Your search keyword '"S Griffith"' showing total 1,194 results

1. Behavioral Indicators of Interactions Between Humans, Virtual Agent Characters and Virtual Avatars.

Author

Tamara S. Griffith, Cali M. Fidopiastis, Patricia Bockelman-Morrow, and Joan Johnston

Published

2020

2. An investigation into the synergistic relationship between lactoferrin and azithromycin with particular reference to periodontopathic bacteria

Author

J, Husain, G S, Griffith, A, Rawlingson, G, Stafford, and Douglas, C.W.I

Published

2019

3. Natural Microbial Exposure from the Earliest Natural Time Point Enhances Immune Development by Expanding Immune Cell Progenitors and Mature Immune Cells

Author

Sarah Burger, Terran Stenger, Mark Pierson, Adhvaith Sridhar, Matthew A. Huggins, Tamara A. Kucaba, Thomas S. Griffith, Sara E. Hamilton, and Nathaniel J. Schuldt

Subjects

Immunology, Immunology and Allergy

Abstract

Microbial experience fundamentally shapes immunity, particularly during the perinatal period when the immune system is underdeveloped, and novel microbial encounters are common. Most animal models are raised in specific pathogen-free (SPF) conditions with relatively uniform microbial communities. How SPF housing conditions alter early-life immune development relative to natural microbial exposure (NME) has not been thoroughly investigated. In this article, we compare immune development in SPF-raised mice with mice born from immunologically experienced mothers in microbially diverse environments. NME induced broad immune cell expansion, including naive cells, suggesting mechanisms besides activation-induced proliferation contribute to the increase in immune cell numbers. We found NME conditions also expanded immune cell progenitor cell populations in the bone marrow, suggesting microbial experience enhances immune development at the earliest stages of immune cell differentiation. Multiple immune functions characteristically impaired in infants were also enhanced by NME, including T cell memory and Th1 polarization, B cell class switching and Ab production, proinflammatory cytokine expression, and bacterial clearance after Listeria monocytogenes challenge. Collectively, our studies reveal numerous impairments in immune development in SPF conditions relative to natural immune development.

Published

2023

4. Polymicrobial Sepsis Impairs Antigen-Specific Memory CD4 T Cell-Mediated Immunity

Author

Frances V. Sjaastad, Tamara A. Kucaba, Thamotharampillai Dileepan, Whitney Swanson, Cody Dail, Javier Cabrera-Perez, Katherine A. Murphy, Vladimir P. Badovinac, and Thomas S. Griffith

Subjects

sepsis, immune suppression, CD4 T cells, memory, IFN-gamma, Immunologic diseases. Allergy, RC581-607

Abstract

Patients who survive sepsis display prolonged immune dysfunction and heightened risk of secondary infection. CD4 T cells support a variety of cells required for protective immunity, and perturbations to the CD4 T cell compartment can decrease overall immune system fitness. Using the cecal ligation and puncture (CLP) mouse model of sepsis, we investigated the impact of sepsis on endogenous Ag-specific memory CD4 T cells generated in C57BL/6 (B6) mice infected with attenuated Listeria monocytogenes (Lm) expressing the I-Ab-restricted 2W1S epitope (Lm-2W). The number of 2W1S-specific memory CD4 T cells was significantly reduced on day 2 after sepsis induction, but recovered by day 14. In contrast to the transient numerical change, the 2W1S-specific memory CD4 T cells displayed prolonged functional impairment after sepsis, evidenced by a reduced recall response (proliferation and effector cytokine production) after restimulation with cognate Ag. To define the extent to which the observed functional impairments in the memory CD4 T cells impacts protection to secondary infection, B6 mice were infected with attenuated Salmonella enterica-2W (Se-2W) 30 days before sham or CLP surgery, and then challenged with virulent Se-2W after surgery. Pathogen burden was significantly higher in the CLP-treated mice compared to shams. Similar reductions in functional capacity and protection were noted for the endogenous OVA323-specific memory CD4 T cell population in sepsis survivors upon Lm-OVA challenge. Our data collectively show CLP-induced sepsis alters the number and function of Ag-specific memory CD4 T cells, which contributes (in part) to the characteristic long-lasting immunoparalysis seen after sepsis.

Published

2020

5. Inefficient Recovery of Repeatedly Stimulated Memory CD8 T Cells after Polymicrobial Sepsis Induction Leads to Changes in Memory CD8 T Cell Pool Composition

Author

Steven J. Moioffer, Roger R. Berton, Patrick W. McGonagill, Isaac J. Jensen, Thomas S. Griffith, and Vladimir P. Badovinac

Subjects

Mice, Inbred C57BL, Mice, Memory T Cells, Lymphopenia, Sepsis, Immunology, Humans, Animals, Cytokines, Immunology and Allergy, CD8-Positive T-Lymphocytes, Immunologic Memory

Abstract

Long-lasting sepsis-induced immunoparalysis has been principally studied in primary (1°) memory CD8 T cells; however, the impact of sepsis on memory CD8 T cells with a history of repeated cognate Ag encounters is largely unknown but important in understanding the role of sepsis in shaping the pre-existing memory CD8 T cell compartment. Higher-order memory CD8 T cells are crucial in providing immunity against common pathogens that reinfect the host or are generated by repeated vaccination. In this study, we analyzed peripheral blood from septic patients and show that memory CD8 T cells with defined Ag specificity for recurring CMV infection proliferate less than bulk populations of central memory CD8 T cells. Using TCR-transgenic T cells to generate 1° and higher-order (quaternary [4°]) memory T cells within the same host, we demonstrate that the susceptibility and loss of both memory subsets are similar after sepsis induction, and sepsis diminished Ag-dependent and -independent (bystander) functions of these memory subsets equally. Both the 1° and 4° memory T cell populations proliferated in a sepsis-induced lymphopenic environment; however, due to the intrinsic differences in baseline proliferative capacity, expression of receptors (e.g., CD127/CD122), and responsiveness to homeostatic cytokines, 1° memory T cells become overrepresented over time in sepsis survivors. Finally, IL-7/anti–IL-7 mAb complex treatment early after sepsis induction preferentially rescued the proliferation and accumulation of 1° memory T cells, whereas recovery of 4° memory T cells was less pronounced. Thus, inefficient recovery of repeatedly stimulated memory cells after polymicrobial sepsis induction leads to changes in memory T cell pool composition, a notion with important implications in devising strategies to recover the number and function of pre-existing memory CD8 T cells in sepsis survivors.

Published

2023

6. Reduced T Cell Priming in Microbially Experienced 'Dirty' Mice Results from Limited IL-27 Production by XCR1+ Dendritic Cells

Author

Frances V. Sjaastad, Matthew A. Huggins, Erin D. Lucas, Cara Skon-Hegg, Whitney Swanson, Matthew D. Martin, Oscar C. Salgado, Julie Xu, Mark Pierson, Thamotharampillai Dileepan, Tamara A. Kucaba, Sara E. Hamilton, and Thomas S. Griffith

Subjects

Mice, Interleukin-27, Immunology, Humans, Animals, Immunology and Allergy, Cell Differentiation, Dendritic Cells, CD8-Positive T-Lymphocytes, CD40 Antigens

Abstract

Successful vaccination strategies offer the potential for lifelong immunity against infectious diseases and cancer. There has been increased attention regarding the limited translation of some preclinical findings generated using specific pathogen-free (SPF) laboratory mice to humans. One potential reason for the difference between preclinical and clinical findings lies in maturation status of the immune system at the time of challenge. In this study, we used a “dirty” mouse model, where SPF laboratory mice were cohoused (CoH) with pet store mice to permit microbe transfer and immune system maturation, to investigate the priming of a naive T cell response after vaccination with a peptide subunit mixed with polyinosinic-polycytidylic acid and agonistic anti-CD40 mAb. Although this vaccination platform induced robust antitumor immunity in SPF mice, it failed to do so in microbially experienced CoH mice. Subsequent investigation revealed that despite similar numbers of Ag-specific naive CD4 and CD8 T cell precursors, the expansion, differentiation, and recall responses of these CD4 and CD8 T cell populations in CoH mice were significantly reduced compared with SPF mice after vaccination. Evaluation of the dendritic cell compartment revealed reduced IL-27p28 expression by XCR1+ dendritic cells from CoH mice after vaccination, correlating with reduced T cell expansion. Importantly, administration of recombinant IL-27:EBI3 complex to CoH mice shortly after vaccination significantly boosted Ag-specific CD8 and CD4 T cell expansion, further implicating the defect to be T cell extrinsic. Collectively, our data show the potential limitation of exclusive use of SPF mice when testing vaccine efficacy.

