS showing no somatic copy number alterations anywhere in the genome. The x-axis represents the chromosomes.D. Copy number ratio profile on chromosome 2 showing no copy number change of ALK and LRRFIP1 genes.E. Two RT-PCR products of 186bp (variant 1) and 189bp (variant 3) were detected by agarose gel electrophoresis with total RNA from tumor specimen ALK.223.F. Primer sequences of ALK-LRRFIP1 (variants 1 and 2) and LRRFIP1-ALK (variant 3) and the predicted DNA product size.G. Western Blot analysis of ALK signaling pathway in subcutaneous tumors treated with vehicle or lorlatinib. Normal brain was used as control.H. Representative 40x images and CellProfiler quantification of Cleaved Caspase 3- and Ki-67- stained subcutaneous tumors.

Published

2023

27. Supplementary Tables 1-8 from ALK Amplification and Rearrangements Are Recurrent Targetable Events in Congenital and Adult Glioblastoma

Author

Keith L. Ligon, Rameen Beroukhim, Pratiti Bandopadhayay, Robert Bachoo, Ralf Kittler, Sanda Alexandrescu, Susan Chi, Brian M. Alexander, Patrick Y. Wen, Pascale Varlet, Melanie Pages, Adrian Dubuc, Azra H. Ligon, Frederik De Smet, Alain Charest, Stanley Chaleff, Benjamin Carcamo, Rishi Lulla, Arnault Tauziede-Espariat, David Reardon, Katie Fehnel, Mark Kieran, Karen Wright, Liliana Goumnerova, Veerle Haemels, Michael Y. Tolstorukov, Matthew A. Booker, Elizabeth F. Cohen, Claire Sinai, Fiona Watkinson, Sarah Becker, Kristine Pelton, Jayne Vogelzang, Robert Jones, Dayle Wang, Jessica Tsai, Kathleen Schoolcraft, Frank Dubois, Lori Ramkissoon, Shakti Ramkissoon, Jared K. Woods, Seth Malinowski, Guadalupe Garcia, Maya Srikanth Graham, Ross Giglio, and Anne-Florence Blandin

Abstract

Additional information tables 1 to 8.

Published

2023

28. Roadmap for Ross procedure: Staged strategy

Author

Michael E. Mitchell, Viktor Hraska, and Ronald K. Woods

Subjects

Heart Valve Prosthesis Implantation, Pulmonary and Respiratory Medicine, medicine.medical_specialty, business.industry, medicine.medical_treatment, Ross procedure, Aortic Valve Insufficiency, Congenital aortic stenosis, Aortic valvuloplasty, Surgery, medicine, Humans, Cardiology and Cardiovascular Medicine, business

Published

2022

29. Matthew C. Canfield: Translating food sovereignty: Cultivating justice in an age of transnational governance

Author

Tiffany K. Woods

Subjects

Agronomy and Crop Science

Published

2023

30. Caution with explant of prestented percutaneous pulmonary valves with infective endocarditis

Author

Ronald K. Woods, Robert D.B. Jaquiss, and Eliot May

Subjects

Pulmonary and Respiratory Medicine, Surgery

Published

2023

31. WrapToR Truss Stiffeners: Lightweight Reinforcement for Composite Skin Panels

Author

Chris F. Grace, Mark Schenk, and Benjamin K. Woods

Published

2023

32. The STEP Environment for Distributed Problem-Based Learning on the World Wide Web

Author

Constance A. Steinkuehler, Sharon J. Derry, David K. Woods, and Cindy E. Hmelo-Silver

Published

2023

33. Integrated response analysis of pediatric low-grade gliomas during and after targeted therapy treatment

Author

Jessica W Tsai, Jungwhan John Choi, Hakim Ouaalam, Efrain Aguilar Murillo, Kee Kiat Yeo, Jayne Vogelzang, Cecilia Sousa, Jared K Woods, Keith L Ligon, Simon K Warfield, Pratiti Bandopadhayay, and Tabitha M Cooney

Subjects

Oncology, Surgery, Neurology (clinical)