Published

2022

7. Opioid Use Disorder

Author

Patricia S. Griffith, Lana M. Brown, Shelly Y. Lensing, Ravi Nahata, Prasad R. Padala, Lisa Snow, Katherine Milholland, and Melinda Mullins

Subjects

Psychiatry and Mental health, Pshychiatric Mental Health

Published

2022

8. Inflammation Controls Susceptibility of Immune-Experienced Mice to Sepsis

Author

Roger R. Berton, Isaac J. Jensen, John T. Harty, Thomas S. Griffith, and Vladimir P. Badovinac

Subjects

Inflammation, Disease Models, Animal, Mice, Sepsis, Immunology, Animals, Humans, Immunology and Allergy, General Medicine, Cecum, Ligation

Abstract

Sepsis, an amplified immune response to systemic infection that leads to life-threatening organ dysfunction, affects >125,000 people/day worldwide with 20% mortality. Modest therapeutic progress for sepsis has been made, in part because of the lack of therapeutic translatability between mouse-based experimental models and humans. One potential reason for this difference stems from the extensive use of immunologically naive specific pathogen-free mice in preclinical research. To address this issue, we used sequential infections with well-defined BSL-2 pathogens to establish a novel immune-experienced mouse model (specific pathogen experienced [SPexp]) to determine the extent to which immunological experience and/or inflammation influences the host capacity to respond to subsequent infections, including sepsis. Consistent with their immunological experience, SPexp inbred or outbred mice had significant changes in the composition and activation status of multiple leukocyte populations known to influence the severity of cecal ligation and puncture–induced sepsis. Importantly, by varying the timing of sepsis induction, we found the level of basal inflammation controls sepsis-induced morbidity and mortality in SPexp mice. In addition, although a beneficial role of NK cells in sepsis was recently demonstrated in specific pathogen-free mice, NK cell depletion before cecal ligation and puncture induction in SPexp mice lead to diminished mortality, suggesting NK cells may have beneficial or detrimental roles in the response to septic insult dependent on host immune status. Thus, data highlight the importance of utilizing immune-experienced models for preclinical studies to interrogate the cellular/molecular mechanism(s) that could be therapeutically exploited during severe and dysregulated infection-induced inflammatory responses, such as sepsis.

Published

2022

9. Hepatic IRE1 Protects Against Septic Cardiac Failure

Author

Mark Li, Roger R. Berton, Qingwen Qian, J. Alan Maschek, Biyi Chen, Elizabeth Barroso, Adam J. Rauckhorst, Thomas S. Griffith, Eric B. Taylor, Vladimir P. Badovinac, Gökhan S. Hotamisligil, Long-Sheng Song, and Ling Yang

Abstract

SUMMARY Metabolic reprogramming in response to infection plays a critical role for septic survival. During a septic episode, the heart heavily relies on hepatic lipid particles to prevent heart damage and failure. Inositol- Requiring Enzyme 1 (IRE1) is the most conserved unfolded protein response (UPR) regulator that governs homeostasis of the endoplasmic reticulum (ER), the major site for lipid synthesis and processing. Here we show that hepatocyte IRE1 is indispensable for protecting against septic mortality in two different rodent models of experimental sepsis. The protective effect of hepatic IRE1 was not attributed to the inflammatory response since hepatic IRE1 deletion did not alter hepatic or systemic cytokine response. However, loss of IRE1 in the liver significantly augmented septic cardiac dysfunction in part due to a skewed immune-metabolic balance. Lipidomic and metabolomic analyses further revealed that loss of IRE1 in the liver compromised adaptive intrahepatic and circulating lipid reprogramming, including VLDL, in response to septic challenge. Furthermore, we identified that the protective effects against septic mortality are mediated by a non-canonical IRE1-dependent mechanism. Together, our study provides the first insight into how a disruption of hepatic ER-mediated lipid metabolic regulation promotes sepsis-associated cardiac immuno-metabolic imbalance.

Published

2023

10. Using antenatal care as a platform for malaria surveillance data collection: study protocol

Author

Julie R. Gutman, Julia Nanteza Mwesigwa, Kyra Arnett, Chabu Kangale, Sijenunu Aaron, Dele Babarinde, Julie Buekens, Baltazar Candrinho, Siaka Debe, Peder Digre, Mary Drake, Adama Gansané, Christelle Gogue, Kevin S. Griffith, Joseph Hicks, Réné Kinda, Hannah Koenker, Ruth Lemwayi, Anna Munsey, Emmanuel Obi, Aurore Ogouyèmi-Hounto, Okefu Oyale Okoko, Faustin Onikpo, Ali Onoja, Travis Porter, Binete Savaio, Kenzie Tynuv, Perpetua Uhomoibhi, Joseph Wagman, Katherine Wolf, Rose Zulliger, Patrick Walker, John M. Miller, and Molly Robertson

Subjects

Infectious Diseases, Parasitology

Abstract

Background While many malaria-endemic countries have health management information systems that can measure and report malaria trends in a timely manner, these routine systems have limitations. Periodic community cross-sectional household surveys are used to estimate malaria prevalence and intervention coverage but lack geographic granularity and are resource intensive. Incorporating malaria testing for all women at their first antenatal care (ANC) visit (i.e., ANC1) could provide a more timely and granular source of data for monitoring trends in malaria burden and intervention coverage. This article describes a protocol designed to assess if ANC-based surveillance could be a pragmatic tool to monitor malaria. Methods This is an observational, cross-sectional study conducted in Benin, Burkina Faso, Mozambique, Nigeria, Tanzania, and Zambia. Pregnant women attending ANC1 in selected health facilities will be tested for malaria infection by rapid diagnostic test and administered a brief questionnaire to capture key indicators of malaria control intervention coverage and care-seeking behaviour. In each location, contemporaneous cross-sectional household surveys will be leveraged to assess correlations between estimates obtained using each method, and the use of ANC data as a tool to track trends in malaria burden and intervention coverage will be validated. Results This study will assess malaria prevalence at ANC1 aggregated at health facility and district levels, and by gravidity relative to current pregnancy (i.e., gravida 1, gravida 2, and gravida 3 +). ANC1 malaria prevalence will be presented as monthly trends. Additionally, correlation between ANC1 and household survey–derived estimates of malaria prevalence, bed net ownership and use, and care-seeking will be assessed. Conclusion ANC1-based surveillance has the potential to provide a cost-effective, localized measure of malaria prevalence that is representative of the general population and useful for tracking monthly changes in parasite prevalence, as well as providing population-representative estimates of intervention coverage and care-seeking behavior. This study will evaluate the representativeness of these measures and collect information on operational feasibility, usefulness for programmatic decision-making, and potential for scale-up of malaria ANC1 surveillance.

Published

2023

11. Polymicrobial sepsis influences NK-cell-mediated immunity by diminishing NK-cell-intrinsic receptor-mediated effector responses to viral ligands or infections.

Author

Isaac J Jensen, Christina S Winborn, Micaela G Fosdick, Peng Shao, Mikaela M Tremblay, Qiang Shan, Sandeep Kumar Tripathy, Christopher M Snyder, Hai-Hui Xue, Thomas S Griffith, Jon C Houtman, and Vladimir P Badovinac

Subjects

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

Abstract

The sepsis-induced cytokine storm leads to severe lymphopenia and reduced effector capacity of remaining/surviving cells. This results in a prolonged state of immunoparalysis, that contributes to enhanced morbidity/mortality of sepsis survivors upon secondary infection. The impact of sepsis on several lymphoid subsets has been characterized, yet its impact on NK-cells remains underappreciated-despite their critical role in controlling infection(s). Here, we observed numerical loss of NK-cells in multiple tissues after cecal-ligation-and-puncture (CLP)-induced sepsis. To elucidate the sepsis-induced lesions in surviving NK-cells, transcriptional profiles were evaluated and indicated changes consistent with impaired effector functionality. A corresponding deficit in NK-cell capacity to produce effector molecules following secondary infection and/or cytokine stimulation (IL-12,IL-18) further suggested a sepsis-induced NK-cell intrinsic impairment. To specifically probe NK-cell receptor-mediated function, the activating Ly49H receptor, that recognizes the murine cytomegalovirus (MCMV) m157 protein, served as a model receptor. Although relative expression of Ly49H receptor did not change, the number of Ly49H+ NK-cells in CLP hosts was reduced leading to impaired in vivo cytotoxicity and the capacity of NK-cells (on per-cell basis) to perform Ly49H-mediated degranulation, killing, and effector molecule production in vitro was also severely reduced. Mechanistically, Ly49H adaptor protein (DAP12) activation and clustering, assessed by TIRF microscopy, was compromised. This was further associated with diminished AKT phosphorylation and capacity to flux calcium following receptor stimulation. Importantly, DAP12 overexpression in NK-cells restored Ly49H/D receptors-mediated effector functions in CLP hosts. Finally, as a consequence of sepsis-dependent numerical and functional lesions in Ly49H+ NK-cells, host capacity to control MCMV infection was significantly impaired. Importantly, IL-2 complex (IL-2c) therapy after CLP improved numbers but not a function of NK-cells leading to enhanced immunity to MCMV challenge. Thus, the sepsis-induced immunoparalysis state includes numerical and NK-cell-intrinsic functional impairments, an instructive notion for future studies aimed in restoring NK-cell immunity in sepsis survivors.