Abstract

BackgroundPediatric low-grade gliomas (pLGGs) are the most common central nervous system tumor in children, characterized by RAS/MAPK pathway driver alterations. Genomic advances have facilitated the use of molecular targeted therapies, however, their long-term impact on tumor behavior remains critically unanswered.MethodsWe performed an IRB-approved, retrospective chart and imaging review of pLGGs treated with off-label targeted therapy at Dana-Farber/Boston Children’s from 2010 to 2020. Response analysis was performed for BRAFV600E and BRAF fusion/duplication-driven pLGG subsets.ResultsFifty-five patients were identified (dabrafenib n = 15, everolimus n = 26, trametinib n = 11, and vemurafenib n = 3). Median duration of targeted therapy was 9.48 months (0.12–58.44). The 1-year, 3-year, and 5-year EFS from targeted therapy initiation were 62.1%, 38.2%, and 31.8%, respectively. Mean volumetric change for BRAFV600E mutated pLGG on BRAF inhibitors was −54.11%; median time to best volumetric response was 8.28 months with 9 of 12 (75%) objective RAPNO responses. Median time to largest volume post-treatment was 2.86 months (+13.49%); mean volume by the last follow-up was −14.02%. Mean volumetric change for BRAF fusion/duplication pLGG on trametinib was +7.34%; median time to best volumetric response was 6.71 months with 3 of 7 (43%) objective RAPNO responses. Median time to largest volume post-treatment was 2.38 months (+71.86%); mean volume by the last follow-up was +39.41%.ConclusionsOur integrated analysis suggests variability in response by pLGG molecular subgroup and targeted therapy, as well as the transience of some tumor growth following targeted therapy cessation.

Published

2022

34. Correction to: Clinical trial-ready patient cohorts for multiple system atrophy: coupling biospecimen and iPSC banking to longitudinal deep-phenotyping

Author

Alain Ndayisaba, Ariana T. Pitaro, Andrew S. Willett, Kristie A. Jones, Claudio Melo de Gusmao, Abby L. Olsen, Jisoo Kim, Eero Rissanen, Jared K. Woods, Sharan R. Srinivasan, Anna Nagy, Amanda Nagy, Merlyne Mesidor, Steven Cicero, Viharkumar Patel, Derek H. Oakley, Idil Tuncali, Katherine Taglieri-Noble, Emily C. Clark, Jordan Paulson, Richard C. Krolewski, Gary P. Ho, Albert Y. Hung, Anne-Marie Wills, Michael T. Hayes, Jason P. Macmore, Luigi Warren, Pamela G. Bower, Carol B. Langer, Lawrence R. Kellerman, Christopher W. Humphreys, Bonnie I. Glanz, Elodi J. Dielubanza, Matthew P. Frosch, Roy L. Freeman, Christopher H. Gibbons, Nadia Stefanova, Tanuja Chitnis, Howard L. Weiner, Clemens R. Scherzer, Sonja W. Scholz, Dana Vuzman, Laura M. Cox, Gregor Wenning, Jeremy D. Schmahmann, Anoopum S. Gupta, Peter Novak, Geoffrey S. Young, Mel B. Feany, Tarun Singhal, and Vikram Khurana

Subjects

Neurology, Neurology (clinical)

Published

2022

35. Using Seafloor Geodesy to Detect Vertical Deformation at the Hikurangi Subduction Zone: Insights From Self‐Calibrating Pressure Sensors and Ocean General Circulation Models

Author

K. Woods, S. C. Webb, L. M. Wallace, Y. Ito, C. Collins, N. Palmer, R. Hino, M. K. Savage, D. M. Saffer, E. E. Davis, and D. H. N. Barker

Subjects

Geophysics, Space and Planetary Science, Geochemistry and Petrology, Earth and Planetary Sciences (miscellaneous)

Published

2022

36. Nuclear Cell-Free DNA Predicts Adverse Events After Pediatric Cardiothoracic Surgery

Author

Justinn M. Tanem, John P. Scott, George M. Hoffman, Robert A. Niebler, Aoy Tomita-Mitchell, Karl D. Stamm, Huan-Ling Liang, Paula E. North, Rebecca A. Bertrandt, Ronald K. Woods, Viktor Hraska, and Michael E. Mitchell

Subjects

Pulmonary and Respiratory Medicine, Surgery, Cardiology and Cardiovascular Medicine

Published

2022

37. Is native aortic valvuloplasty at time of Norwood operation in infants with hypoplastic left heart syndrome and aortic stenosis safe?

Author

David E. Segar, Peter C. Frommelt, and Ronald K. Woods

Subjects

Pediatrics, Perinatology and Child Health, General Medicine, Cardiology and Cardiovascular Medicine

Abstract

In hypoplastic left heart syndrome, the size and function of the left ventricle vary and are dependent on the patency of the aortic valve. A patent native aortic valve, permitting left ventricular ejection, can augment cardiac output. We performed a retrospective chart review of patients with hypoplastic left heart syndrome and a stenotic aortic valve who underwent native aortic valvuloplasty at the time of Norwood and found that none of the eight patients identified had clinically significant aortic insufficiency. This case series suggests that surgical aortic valvuloplasty at Norwood is associated with aortic valve patency/augmented systemic cardiac output without the development of clinically significant aortic regurgitation at intermediate follow-up in a limited cohort.

Published

2022

38. Caring for Our Children While Training to Care for All Children

Author

Judy Schaechter, Suzanne K. Woods, and Laurel K. Leslie

Subjects

Pediatrics, Perinatology and Child Health

Published

2022

39. Clinical Trial-Ready Patient Cohorts for Multiple System Atrophy: Coupling Biospecimen and iPSC Banking to Longitudinal Deep-Phenotyping

Author

Alain Ndayisaba, Ariana T. Pitaro, Andrew S. Willett, Kristie A. Jones, Claudio Melo de Gusmao, Abby L. Olsen, Jisoo Kim, Eero Rissanen, Jared K. Woods, Sharan R. Srinivasan, Anna Nagy, Amanda Nagy, Merlyne Mesidor, Steven Cicero, Viharkumar Patel, Derek H. Oakley, Idil Tuncali, Katherine Taglieri-Noble, Emily C. Clark, Jordan Paulson, Richard C. Krolewski, Gary P. Ho, Albert Y. Hung, Anne-Marie Wills, Michael T. Hayes, Jason P. Macmore, Luigi Warren, Pamela G. Bower, Carol B. Langer, Lawrence R. Kellerman, Christopher W. Humphreys, Bonnie I. Glanz, Elodi J. Dielubanza, Matthew P. Frosch, Roy L. Freeman, Christopher H. Gibbons, Nadia Stefanova, Tanuja Chitnis, Howard L. Weiner, Clemens R. Scherzer, Sonja W. Scholz, Dana Vuzman, Laura M. Cox, Gregor Wenning, Jeremy D. Schmahmann, Anoopum S. Gupta, Peter Novak, Geoffrey S. Young, Mel B. Feany, Tarun Singhal, and Vikram Khurana

Subjects

Neurology, Neurology (clinical)

Abstract

Multiple system atrophy (MSA) is a fatal neurodegenerative disease of unknown etiology characterized by widespread aggregation of the protein alpha-synuclein in neurons and glia. Its orphan status, biological relationship to Parkinson’s disease (PD), and rapid progression have sparked interest in drug development. One significant obstacle to therapeutics is disease heterogeneity. Here, we share our process of developing a clinical trial-ready cohort of MSA patients (69 patients in 2 years) within an outpatient clinical setting, and recruiting 20 of these patients into a longitudinal “n-of-few” clinical trial paradigm. First, we deeply phenotype our patients with clinical scales (UMSARS, BARS, MoCA, NMSS, and UPSIT) and tests designed to establish early differential diagnosis (including volumetric MRI, FDG-PET, MIBG scan, polysomnography, genetic testing, autonomic function tests, skin biopsy) or disease activity (PBR06-TSPO). Second, we longitudinally collect biospecimens (blood, CSF, stool) and clinical, biometric, and imaging data to generate antecedent disease-progression scores. Third, in our Mass General Brigham SCiN study (stemcellsinneurodegeneration), we generate induced pluripotent stem cell (iPSC) models from our patients, matched to biospecimens, including postmortem brain. We present 38 iPSC lines derived from MSA patients and relevant disease controls (spinocerebellar ataxia and PD, including alpha-synuclein triplication cases), 22 matched to whole-genome sequenced postmortem brain. iPSC models may facilitate matching patients to appropriate therapies, particularly in heterogeneous diseases for which patient-specific biology may elude animal models. We anticipate that deeply phenotyped and genotyped patient cohorts matched to cellular models will increase the likelihood of success in clinical trials for MSA.