Published

2018

12. Improving retention of community-recruited participants in HIV prevention research through Saturday household visits; findings from the HPTN 071 (PopART) study in South Africa

Author

N. F. Bell-Mandla, R. Sloot, G. Maarman, S. Griffith, A. Moore, S. Floyd, R. Hayes, S. Fidler, H. Ayles, P. Bock, and on behalf of the HPTN 071 (PopART) study team

Subjects

Male, medicine.medical_specialty, Medicine (General), Epidemiology, media_common.quotation_subject, Human immunodeficiency virus (HIV), HIV Infections, Health Informatics, Participant retention, medicine.disease_cause, Cohort Studies, South Africa, R5-920, Community-based research, Acquired immunodeficiency syndrome (AIDS), Hygiene, Household visits, medicine, Humans, media_common, Acquired Immunodeficiency Syndrome, Family Characteristics, Univariate analysis, Retention methods, business.industry, Longitudinal studies, Population cohort, Household visit timing, medicine.disease, Confidence interval, Home visits, Longitudinal cohort, Retention, Tropical medicine, Retention strategies, Female, business, Research Article, Demography

Abstract

Background Identifying successful strategies to improve participant retention in longitudinal studies remains a challenge. In this study we evaluated whether non-traditional fieldworker shifts (after hours during the week and weekends) enhanced participant retention when compared to retention during traditional weekday shifts in the HPTN 071 (PopART) population cohort (PC). Methods HPTN 071 (PopART) PC participants were recruited and followed up in their homes on an annual basis by research fieldworkers over a 3-4 year period. The average number of successful follow-up visits, where a PC participant was found and retained in the study, was calculated for each of 3 visit schedules (early weekday shift, late weekday shift, and Saturday shift), and standardized to account for variation in fieldwork shift duration. We used one-way univariate analysis of variance (ANOVA) to describe differences in mean-successful visits and 95% confidence intervals between the shift types. Results Data on 16 651 successful visits were included. Successful visit rates were higher when conducting Saturday visits (14.0; 95% CI: 11.3-16.6) compared to both regular (4.5; 95% CI: 3.7-5.3) and late weekday shifts (5.3; 95% CI: 4.7-5.8) overall and in all subgroup analyses (Pp Conclusion The number of people living with HIV continues to increase annually. High quality evidence from longitudinal studies remains critical for evaluating HIV prevention and treatment strategies. This study showed a significant benefit on participant retention through introduction of Saturday shifts for home visits and these data can make an important contribution to the emerging body of evidence for improving retention in longitudinal research. Trial registration PopART was approved by the Stellenbosch University Health Research Ethics Committees (N12/11/074), London School of Hygiene and Tropical Medicine (6326) ethics committee and the Division of AIDS (DAIDS) (Protocol ID 11865). PopART was registered with ClinicalTrials.gov (registration number NCT01900977).

Published

2021

13. Evaluating remote facilitation intensity for multi-national translation of nurse-initiated stroke protocols (QASC Australasia): a protocol for a cluster randomised controlled trial

Author

O. Fasugba, S. Dale, E. McInnes, D. A. Cadilhac, M. Noetel, K. Coughlan, B. McElduff, J. Kim, T. Langley, N. W. Cheung, K. Hill, V. Pollnow, K. Page, E. Sanjuan Menendez, E. Neal, S. Griffith, L. J. Christie, J. Slark, A. Ranta, C. Levi, J. M. Grimshaw, S. Middleton, Institut Català de la Salut, [Fasugba O, Dale S, McInnes E, Coughlan K] Nursing Research Institute, St Vincent’s Health Network Sydney & St Vincent’s Hospital Melbourne & Australian Catholic University, Darlinghurst, Australia. School of Nursing, Midwifery and Paramedicine, Australian Catholic University, Sydney, Australia. [Cadilhac DA] Stroke and Ageing Research, Department of Medicine, School of Clinical Sciences at Monash Health, Monash University, Melbourne, Victoria, Australia. [Noetel M] School of Psychology, University of Queensland, Brisbane, Australia. [Sanjuan Menendez E] Vall d’Hebron Hospital Universitari, Barcelona, Spain, and Vall d'Hebron Barcelona Hospital Campus

Subjects

Therapeutics::Patient Care Bundles [ANALYTICAL, DIAGNOSTIC AND THERAPEUTIC TECHNIQUES, AND EQUIPMENT], Health Policy, localizaciones geográficas::Oceanía::Australasia [DENOMINACIONES GEOGRÁFICAS], Public Health, Environmental and Occupational Health, Health Informatics, General Medicine, Cardiovascular Diseases::Vascular Diseases::Cerebrovascular Disorders::Stroke [DISEASES], Malalties cerebrovasculars - Tractament - Austràlia, Assistència sanitària - Control de qualitat, Geographic Locations::Oceania::Australasia [GEOGRAPHICALS], Health Care Quality, Access, and Evaluation::Quality of Health Care::Health Care Evaluation Mechanisms::Epidemiologic Study Characteristics::Clinical Protocols [HEALTH CARE], calidad, acceso y evaluación de la atención sanitaria::calidad de la atención sanitaria::mecanismos de evaluación de la atención sanitaria::características de los estudios epidemiológicos::protocolos clínicos [ATENCIÓN DE SALUD], Infermeres, Protocols clínics, enfermedades cardiovasculares::enfermedades vasculares::trastornos cerebrovasculares::accidente cerebrovascular [ENFERMEDADES], personas::grupos profesionales::personal sanitario::enfermeros [DENOMINACIONES DE GRUPOS], terapéutica::paquetes de medidas asistenciales [TÉCNICAS Y EQUIPOS ANALÍTICOS, DIAGNÓSTICOS Y TERAPÉUTICOS], Persons::Occupational Groups::Health Personnel::Nurses [NAMED GROUPS]

Abstract

Background Facilitated implementation of nurse-initiated protocols to manage fever, hyperglycaemia (sugar) and swallowing difficulties (FeSS Protocols) in 19 Australian stroke units resulted in reduced death and dependency for stroke patients. However, a significant gap remains in translating this evidence-based care bundle protocol into standard practice in Australia and New Zealand. Facilitation is a key component for increasing implementation. However, its contribution to evidence translation initiatives requires further investigation. We aim to evaluate two levels of intensity of external remote facilitation as part of a multifaceted intervention to improve FeSS Protocol uptake and quality of care for patients with stroke in Australian and New Zealand acute care hospitals. Methods A three-arm cluster randomised controlled trial with a process evaluation and economic evaluation. Australian and New Zealand hospitals with a stroke unit or service will be recruited and randomised in blocks of five to one of the three study arms—high- or low-intensity external remote facilitation or a no facilitation control group—in a 2:2:1 ratio. The multicomponent implementation strategy will incorporate implementation science frameworks (Theoretical Domains Framework, Capability, Opportunity, Motivation – Behaviour Model and the Consolidated Framework for Implementation Research) and include an online education package, audit and feedback reports, local clinical champions, barrier and enabler assessments, action plans, reminders and external remote facilitation. The primary outcome is implementation effectiveness using a composite measure comprising six monitoring and treatment elements of the FeSS Protocols. Secondary outcome measures are as follows: composite outcome of adherence to each of the combined monitoring and treatment elements for (i) fever (n=5); (ii) hyperglycaemia (n=6); and (iii) swallowing protocols (n=7); adherence to the individual elements that make up each of these protocols; comparison for composite outcomes between (i) metropolitan and rural/remote hospitals; and (ii) stroke units and stroke services. A process evaluation will examine contextual factors influencing intervention uptake. An economic evaluation will describe cost differences relative to each intervention and study outcomes. Discussion We will generate new evidence on the most effective facilitation intensity to support implementation of nurse-initiated stroke protocols nationwide, reducing geographical barriers for those in rural and remote areas. Trial registration ACTRN12622000028707. Registered 14 January, 2022.