Published

2022

40. The prognostic significance of troponin level in patients with malignancy (NIHR Health Informatics Collaborative TROP-MALIGNANCY study)

Author

A Kaura, N A Samuel, A J Roddick, B Glampson, A Mulla, J Davies, K Woods, R S Patel, A M Shah, D Perera, K M Channon, A S V Shah, and J Mayet

Subjects

Cardiology and Cardiovascular Medicine

Abstract

Background Cardiac troponin is commonly raised in patients with malignancy and may aid clinicians in risk prediction. The prognostic significance of raised troponin in these patients with known malignancies remains unclear. Purpose We sought to investigate the relation between troponin and mortality in a large, well characterised cohort of patients undergoing cardiac troponin testing with a concomitant malignancy. Methods A retrospective cohort study was carried out using the National Institute for Health Research Health Informatics Collaborative Cardiovascular dataset of all consecutive patients who had a troponin measured at five hospitals between 2010 and 2017. Patients with a primary inpatient diagnosis of malignancy who had at least one cTn measurement during their hospital stay were identified. Patients were classified into solid tumour or haematological malignancy subgroups. Survival analyses were performed using multivariate Cox regression analyses and Kaplan-Meier plots. Cox regression analyses were adjusted for age, gender, C-reactive protein, haemoglobin, platelet count, white cell count, acute coronary syndrome, diabetes mellitus, heart failure, chronic kidney disease, chronic obstructive pulmonary disease, atrial fibrillation and angiography. The peak cTn level (highest level measured), standardised to the upper limit of normal (ULN), was used for all analyses. Results 5571 patients undergoing troponin testing had a primary diagnosis of malignancy and comprised of twenty-one different cancer types. 4649 patients were diagnosed with solid tumours and 922 patients were diagnosed with haematological malignancies. Patients with raised troponin had a higher burden of cardiovascular comorbidities compared to patients with a troponin level below the ULN. The median follow-up in the cohort was 14 months (interquartile range 2–39 months). At 1-year follow-up, 2495 (42%) of patients died. Figure 1 shows Kaplan-Meier plots for patients stratified by troponin level. Patients with a troponin level ≥1xULN had a higher risk of death compared to patients with a troponin level Conclusion A raised troponin was associated with an increased mortality risk in patients with malignancy regardless of cancer subtype. Stratification of mortality risk using troponin may help guide clinicians in making management decisions for patients with malignancy. Funding Acknowledgement Type of funding sources: Public grant(s) – National budget only. Main funding source(s): NIHR Imperial Biomedical Research Centre, as part of the NIHR Health Informatics Collaborative, and 2) British Heart Foundation

Published

2022

41. The association between age, troponin level, and mortality in patients hospitalised with acute pulmonary embolism (NIHR Health Informatics Collaborative TROP-PE study)

Author

A Kaura, S Goswami, A Mulla, B Glampson, J Davies, K Woods, A M Shah, R Kharbanda, R S Patel, D Perera, K M Channon, J Quint, and J Mayet

Subjects

Cardiology and Cardiovascular Medicine

Abstract

Background A positive cardiac troponin (cTn) is an independent predictor of short-term mortality in individuals presenting with acute pulmonary embolism (PE). However, there is limited evidence regarding the impact age has on the association between cTn levels and mortality in patients with PE. Purpose The aim of our study was to investigate the relationship between cTn level, age, and all-cause mortality, in hospitalised patients diagnosed with an acute PE. Methods A retrospective cohort study using the National Institute for Health Research Health Informatics Collaborative Cardiovascular dataset of all consecutive patients who had a troponin measured at five hospitals between 2010 and 2017. Patients admitted to hospital with a primary diagnosis of PE with at least one cTn measurement were included. We modelled the relation between peak troponin level and all-cause mortality using multivariable adjusted restricted cubic spline Cox regression analyses. Effect estimates were adjusted for age, gender, high-sensitivity troponin assay, C-reactive protein, haemoglobin, platelet count, white cell count, creatinine, sodium, potassium, diabetes, hypertension, hypercholesterolaemia, acute coronary syndrome, atrial fibrillation, heart failure, acute kidney injury, chronic kidney disease, obstructive lung disease, inflammatory disorders, pneumonia and malignancy. The peak cTn level (highest level measured), standardised to the upper limit of normal (ULN), was used for all analyses. Results 1,477 patients with at least one cTn measurement and a diagnosis of acute PE were included. During a median follow-up of 34.8 months, there were 290 (19.6%) deaths. Elevated cTn (>1xULN) was associated with a hazard ratio (HR) of 3.29 (95% confidence interval [CI] 1.95–5.53) for 30-day mortality and 2.12 (95% CI 1.63–2.75) for 3-year mortality. Higher cTn levels were progressively associated with a higher mortality risk, reaching a maximum HR of 2.59 (95% CI 1.64–4.09) at 141xULN (Figure 1). Younger patients ( Conclusion Elevated cTn, at all ages, is associated with an increased mortality risk in patients presenting with PE, with increasing cTn levels conferring a progressively worse long-term prognosis. Elevated cTn, no matter how small, needs to be taken seriously, particularly in young patients with an acute PE. Funding Acknowledgement Type of funding sources: Public grant(s) – National budget only. Main funding source(s): 1) NIHR Imperial Biomedical Research Centre, as part of the NIHR Health Informatics Collaborative, and 2) British Heart Foundation

Published

2022

42. The association between troponin level and mortality in patients admitted to hospital with acute stroke (NIHR Health Informatics Collaborative TROP-STROKE study)

Author

A Kaura, A J Roddick, N A Samuel, A Mulla, B Glampson, J Davies, K Woods, R Kharbanda, R S Patel, A M Shah, D Perera, K M Channon, and J Mayet

Subjects

Cardiology and Cardiovascular Medicine

Abstract

Introduction Acute stroke accounts for significant morbidity and mortality globally. The role of troponin for risk stratification in stroke is unclear. Purpose The aims of this study were to assess the relationship between peak troponin and mortality in patients with ischaemic stroke, haemorrhagic stroke, or subarachnoid haemorrhage and to compare this with the predictive value of first troponin or dynamic troponin change. Methods A retrospective cohort study was carried out using the National Institute for Health Research Health Informatics Collaborative Cardiovascular dataset of all consecutive patients who had a troponin measured at five hospitals between 2010 and 2017. Patients with at least one troponin measurement and a primary diagnosis of ischaemic stroke, haemorrhagic stroke or subarachnoid haemorrhage during a hospital admission were included. The main exposure variables were first and peak troponin, and dynamic troponin change, and the main outcome was all-cause mortality. Results were analysed using multivariable adjusted restricted cubic spline Cox regression. Survival analyses were adjusted for troponin assay, assay sensitivity (standard or highly sensitive), number of troponin measurements, age, sex, C-reactive protein level, white blood cell count, platelet count, haemoglobin, estimated glomerular filtration rate, angiography during admission, acute coronary syndrome during admission, and cardiovascular history (history of diabetes mellitus, myocardial infarction, heart failure, hypertension, stroke or atrial fibrillation). Receiver Operator Characteristic (ROC) curves were used to assess the predictive value of each exposure variable. Results 4,712 patients were included in the analysis (ischaemic stroke: 3,346; haemorrhagic stroke: 718; subarachnoid haemorrhage: 648). Peak troponin was above the upper limit of normal in 47.4% of ischaemic stroke patients, 52.8% of haemorrhagic stroke patients, and 57.1% of subarachnoid haemorrhage patients. Patients with elevated peak troponin were older and had more cardiovascular risk factors. A direct positive relationship was seen between peak troponin level and mortality hazard ratio in all three stroke subtypes (Figure 1). This relationship was consistent when considering dynamic troponin fold change for ischaemic or haemorrhagic stroke. For all three stroke subtypes, there was no added predictive value of peak troponin or dynamic troponin change over first troponin in predicting mortality (Figure 2). Conclusions A positive peak troponin was associated with increased mortality in patients presenting with ischaemic stroke, haemorrhagic stroke, or subarachnoid haemorrhage. Overall, serial troponin measurements may not improve mortality prediction beyond a single measurement. These findings may have implications for risk stratification of patients with acute stroke syndromes. Funding Acknowledgement Type of funding sources: Public grant(s) – National budget only. Main funding source(s): NIHR Imperial Biomedical Research Centre, as part of the NIHR Health Informatics Collaborative, and 2) British Heart Foundation

Published

2022

43. Targeted protein S-nitrosylation of ACE2 inhibits SARS-CoV-2 infection

Author

Chang-ki Oh, Tomohiro Nakamura, Nathan Beutler, Xu Zhang, Juan Piña-Crespo, Maria Talantova, Swagata Ghatak, Dorit Trudler, Lauren N. Carnevale, Scott R. McKercher, Malina A. Bakowski, Jolene K. Diedrich, Amanda J. Roberts, Ashley K. Woods, Victor Chi, Anil K. Gupta, Mia A. Rosenfeld, Fiona L. Kearns, Lorenzo Casalino, Namir Shaabani, Hejun Liu, Ian A. Wilson, Rommie E. Amaro, Dennis R. Burton, John R. Yates, Cyrus Becker, Thomas F. Rogers, Arnab K. Chatterjee, and Stuart A. Lipton