Published

2023

14. Sepsis-induced changes in differentiation, maintenance, and function of memory CD8 T cell subsets

Author

Mohammad Heidarian, Thomas S. Griffith, and Vladimir P. Badovinac

Subjects

Immunology, Immunology and Allergy

Abstract

Formation of long-lasting memory lymphocytes is one of the foundational characteristics of adaptive immunity and the basis of many vaccination strategies. Following the rapid expansion and contraction of effector CD8 T cells, the surviving antigen (Ag)-specific cells give rise to the memory CD8 T cells that persist for a long time and are phenotypically and functionally distinct from their naïve counterparts. Significant heterogeneity exists within the memory CD8 T cell pool, as different subsets display distinct tissue localization preferences, cytotoxic ability, and proliferative capacity, but all memory CD8 T cells are equipped to mount an enhanced immune response upon Ag re-encounter. Memory CD8 T cells demonstrate numerical stability under homeostatic conditions, but sepsis causes a significant decline in the number of memory CD8 T cells and diminishes their Ag-dependent and -independent functions. Sepsis also rewires the transcriptional profile of memory CD8 T cells, which profoundly impacts memory CD8 T cell differentiation and, ultimately, the protective capacity of memory CD8 T cells upon subsequent stimulation. This review delves into different aspects of memory CD8 T cell subsets as well as the immediate and long-term impact of sepsis on memory CD8 T cell biology.

Published

2023

15. Epilepsy Is Heterogeneous in Early-Life Tuberous Sclerosis Complex

Author

Molly S. Griffith, Darcy A. Krueger, Hope Northrup, E. Martina Bebin, S Katie Z Ihnen, Joyce Y. Wu, Paul S. Horn, Jamie K. Capal, and Mustafa Sahin

Subjects

Male, Pediatrics, medicine.medical_specialty, Population, Article, Tuberous sclerosis, Epilepsy, Developmental Neuroscience, Seizure diary, Tuberous Sclerosis, medicine, Humans, Longitudinal Studies, Age of Onset, education, education.field_of_study, business.industry, Seizure types, Infant, Newborn, Infant, medicine.disease, Early life, Epileptic spasms, Neurology, Child, Preschool, Pediatrics, Perinatology and Child Health, Female, Epilepsies, Partial, Neurology (clinical), Age of onset, business, Spasms, Infantile

Abstract

Background Epilepsy in tuberous sclerosis complex (TSC) typically presents with early onset, multiple seizure types, and intractability. However, variability is observed among individuals. Here, detailed individual data on seizure characteristics collected prospectively during early life were used to define epilepsy profiles in this population. Methods Children aged zero to 36 months were followed longitudinally. Caregivers kept daily seizure diaries, including onset and daily counts for each seizure type. Patients with >70% seizure diary completion and >365 diary days were included. Developmental outcomes at 36 months were compared between subgroups. Results Epilepsy was seen in 124 of 156 (79%) participants. Seizure onset occurred from zero to 29.5 months; 93% had onset before age 12 months. Focal seizures and epileptic spasms were most common. Number of seizures (for median 897 days) ranged from 1 to 9128. Hierarchical clustering based on six metrics of seizure burden (age of onset, total seizures, ratio of seizure days to nonseizure days, seizures per seizure day, and worst seven- and 30-day stretches) revealed two distinct groups with broadly favorable and unfavorable epilepsy profiles. Subpopulations within each group showed clinically meaningful differences in seizure burden. Groups with higher seizure burden had worse developmental outcomes at 36 months. Conclusions Although epilepsy is highly prevalent in TSC, not all young children with TSC have the same epilepsy profile. At least two phenotypic subpopulations are discernible based on seizure burden. Early and aggressive treatments for epilepsy in TSC may be best leveraged by targeting specific subgroups based on phenotype severity.

Published

2021

16. Hominids Foraging in a Complex Landscape: Could Homo ergaster and Australopithecus boisei Meet Their Calories Requirements?

Author

Marco A. Janssen, Jeanne M. Sept, and Cameron S. Griffith

Published

2006

17. Polymicrobial sepsis impairs bystander recruitment of effector cells to infected skin despite optimal sensing and alarming function of skin resident memory CD8 T cells.

Author

Derek B Danahy, Scott M Anthony, Isaac J Jensen, Stacey M Hartwig, Qiang Shan, Hai-Hui Xue, John T Harty, Thomas S Griffith, and Vladimir P Badovinac

Subjects

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

Abstract

Sepsis is a systemic infection that enhances host vulnerability to secondary infections normally controlled by T cells. Using CLP sepsis model, we observed that sepsis induces apoptosis of circulating memory CD8 T-cells (TCIRCM) and diminishes their effector functions, leading to impaired CD8 T-cell mediated protection to systemic pathogen re-infection. In the context of localized re-infections, tissue resident memory CD8 T-cells (TRM) provide robust protection in a variety of infectious models. TRM rapidly 'sense' infection in non-lymphoid tissues and 'alarm' the host by enhancing immune cell recruitment to the site of the infection to accelerate pathogen clearance. Here, we show that compared to pathogen-specific TCIRCM, sepsis does not invoke significant numerical decline of Vaccinia virus induced skin-TRM keeping their effector functions (e.g., Ag-dependent IFN-γ production) intact. IFN-γ-mediated recruitment of immune cells to the site of localized infection was, however, reduced in CLP hosts despite TRM maintaining their 'sensing and alarming' functions. The capacity of memory CD8 T-cells in the septic environment to respond to inflammatory cues and arrive to the site of secondary infection/antigen exposure remained normal suggesting T-cell-extrinsic factors contributed to the observed lesion. Mechanistically, we showed that IFN-γ produced rapidly during sepsis-induced cytokine storm leads to reduced IFN-γR1 expression on vascular endothelium. As a consequence, decreased expression of adhesion molecules and/or chemokines (VCAM1 and CXCL9) on skin endothelial cells in response to TRM-derived IFN-γ was observed, leading to sub-optimal bystander-recruitment of effector cells and increased susceptibility to pathogen re-encounter. Importantly, as visualized by intravital 2-photon microscopy, exogenous administration of CXCL9/10 was sufficient to correct sepsis-induced impairments in recruitment of effector cells at the localized site of TRM antigen recognition. Thus, sepsis has the capacity to alter skin TRM anamnestic responses without directly impacting TRM number and/or function, an observation that helps to further define the immunoparalysis phase in sepsis survivors.

Published

2017

18. Generation of a Beta-Cell Transplant Animal Model of Diabetes Using CRISPR Technology

Author

Yunus Emre, Eksi, Atil, Bisgin, Ahter D, Sanlioglu, Reha Onur, Azizoglu, Mustafa Kemal, Balci, Thomas S, Griffith, and Salih, Sanlioglu

Abstract

Since insulin deficiency results from pancreatic beta-cell destruction, all type 1 and most type 2 diabetes patients eventually require life-long insulin injections. Insulin gene synthesis could also be impaired due to insulin gene mutations as observed in diabetic patients with MODY 10. At this point, insulin gene therapy could be very effective to recompense insulin deficiency under these circumstances. For this reason, an HIV-based lentiviral vector carrying the insulin gene under the control of insulin promoter (LentiINS) was generated, and its therapeutic efficacy was tested in a beta-cell transplant model lacking insulin produced by CRISPR/Cas9-mediated genetically engineered pancreatic beta cells. To generate an insulin knockout beta-cell transplant animal model of diabetes, a dual gene knockout plasmid system involving CRISPR/Cas9 was transfected into a mouse pancreatic beta cell line (Min6). Fluorescence microscopy and antibiotic selection were utilized to select the insulin gene knockout clones. Transplantation of the genetically engineered pancreatic beta cells under the kidney capsule of STZ-induced diabetic rats revealed LentiINS- but not LentiLacZ-infected Ins2KO cells transiently reduced hyperglycemia similar to that of MIN6 in diabetic animals. These results suggest LentiINS has the potential to functionally restore insulin production in an insulin knockout beta-cell transplant animal model of diabetes.

Published

2022

19. Immunotherapy for Bladder Cancer: Latest Advances and Ongoing Clinical Trials

Author

Daniela F. Ward Grados, Hamed Ahmadi, Thomas S Griffith, and Christopher A. Warlick

Subjects

Urinary Bladder Neoplasms, Immunology, Humans, General Medicine, Immunotherapy

Abstract

For nearly 50 years, immunotherapy has been used in patients with bladder cancer in the form of

Published

2022

20. Chlorine as a primary radical: evaluation of methods to understand its role in initiation of oxidative cycles

Author

C. J. Young, R. A. Washenfelder, P. M. Edwards, D. D. Parrish, J. B. Gilman, W. C. Kuster, L. H. Mielke, H. D. Osthoff, C. Tsai, O. Pikelnaya, J. Stutz, P. R. Veres, J. M. Roberts, S. Griffith, S. Dusanter, P. S. Stevens, J. Flynn, N. Grossberg, B. Lefer, J. S. Holloway, J. Peischl, T. B. Ryerson, E. L. Atlas, D. R. Blake, and S. S. Brown

Subjects

Physics, QC1-999, Chemistry, QD1-999

Abstract

The role of chlorine atoms (Cl) in atmospheric oxidation has been traditionally thought to be limited to the marine boundary layer, where they are produced through heterogeneous reactions involving sea salt. However, recent observation of photolytic Cl precursors (ClNO2 and Cl2) formed from anthropogenic pollution has expanded the potential importance of Cl to include coastal and continental urban areas. Measurements of ClNO2 in Los Angeles during CalNex (California Nexus – Research at the Nexus of Air Quality and Climate Change) showed it to be an important primary (first generation) radical source. Evolution of ratios of volatile organic compounds (VOCs) has been proposed as a method to quantify Cl oxidation, but we find no evidence from this approach for a significant role of Cl oxidation in Los Angeles. We use a box model with the Master Chemical Mechanism (MCM v3.2) chemistry scheme, constrained by observations in Los Angeles, to examine the Cl sensitivity of commonly used VOC ratios as a function of NOx and secondary radical production. Model results indicate VOC tracer ratios could not detect the influence of Cl unless the ratio of [OH] to [Cl] was less than 200 for at least a day. However, the model results also show that secondary (second generation) OH production resulting from Cl oxidation of VOCs is strongly influenced by NOx, and that this effect obscures the importance of Cl as a primary oxidant. Calculated concentrations of Cl showed a maximum in mid-morning due to a photolytic source from ClNO2 and loss primarily to reactions with VOCs. The [OH] to [Cl] ratio was below 200 for approximately 3 h in the morning, but Cl oxidation was not evident from the measured ratios of VOCs. Instead, model simulations show that secondary OH production causes VOC ratio evolution to follow that expected for OH oxidation, despite the significant input of primary Cl from ClNO2 photolysis in the morning. Even though OH is by far the dominant oxidant in Los Angeles, Cl atoms do play an important role in photochemistry there, constituting 9% of the primary radical source. Furthermore, Cl–VOC reactivity differs from that of OH, being more than an order of magnitude larger and dominated by VOCs, such as alkanes, that are less reactive toward OH. Primary Cl is also slightly more effective as a radical source than primary OH due to its greater propensity to initiate radical propagation chains via VOC reactions relative to chain termination via reaction with nitrogen oxides.

Published

2014

21. Sepsis, Cytokine Storms, and Immunopathology: The Divide between Neonates and Adults

Author

Kathryn A. Knoop, Kara G. Greenfield, Vladimir P. Badovinac, and Thomas S. Griffith

Subjects

Adult, medicine.medical_specialty, medicine.medical_treatment, Immunology, Severity of Illness Index, Article, Disease course, Sepsis, Immune system, Immunopathology, medicine, Immunology and Allergy, Animals, Humans, Intensive care medicine, Neonatal sepsis, business.industry, Age Factors, Infant, Newborn, General Medicine, medicine.disease, Disease Models, Animal, Cytokine, Bacteremia, Host-Pathogen Interactions, Disease Progression, business, Cytokine Release Syndrome

Abstract

Sepsis can result from a variety of pathogens, originating from a range of sources. A vast range of presenting symptoms is included in the catch-all term of “bacteremia,” making diagnosis and prognosis particularly troublesome. One underexplored factor contributing to disparate outcomes is the age of the patient. Neonatal sepsis in very-low-birth-weight infants can result in vastly different immunological outcomes unique from sepsis in adults. It is also becoming increasingly clear, both from preclinical experimental models and clinical observations, that the age and history of previous microbial exposures can significantly influence the course of infection from sepsis and cytokine storms to immunopathology. In this study, we will explore key differences between neonatal and adult sepsis, experimental models used to study sepsis, and how responses to the surrounding microbial universe shape development of the immune system and impact, positively or negatively, the course of disease.

Published

2021

22. Prolonged Reactive Oxygen Species Production following Septic Insult

Author

Vladimir P. Badovinac, Garry R. Buettner, Isaac J. Jensen, Roger R. Berton, Patrick W. McGonagill, Thomas S. Griffith, Elvia E. Silva, and Brett A. Wagner

Subjects

Adult, Male, Antioxidant, Adolescent, medicine.medical_treatment, Lymphocyte, Immunology, Ascorbic Acid, Severity of Illness Index, Antioxidants, Article, Immature Monocyte, Sepsis, Mice, Young Adult, Immune system, Disease severity, Animals, Humans, Immunology and Allergy, Medicine, Aged, Aged, 80 and over, chemistry.chemical_classification, Reactive oxygen species, Vitamin C, business.industry, General Medicine, Middle Aged, medicine.disease, Healthy Volunteers, Disease Models, Animal, medicine.anatomical_structure, chemistry, Case-Control Studies, Leukocytes, Mononuclear, Female, Reactive Oxygen Species, business

Abstract

The dysregulated host response and organ damage following systemic infection that characterizes a septic event predisposes individuals to a chronic immunoparalysis state associated with severe transient lymphopenia and diminished lymphocyte function, thereby reducing long-term patient survival and quality of life. Recently, we observed lasting production of reactive oxygen species (ROS) in mice that survive sepsis. ROS production is a potent mechanism for targeting infection, but excessive ROS production can prove maladaptive by causing organ damage, impairing lymphocyte function, and promoting inflammaging, concepts paralleling sepsis-induced immunoparalysis. Notably, we observed an increased frequency of ROS-producing immature monocytes in septic hosts that was sustained for greater than 100 days postsurgery. Recent clinical trials have explored the use of vitamin C, a potent antioxidant, for treating septic patients. We observed that therapeutic vitamin C administration for sepsis limited ROS production by monocytes and reduced disease severity. Importantly, we also observed increased ROS production by immature monocytes in septic patients both at admission and ∼28 days later, suggesting a durable and conserved feature that may influence the host immune response. Thus, lasting ROS production by immature monocytes is present in septic patients, and early intervention strategies to reduce it may improve host outcomes, potentially reducing sepsis-induced immunoparalysis.

Published

2021

23. Current Update on Severe Acute Respiratory Syndrome Coronavirus 2 Vaccine Development with a Special Emphasis on Gene Therapy Viral Vector Design and Construction for Vaccination

Author

Thomas S. Griffith, Ahter Dilsad Sanlioglu, Atil Bisgin, Yunus Emre Ekşi, and Salih Sanlioglu

Subjects

COVID-19 Vaccines, viruses, medicine.medical_treatment, Genetic Vectors, Vaccines, Attenuated, medicine.disease_cause, Adenoviridae, DNA vaccination, Viral vector, 03 medical and health sciences, 0302 clinical medicine, Immune system, Vaccines, DNA, Genetics, medicine, Humans, Molecular Biology, 030304 developmental biology, Coronavirus, Viral Structural Proteins, Vaccines, Synthetic, 0303 health sciences, Attenuated vaccine, SARS-CoV-2, business.industry, Viral Vaccine, Lentivirus, Genetic Therapy, Virology, Vaccination, 030220 oncology & carcinogenesis, Molecular Medicine, business, Adjuvant

Abstract

Severe acute respiratory syndrome (SARS) is a newly emerging infectious disease (COVID-19) caused by the novel coronavirus SARS-coronavirus 2 (CoV-2). To combat the devastating spread of SARS-CoV-2, extraordinary efforts from numerous laboratories have focused on the development of effective and safe vaccines. Traditional live-attenuated or inactivated viral vaccines are not recommended for immunocompromised patients as the attenuated virus can still cause disease via phenotypic or genotypic reversion. Subunit vaccines require repeated dosing and adjuvant use to be effective, and DNA vaccines exhibit lower immune responses. mRNA vaccines can be highly unstable under physiological conditions. On the contrary, naturally antigenic viral vectors with well-characterized structure and safety profile serve as among the most effective gene carriers to provoke immune response via heterologous gene transfer. Viral vector-based vaccines induce both an effective cellular immune response and a humoral immune response owing to their natural adjuvant properties via transduction of immune cells. Consequently, viral vectored vaccines carrying the SARS-CoV-2 spike protein have recently been generated and successfully used to activate cytotoxic T cells and develop a neutralizing antibody response. Recent progress in SARS-CoV-2 vaccines, with an emphasis on gene therapy viral vector-based vaccine development, is discussed in this review.