Subjects

Biochemistry & Molecular Biology, SARS-CoV-2, Prevention, viruses, COVID-19, Pneumonia, Cell Biology, Peptidyl-Dipeptidase A, Article, Vaccine Related, Medicinal and Biomolecular Chemistry, Emerging Infectious Diseases, Infectious Diseases, Good Health and Well Being, 5.1 Pharmaceuticals, Biodefense, Pneumonia & Influenza, Humans, Angiotensin-Converting Enzyme 2, Biochemistry and Cell Biology, Development of treatments and therapeutic interventions, Infection, Lung, Molecular Biology, Protein Binding

Abstract

Prevention of infection and propagation of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is a high priority in the Coronavirus Disease 2019 (COVID-19) pandemic. Here we describe S-nitrosylation of multiple proteins involved in SARS-CoV-2 infection, including angiotensin-converting enzyme 2 (ACE2), the receptor for viral entry. This reaction prevents binding of ACE2 to the SARS-CoV-2 spike protein, thereby inhibiting viral entry, infectivity and cytotoxicity. Aminoadamantane compounds also inhibit coronavirus ion channels formed by envelope (E) protein. Accordingly, we developed dual-mechanism aminoadamantane nitrate compounds that inhibit viral entry and, thus, the spread of infection by S-nitrosylating ACE2 via targeted delivery of the drug after E protein channel blockade. These non-toxic compounds are active in vitro and in vivo in the Syrian hamster COVID-19 model and, thus, provide a novel avenue to pursue therapy.

Published

2022

44. Abstract 104: Kisspeptin Signaling And Pregnancy Outcomes Are Ameliorated In The Preeclamptic-like BPH/5 Mouse After Synchronization Of Sex Steroid Hormones

Author

Viviane C Gomes, Ashley K Woods, Camille A Landry, Kassandra R Crissman, and Jennifer L Sones

Subjects

Internal Medicine

Abstract

Kisspeptins (KP), encoded by Kiss1 , are reported to play a role in early-onset preeclampsia (ePE), a life-threatening hypertensive disorder of pregnancy. KP is higher in term ePE placentae than in normal pregnancies. However, the role of KP in PE has not been confirmed. The Blood Pressure High Subline 5 (BPH/5) mouse model spontaneously develops the main features of ePE, including impaired placental expansion and maternal hypertension. We have shown that Kiss1 is higher at the BPH/5 maternal-fetal interface on embryonic days (e) 4.5 and 7.5. BPH/5 females have abnormal circulating sex steroid hormones (SSH) during early gestation (e2.5), with lower estradiol-17ß (E2) and higher progesterone (P4). Since E2 and P4 may modulate uterine Kiss1 , we aimed to investigate the effects of artificial synchronization of SSH (AS-SSH) in BPH/5 uteroplacental KP signaling and placental development. We hypothesized that AS-SSH would prevent BPH/5 uteroplacental Kiss1 upregulation and normalize KP downstream expression of tissue inhibitor of metalloproteinase (TIMP) 2 and placental defects. AS-SSH was performed after ovariectomy of pregnant BPH/5 and C57 females (n = 8/strain) at e2.5 with one dose of E2 (25 ng/mouse, subcutaneously), and daily subcutaneous injections of P4 (1ng/mouse) until embryonic implantation sites (eIS) were collected 3 days post-surgery (n = 8/group). Contrary to natural (Nat) BPH/5 pregnancies, eIS Kiss1 and TIMP2 expression was not different between AS-SSH BPH/5 and C57 (p > 0.05). Nat and AS-SSH pregnant mice were anesthetized at e12.5 to assess umbilical cord blood flow via ultrasound and uteroplacental units were harvested for placental morphometry (n = 4-6/group). Placental expansion into the maternal decidua was measured and expressed as the ratio of the placenta depth in relation to the placenta + decidua. Nat BPH/5 had lower placental expansion and umbilical blood flow than Nat C57, whereas AS-SSH BPH/5 had higher placental expansion and umbilical blood flow than Nat BPH/5 (p < 0.05). In conclusion, synchronization of the E2 and P4 profile in the BPH/5 mouse early gestation mitigated Kiss1 and TIMP2 upregulation at the maternal-fetal interface and ameliorated the placental defects previously reported in this model.