Published

2021

24. Temporal association rules discovery algorithm based on improved index tree

Author

Wang Rui, Zeng Bin, W. S. Griffith, and Chen Yuanyuan

Subjects

0209 industrial biotechnology, Index (economics), General Computer Science, Association rule learning, Computer science, Applied Mathematics, Association (object-oriented programming), 02 engineering and technology, Space (commercial competition), Tree (data structure), 020901 industrial engineering & automation, Modeling and Simulation, 0202 electrical engineering, electronic engineering, information engineering, A priori and a posteriori, 020201 artificial intelligence & image processing, Predictability, Engineering (miscellaneous), Algorithm, Big data mining

Abstract

With the rapid increase of information generated from all kinds of sources, temporal big data mining in business area has been paid more and more attention recently. A novel data mining algorithm for mining temporal association is proposed. Mining temporal association can not only provide better predictability for customer behaviour but also help organisations with better strategies and marketing decisions. To compare the proposed algorithm, two methods to mine temporal association are presented. One is improved based on a traditional mining algorithm, Apriori. The other is based on an Index-Tree. Moreover, the proposed method is extended to mine temporal association in multi-dimensional space. The experimental results show that the Index-Tree method outperforms the Apriori-modified method in all cases.

Published

2021

25. Two Distinct Yersinia pestis Populations Causing Plague among Humans in the West Nile Region of Uganda.

Author

Laurel B Respicio-Kingry, Brook M Yockey, Sarah Acayo, John Kaggwa, Titus Apangu, Kiersten J Kugeler, Rebecca J Eisen, Kevin S Griffith, Paul S Mead, Martin E Schriefer, and Jeannine M Petersen

Subjects

Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270

Abstract

Plague is a life-threatening disease caused by the bacterium, Yersinia pestis. Since the 1990s, Africa has accounted for the majority of reported human cases. In Uganda, plague cases occur in the West Nile region, near the border with Democratic Republic of Congo. Despite the ongoing risk of contracting plague in this region, little is known about Y. pestis genotypes causing human disease.During January 2004-December 2012, 1,092 suspect human plague cases were recorded in the West Nile region of Uganda. Sixty-one cases were culture-confirmed. Recovered Y. pestis isolates were analyzed using three typing methods, single nucleotide polymorphisms (SNPs), pulsed field gel electrophoresis (PFGE), and multiple variable number of tandem repeat analysis (MLVA) and subpopulations analyzed in the context of associated geographic, temporal, and clinical data for source patients. All three methods separated the 61 isolates into two distinct 1.ANT lineages, which persisted throughout the 9 year period and were associated with differences in elevation and geographic distribution.We demonstrate that human cases of plague in the West Nile region of Uganda are caused by two distinct 1.ANT genetic subpopulations. Notably, all three typing methods used, SNPs, PFGE, and MLVA, identified the two genetic subpopulations, despite recognizing different mutation types in the Y. pestis genome. The geographic and elevation differences between the two subpopulations is suggestive of their maintenance in highly localized enzootic cycles, potentially with differing vector-host community composition. This improved understanding of Y. pestis subpopulations in the West Nile region will be useful for identifying ecologic and environmental factors associated with elevated plague risk.

Published

2016

26. A framework to assess higher education faculty workload in U.S. universities

Author

Andrew S Griffith and Zeynep Altinay

Subjects

Service (business), 2019-20 coronavirus outbreak, Medical education, genetic structures, 020205 medical informatics, Higher education, business.industry, education, 05 social sciences, Higher education policy, 050301 education, Workload, 02 engineering and technology, Education, Scholarship, Political science, ComputingMilieux_COMPUTERSANDEDUCATION, 0202 electrical engineering, electronic engineering, information engineering, Time management, business, 0503 education, Productivity, psychological phenomena and processes

Abstract

Faculty are often evaluated on perceptions of their teaching effectiveness, their service activities, and their research productivity. To meet their institutional standards in each area, the facult...

Published

2020

27. TLR7/8 Agonist-Loaded Nanoparticles Augment NK Cell-Mediated Antibody-Based Cancer Immunotherapy

Author

Tamara A. Kucaba, Drishti Sehgal, Vidhi Khanna, Jayanth Panyam, Thomas S. Griffith, David M. Ferguson, Hyunjoon Kim, and Wenqiu Zhang

Subjects

Male, Agonist, medicine.drug_class, medicine.medical_treatment, Pharmaceutical Science, 02 engineering and technology, 030226 pharmacology & pharmacy, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cancer immunotherapy, Epidermal growth factor, In vivo, Drug Discovery, medicine, Animals, Humans, Receptor, Antibody-dependent cell-mediated cytotoxicity, Mice, Inbred BALB C, Imiquimod, Chemistry, Dendritic Cells, Flow Cytometry, 021001 nanoscience & nanotechnology, Killer Cells, Natural, Mice, Inbred C57BL, Imidazoquinoline, Nanomedicine, Toll-Like Receptor 7, A549 Cells, Toll-Like Receptor 8, Leukocytes, Mononuclear, Cancer research, Nanoparticles, Molecular Medicine, Cytokine secretion, Immunotherapy, 0210 nano-technology

Abstract

Activated natural killer (NK) cells can kill malignant tumor cells via granule exocytosis and secretion of IFN-γ, a key regulator of the TH1 response. Thus, mobilization of NK cells can augment cancer immunotherapy, particularly when mediated through antibody-dependent cellular cytotoxicity (ADCC). Stimulation of toll-like receptor (TLR)7/8 activity in dendritic cells promotes pro-inflammatory cytokine secretion and costimulatory molecule upregulation, both of which can potentiate NK cell activation. However, currently available TLR7/8 agonists exhibit unfavorable pharmacokinetics, limiting their in vivo efficacy. To enable efficient delivery to antigen-presenting cells, we encapsulated a novel imidazoquinoline-based TLR7/8 agonist in pH-responsive polymeric NPs. Enhanced costimulatory molecule expression on dendritic cells and a stronger pro-inflammatory cytokine response were observed with a NP-encapsulated agonist, compared to that with the soluble form. Treatment with NP-encapsulated agonists resulted in stronger in vivo cytotoxicity and prolonged activation of NK cells compared to that with a soluble agonist. In addition, TLR7/8 agonist-loaded NPs potentiated stronger NK cell degranulation, which resulted in enhanced in vitro and in vivo ADCC mediated by the epidermal growth factor receptor-targeting antibody cetuximab. TLR7/8 agonist-loaded NP treatment significantly enhanced the antitumor efficacy of cetuximab and an anti-HER2/neu antibody in mouse tumor models. Collectively, our data show that a pH-responsive NP-encapsulating TLR7/8 agonist could be used as a potent immunostimulatory adjuvant for antibody-based cancer immunotherapy by promoting NK cell activation.

Published

2020

28. Exploiting antibody biology for the treatment of cancer

Author

Thomas S. Griffith, Vidhi Khanna, and Jayanth Panyam

Subjects

biology, medicine.drug_class, Immunology, Antibody-Dependent Cell Cytotoxicity, Cancer, Computational biology, Monoclonal antibody, medicine.disease, Antibodies, Antineoplastic Agents, Immunological, Oncology, Antigens, Neoplasm, Neoplasms, medicine, biology.protein, Humans, Immunology and Allergy, Drug Therapy, Combination, Antibody, Immune Checkpoint Inhibitors, Monoclonal antibody therapy

Abstract

Over the last decade, antibodies have become an important component in the arsenal of cancer therapeutics. High-specificity, low off-target effects, desirable pharmacokinetics and high success rate are a few of the many attributes that make antibodies amenable for development as drugs. To design antibodies for successful clinical applications, however, it is critical to have an understanding of their structure, functions, mechanisms of action and pharmacokinetic/pharmacodynamic properties. This review highlights some of these key aspects, as well as certain limitations encountered, with monoclonal antibody therapy. Further, we discuss rational combination therapies for clinical applications, some of which could help overcome the limitations.