Published

2022

45. Neuronal, Affective, and Sensory Correlates of Targeted Helping Behavior in Male and Female Sprague Dawley Rats

Author

Stewart S. Cox, Brogan J. Brown, Samuel K Woods, Samantha J. Brown, Angela M. Kearns, and Carmela M. Reichel

Abstract

Empathy is an innate ability to understand the emotional states of others along with the motivation to improve it. It has evolved over time into highly complex behaviors, the basis of which can be described using the Perception Action Model (PAM), where shared affect promotes an action that eliminates the distress of both the passive “Target” and, by extension, the active “Observer.” There are myriad biological variables that may modulate empathic behavior, including sex, sensory modalities, and neural activity. In the following studies, using our lab’s model of social contact-independent targeted helping, we first tested whether sex differences exist in helping behavior. Next, we explored sex differences in sensory and affective signaling, including the impact of direct visualization of a distressed conspecific and the type of ultrasonic vocalizations (USV) made between animal pairs during the task. Finally, we examined the neural activity of multiple cortical and subcortical regions of interest across time during targeted helping between males and females. We show both sexes exhibit similar helping behavior, but sensory and affective signaling differs between sexes. Further, changes in neural activity exhibited distinct sex-specific patterns across time. Our results indicate sex differences are not a ubiquitous presence in targeted helping. Instead, it is likely sex differences may be a convergent phenomenon in which the behavior is similar, but the underlying biological mechanisms are distinct. These results lay the groundwork for future studies to explore the similarities and differences that drive empathic behavior in both males and females.

Published

2022

46. An assessment of Nano-RECall: Interpretation of Oxford Nanopore sequence data for HIV-1 drug resistance testing

Author

Kayla Eileen Delaney, Trevor Ngobeni, Conan K. Woods, Carli Gordijn, Mathilda Claassen, Urvi Parikh, P. Richard Harrigan, and Gert Uves van Zyl

Abstract

IntroductionOxford Nanopore Technologies (ONT) offer sequencing with low-capital-layout sequencing options, which could assist in expanding HIV drug resistance testing to resource limited settings. However, sequence analysis remains time time-consuming and reliant on skilled personnel. Moreover, current ONT bioinformatic pipelines provide a single consensus sequence that is not equivalent to Sanger sequencing, as drug resistance is often detected in mixed populations. We have therefore investigated an integrated bioinformatic pipeline, Nano-RECall, for seamless drug resistance of low read coverage ONT sequence data from affordable Flongle or MinION flow cells.MethodsWe compared Sanger sequencing to ONT sequencing of the same HIV-1 subtype C polymerase chain reaction (PCR) amplicons, respectively using RECall and the novel Nano-RECall bioinformatics pipelines. Amplicons were from separate assays a) Applied Biosystems HIV-1 Genotyping Kit (ThermoFisher) spanning protease (PR) to reverse transcriptase (RT) (PR-RT) (n=46) and b) homebrew integrase (IN) (n=21). We investigated optimal read-depth by assessing the coefficient of variation (CV) of nucleotide proportions for various read-depths; and between replicates of 400 reads. The agreement between Sanger sequences and ONT sequences were assessed at nucleotide level, and at codon level for Stanford HIV drug resistance database mutations.ResultsThe coefficient of variation of ONT minority variants plateaued after a read depth of 400-fold implying limited benefit of additional depth and replicates of 400 reads showed a CV of ∼6 % for a representative position. The average sequence similarity between ONT and Sanger sequences was 99.3% (95% CI: 99.1-99.4%) for PR-RT and 99.6% (95% CI: 99.4-99.7%) for INT. Drug resistance mutations did not differ for 21 IN sequences; 16 mutations were detected by both ONT- and Sanger sequencing. For the 46 PR and RT sequences, 245 mutations were detected by either ONT or Sanger, of these 238 (97.1%) were detected by both.ConclusionsThe Nano-RECall pipeline, freely available as a downloadable application on a Windows computer, provides Sanger-equivalent HIV drug resistance interpretation. This novel pipeline combined with a simple workflow and multiplexing samples on ONT flow-cells would contribute to making HIV drug resistance sequencing feasible for resource limited settings.

Published

2022

47. Abstract 1201: ALK amplification and rearrangements are recurrent targetable events in congenital and adult glioblastoma

Author

Anne-Florence Blandin, Ross Giglio, Maya Srikanth Graham, Guadalupe Garcia, Seth Malinowski, Jared K. Woods, Shakti Ramkissoon, Lori Ramkissoon, Frank Dubois, Kate Schoolcraft, Jessica W. Tsai, Dayle K. Wang, Robert Jones, Jayne Vogelzang, Kristine Pelton, Sarah Becker, Fiona Watkinson, Claire Sinai, Elizabeth Cohen, Matthew Booker, Michael Tolstorukov, Veerle Haemels, Liliana Goumnerova, Karen Wright, Mark Kieran, Katie Fehnel, David Reardon, Arnault Tauziede-Espariat, Rishi Lulla, Benjamin Carcamo, Stanley Chaleff, Alain Charest, Frederik De Smet, Azra H. Ligon, Adrian Dubuc, Melanie Pagès, Pascale Varlet, Patrick Wen, Brian Alexander, Susan Chi, Sanda Alexandrescu, Ralf Kittler, Robert Bachoo, Rameen Beroukhim, Pratiti Bandopadhayay, and Keith L. Ligon

Subjects

Cancer Research, Oncology

Abstract

Purpose: Anaplastic Lymphoma Kinase (ALK) aberrations have been identified in pediatric type infant gliomas, but their occurrence across age groups, functional effects, and treatment response have not been broadly established. Experimental Design: We performed a comprehensive analysis of ALK expression and genomic aberrations in both newly-generated and retrospective data from 371 glioblastomas (156 adult, 205 infant/pediatric and 10 congenital) with in vitro and in vivo validation of aberrations. Results: ALK aberrations at the protein or genomic level were detected in 12% of gliomas (45/371) in a wide age range (0-80 years). Recurrent as well as novel ALK fusions (LRRFIP1-ALK, DCTN1-ALK, PRKD3-ALK) were present in 50% (5/10) of congenital/infant, 1.4% (3/205) of pediatric, and 1.9% (3/156) of adult GBMs. ALK fusions were present as the only candidate driver in congenital/infant GBMs, and were sometimes focally amplified. In contrast, adult ALK fusions co-occurred with other oncogenic drivers. No activating ALK mutations were identified in any age group. Novel and recurrent ALK rearrangements promoted STAT3 and ERK1/2 pathways and transformation in vitro and in vivo. ALK-fused GBM cellular and mouse models were responsive to ALK inhibitors, including in patient cells derived from a congenital GBM. Relevant to treatment of infant gliomas, we showed that ALK protein appears minimally expressed in the forebrain at perinatal stages and no gross effects on perinatal brain development was seen in pregnant mice treated with the ALK inhibitor ceritinib. Conclusions: These findings support expanded evaluation of brain-penetrant ALK inhibitors in clinical trials across infant, pediatric, and adult GBMs. Citation Format: Anne-Florence Blandin, Ross Giglio, Maya Srikanth Graham, Guadalupe Garcia, Seth Malinowski, Jared K. Woods, Shakti Ramkissoon, Lori Ramkissoon, Frank Dubois, Kate Schoolcraft, Jessica W. Tsai, Dayle K. Wang, Robert Jones, Jayne Vogelzang, Kristine Pelton, Sarah Becker, Fiona Watkinson, Claire Sinai, Elizabeth Cohen, Matthew Booker, Michael Tolstorukov, Veerle Haemels, Liliana Goumnerova, Karen Wright, Mark Kieran, Katie Fehnel, David Reardon, Arnault Tauziede-Espariat, Rishi Lulla, Benjamin Carcamo, Stanley Chaleff, Alain Charest, Frederik De Smet, Azra H. Ligon, Adrian Dubuc, Melanie Pagès, Pascale Varlet, Patrick Wen, Brian Alexander, Susan Chi, Sanda Alexandrescu, Ralf Kittler, Robert Bachoo, Rameen Beroukhim, Pratiti Bandopadhayay, Keith L. Ligon. ALK amplification and rearrangements are recurrent targetable events in congenital and adult glioblastoma [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 1 (Regular and Invited Abstracts); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(7_Suppl):Abstract nr 1201.

Published

2023

48. Safety of Tocilizumab in Patients Treated for Covid-19 in a London Hospital

Author

C. Nimmo, A. Read, R. Priyadarshi, A. Parry, A. Boyd, and K. Woods

Published

2022

49. Determining the Relationship Between Clofazimine Gastrointestinal Levels and anti‐ Cryptosporidium Efficacy in Mice

Author

Cindy X. Zhang, Mellisa S. Love, Case W. McNamara, Victor Chi, Ashley K. Woods, Sean Joseph, and Samuel L. Arnold

Subjects

Genetics, Molecular Biology, Biochemistry, Biotechnology

Published

2022

50. Artificial Synchronization of Sex Steroid Hormones Normalizes Kisspeptin Expression and Placentation in the Preeclamptic‐Like BPH/5 Mouse

Author

Viviane C. Gomes, Ashley K. Woods, Camille A. Landry, and Jennifer L. Sones

Subjects

Genetics, Molecular Biology, Biochemistry, Biotechnology

Published

2022