Published

2020

29. Applying Chickering and Gamson's Principles to Engage Today's Online Learner

Author

Jennifer S. Griffith, Aubrey L. C. Statti, and Kelly M. Torres

Subjects

ComputingMilieux_COMPUTERSANDEDUCATION

Abstract

Chickering and Gamson introduced seven principles for engaging undergraduate students into the literature in 1987. The principles provided faculty with the foundational best practices they could incorporate into their own courses. Using Chickering and Gamson's best practices, the authors of this chapter conducted a literature review on how these best practices could be used for engaging learners through the support of technology. Institutions of higher education are incorporating online degree programs in their strategies and should understand how to prepare faculty, especially new faculty, for facilitating online courses for nontraditional students using the learning management system (LMS), technology, pedagogical approaches, and best practices.

Published

2022

30. Contributions of individual reactive biogenic volatile organic compounds to organic nitrates above a mixed forest

Author

K. A. Pratt, L. H. Mielke, P. B. Shepson, A. M. Bryan, A. L. Steiner, J. Ortega, R. Daly, D. Helmig, C. S. Vogel, S. Griffith, S. Dusanter, P. S. Stevens, and M. Alaghmand

Subjects

Physics, QC1-999, Chemistry, QD1-999

Abstract

Biogenic volatile organic compounds (BVOCs) can react in the atmosphere to form organic nitrates, which serve as NOx (NO + NO2) reservoirs, impacting ozone and secondary organic aerosol production, the oxidative capacity of the atmosphere, and nitrogen availability to ecosystems. To examine the contributions of biogenic emissions and the formation and fate of organic nitrates in a forest environment, we simulated the oxidation of 57 individual BVOCs emitted from a rural mixed forest in northern Michigan. Key BVOC-oxidant reactions were identified for future laboratory and field investigations into reaction rate constants, yields, and speciation of oxidation products. Of the total simulated organic nitrates, monoterpenes contributed ~70% in the early morning at ~12 m above the forest canopy when isoprene emissions were low. In the afternoon, when vertical mixing and isoprene nitrate production were highest, the simulated contribution of isoprene-derived organic nitrates was greater than 90% at all altitudes, with the concentration of secondary isoprene nitrates increasing with altitude. Notably, reaction of isoprene with NO3 leading to isoprene nitrate formation was found to be significant (~8% of primary organic nitrate production) during the daytime, and monoterpene reactions with NO3 were simulated to comprise up to ~83% of primary organic nitrate production at night. Lastly, forest succession, wherein aspen trees are being replaced by pine and maple trees, was predicted to lead to increased afternoon concentrations of monoterpene-derived organic nitrates. This further underscores the need to understand the formation and fate of these species, which have different chemical pathways and oxidation products compared to isoprene-derived organic nitrates and can lead to secondary organic aerosol formation.

Published

2012

31. The analysis and comparison of start-up demonstration tests.

Author

Michelle L. DePoy Smith and William S. Griffith

Published

2008

32. Generation of a Beta-Cell Transplant Animal Model of Diabetes Using CRISPR Technology

Author

Yunus Emre Eksi, Atil Bisgin, Ahter D. Sanlioglu, Reha Onur Azizoglu, Mustafa Kemal Balci, Thomas S. Griffith, and Salih Sanlioglu

Published

2022

33. Physiological microbial exposure transiently inhibits mouse lung ILC2 responses to allergens

Author

Katharine E. Block, Koji Iijima, Mark J. Pierson, Daniel A. Walsh, Rinna Tei, Tamara A. Kucaba, Julie Xu, Mohammad Haneef Khan, Christopher Staley, Thomas S. Griffith, Henry J. McSorley, Hirohito Kita, and Stephen C. Jameson

Subjects

Immunology, Immunology and Allergy, Article

Abstract

Lung group 2 innate lymphoid cells (ILC2) determine the nature of the immune response to airway allergens. Some microbial products, including those stimulating interferons, block ILC2 activation, but whether this occurs following natural infections or causes durable ILC2 inhibition is unclear. We tested this using a model of physiological microbial exposures through cohousing laboratory and pet store mice. Laboratory mice cohoused for two weeks displayed an impaired ILC2 response and reduced lung eosinophilia toward intranasal allergens, while these responses were restored in mice cohoused at least two months. ILC2 inhibition at two weeks correlated with increased interferon receptor signaling, which waned by two months of cohousing. Re-induction of interferons in two-month cohoused mice blocked ILC2 activation. These findings suggest ILC2 respond dynamically to environmental cues and that microbial exposures do not dictate long-term desensitization of innate type-2 responses to allergens.

Published

2021

34. Toll-like receptor 7 and 8 imidazoquinoline-based agonist/antagonist pairs

Author

Mu Yang, Peter G. Larson, Lincoln Brown, John R. Schultz, Tamara A. Kucaba, Thomas S. Griffith, and David M. Ferguson

Subjects

Dose-Response Relationship, Drug, Molecular Structure, Organic Chemistry, Clinical Biochemistry, Imidazoles, Pharmaceutical Science, Biochemistry, Structure-Activity Relationship, Toll-Like Receptor 7, Toll-Like Receptor 8, Drug Discovery, Quinolines, Molecular Medicine, Humans, Molecular Biology

Abstract

Toll-like receptors (TLRs) 7 and 8 are key targets in the development of immunomodulatory drugs for treating infectious disease, cancer, and autoimmune disorders. These receptors can adopt both agonist and antagonist binding conformations that switch the receptor signal on or off to the downstream production of cytokines. In this study, we examined the effect of simple isomeric substitutions to the C2-butyl group of two imidazoquinoline agonists and evaluated the activity of these analogs using both TLR7 and TLR8 reporter cells and cytokine induction assays. Results are presented showing the C2-isobutyl and C2-cyclopropylmethyl isomers are both mixed TLR7/8 competitive antagonists of the parent agonist [4-Amino-1-(4-(aminomethyl)benzyl)-2-butyl-7-methoxycarbonyl-1H-imidazo[4,5-c]quinoline], indicating the conformation of the dimeric receptor complex is highly sensitive to steric perturbations to the ligand binding pocket. This observation is consistent with prior work demonstrating TLR7 and TLR8 activity is directly correlated to C2-alkyl substitutions that project into a hydrophobic pocket at the dimer interface of the receptor. The close structural relationship of the agonist/antagonist pairs identified here highlights the importance of this pocket in tipping the balance between the agonist and antagonist binding states of the receptor which may have significant ramifications to the design of imidazoquinoline-based immunomodulatory agents.

Published

2021

35. Comparing methods for estimating hemispheric dominance for language using TMS: A multicenter study

Author

Talitha Boardman, Molly S. Griffith, Joanne Hall, James W. Wheless, Hansel Greiner, Alexander Rotenberg, and Shalini Narayana

Subjects

General Neuroscience, Biophysics, Neurology (clinical)

Published

2023

36. Black women’s menstrual and reproductive health: a critical call for action in the UK

Author

Danielle Perro, Holly Seglah, Victoria Abrahams, Annalise Weckesser, and Véronique A S Griffith

Subjects

General Medicine

Published

2022

37. Combination of STING and TLR 7/8 Agonists as Vaccine Adjuvants for Cancer Immunotherapy

Author

Shubhmita Bhatnagar, Vishnu Revuri, Manan Shah, Peter Larson, Zekun Shao, Daohai Yu, Swayam Prabha, Thomas S. Griffith, David Ferguson, and Jayanth Panyam

Subjects

Cancer Research, Oncology, cancer immunotherapy, cancer vaccine, toll-like receptors, STING, DMXAA

Abstract

Immunostimulatory adjuvants that potently activate antigen-presenting cells and (in turn) prime cytotoxic T cells are a key component of anticancer vaccines. In this study, we investigated a multi-adjuvant approach combining a TLR 7/8 agonist (522) and a STING agonist (DMXAA) to promote enhanced antigen cross-presentation, stimulate specific antitumor T-cell responses, and provide improved anticancer efficacy. In vitro experiments using bone marrow-derived dendritic cells (BMDCs) confirmed enhanced activation with the 522-DMXAA combination based on both co-stimulatory molecule expression and pro-inflammatory cytokine secretion. The immunization of mice with vaccines comprising both 522 and DMXAA resulted in greater antitumor efficacy in B16F10 melanoma and MB49 bladder tumor models relative to mono-agonist vaccines. Flow cytometry-based analysis of immune cells from immunized mice revealed the significant activation of antigen-presenting cells, increased numbers of activated and Ag-specific CD8+ T cells in the spleen and lymph nodes, modest NK cell activation, and an overall reduction in CD206+ macrophages. These results were supported by an increase in the levels of IFN-γ and a reduction in IL-10 levels in the sera. Taken together, these findings demonstrate the potential of the TLR7/8 and STING agonist combination as vaccine adjuvants to activate both innate and adaptive immune responses.

Published

2022

38. Extended block replacement policy with shock models and used items.

Author

Shey-Huei Sheu and William S. Griffith

Published

2002

39. Optimal age-replacement policy with age-dependent minimal-repair and random-leadtime.

Author

Shey-Huei Sheu and William S. Griffith

Published

2001

40. Using group concept mapping software to develop a conceptual framework of left ventricular assist device recipients' experiences

Author

A.L Slade, S Griffith, S Lim, M.E O'Hara, Melanie Calvert, David W. Quinn, Deirdre A. Lane, L Marley, and M.S Haque

Subjects

Group concept mapping, Software, Conceptual framework, business.industry, Ventricular assist device, medicine.medical_treatment, medicine, Cardiology and Cardiovascular Medicine, Software engineering, business

Abstract

Background Advanced Heart failure (AHF) carries a high mortality rate. Heart transplantation is one therapeutic option, but low donation rates limits its availability. A left ventricular assist device (LVAD) is an alternative therapy which helps relieve symptoms, while improving prognosis and quality of life. However, lack of donors also means that the LVAD becomes a destination therapy by default.(1) Living with an LVAD requires significant psychological, social and physical adaptation for the recipients' and their families.(2) Patient reported outcome measures (PROMs) are one way of capturing these concerns and ongoing problems. Discussions with a patient and public involvement group found a range of issues not currently captured by available PROMS. Aim To develop a conceptual framework which reflects the experiences of LVAD recipients' and evaluate their importance for inclusion in PROMs using a research web platform. Method Participants were recruited from a regional transplant centre which covers a wide geographical area in the UK. Ethical approval was obtained and participants were recruited through routine LVAD clinics. Group concept mapping (GCM) is a semi-quantitative mixed methods approach that can be used to capture and quantify recipients' experiences.(3) Groupwisdom concept mapping software was used as the electronic data collection platform.(4) GCM consists of 3 stages: statement generation, thematic statement sorting, and rating statements for importance, relevance and frequency of impact. Multidimensional scaling and hierarchical cluster analysis produces visual representations of recipients' experiences as a points and cluster map, and scoring of statements produces relative importance of items across the clusters. Results 18 LVAD recipients consented to take part. 101 items and 9 clusters were generated. Clusters represented: Activities; Partner/family dependency; Travel; Mental well-being; LVAD challenges; Equipment and clothing; Physical and cognitive limitations; Restrictions, and LVAD positives. LVAD Positives and LVAD restrictions were rated high for frequency, relevance and importance. Physical and cognitive limitations was rated high for importance and frequency. Equipment was rated high for relevance and frequency, and Challenges was rated high for relevance. Conclusion GCM and the online software is a useful tool for developing a conceptual framework and mapping key areas of importance for LVAD recipients, especially, when prioritising important patient reported outcome domains for use in clinical practice, future research and design evolution. Using an electronic platform allowed us to reach participants dispersed over a wide geographical area. Funding Acknowledgement Type of funding sources: Other. Main funding source(s): British Heart FoundationNational Institute for Health Research Cluster Rating Map for Importance

Published

2021

41. Sepsis leads to lasting changes in phenotype and function of memory CD8 T cells

Author

Mikaela M. Tremblay, Isaac J. Jensen, Thomas S. Griffith, Weiqun Peng, Micaela G. Fosdick, Qiang Shan, Vladimir P. Badovinac, Xiang Li, Jon C. D. Houtman, Patrick W. McGonagill, and Hai-Hui Xue

Subjects

Male, Mouse, Transcription, Genetic, Cell, CD8-Positive T-Lymphocytes, sepsis, Mice, Immunology and Inflammation, Cytotoxic T cell, homeostatic proliferation, Biology (General), education.field_of_study, General Neuroscience, General Medicine, Middle Aged, Phenotype, Vaccination, medicine.anatomical_structure, Medicine, Female, medicine.symptom, Research Article, central memory, Human, Adult, QH301-705.5, Science, Population, Inflammation, Biology, General Biochemistry, Genetics and Molecular Biology, Sepsis, Immune system, medicine, Animals, Humans, education, Aged, Cell Proliferation, General Immunology and Microbiology, medicine.disease, Chromatin Assembly and Disassembly, Listeria monocytogenes, CD8 T cell, Case-Control Studies, Immunology, Immunologic Memory

Abstract

The global health burden due to sepsis and the associated cytokine storm is substantial. While early intervention has improved survival during the cytokine storm, those that survive can enter a state of chronic immunoparalysis defined by transient lymphopenia and functional deficits of surviving cells. Memory CD8 T cells provide rapid cytolysis and cytokine production following re-encounter with their cognate antigen to promote long-term immunity, and CD8 T cell impairment due to sepsis can pre-dispose individuals to re-infection. While the acute influence of sepsis on memory CD8 T cells has been characterized, if and to what extent pre-existing memory CD8 T cells recover remains unknown. Here, we observed that central memory CD8 T cells (TCM) from septic patients proliferate more than those from healthy individuals. Utilizing LCMV immune mice and a CLP model to induce sepsis, we demonstrated that TCM proliferation is associated with numerical recovery of pathogen-specific memory CD8 T cells following sepsis-induced lymphopenia. This increased proliferation leads to changes in composition of memory CD8 T cell compartment and altered tissue localization. Further, memory CD8 T cells from sepsis survivors have an altered transcriptional profile and chromatin accessibility indicating long-lasting T cell intrinsic changes. The sepsis-induced changes in the composition of the memory CD8 T cell pool and transcriptional landscape culminated in altered T cell function and reduced capacity to control L. monocytogenes infection. Thus, sepsis leads to long-term alterations in memory CD8 T cell phenotype, protective function and localization potentially changing host capacity to respond to re-infection., eLife digest A dirty cut, a nasty burn, a severe COVID infection; there are many ways for someone to develop sepsis. This life-threatening condition emerges when the immune system overreacts to a threat and ends up damaging the body. Even when patients survive, they are often left with a partially impaired immune system that cannot adequately protect against microbes and cancer; this is known as immunoparalysis. Memory CD8 T cells, a type of immune cell that is compromised by sepsis, are a long-lived population of cells that ‘remember’ previous infection or vaccination, and then react faster to prevent the same illness if the person ever encounters the same threat again. Yet it is unclear how exactly sepsis harms the function and representation of memory CD8 T cells, and the immune system in general. Jensen et al. investigated this question, first by showing that sepsis leads to a profound loss of memory CD8 T cells, but that surviving memory CD8 T cells multiply quickly – especially a subpopulation known as central memory CD8 T cells – to re-establish the memory CD8 T cell population. Since the central memory CD8 T cells proliferate better than the other memory T cells this alters the overall composition of the pool of memory CD8 T cells, with central memory cells becoming overrepresented. Further experiments revealed that this biasing toward central memory T cells, due to sepsis, created long-term changes in the distribution of memory CD8 T cells throughout the body. The way the genetic information of these cells was packaged had also been altered, as well as which genes were switched on or off. Overall, these changes reduced the ability of memory CD8 T cells to control infections. Together, these findings help to understand how immunoparalysis can emerge after sepsis, and what could be done to correct it. These findings could also be applied to other conditions – such as COVID-19 – which may cause similar long-term changes to the immune system.

Published

2021

42. Author response: Sepsis leads to lasting changes in phenotype and function of memory CD8 T cells

Author

Thomas S. Griffith, Weiqun Peng, Micaela G. Fosdick, Jon C. D. Houtman, Vladimir P. Badovinac, Xiang Li, Qiang Shan, Isaac J. Jensen, Mikaela M. Tremblay, Patrick W. McGonagill, and Hai-Hui Xue

Subjects

Sepsis, business.industry, Immunology, Medicine, Cytotoxic T cell, business, medicine.disease, Phenotype, Function (biology)

Published

2021

43. Bioterrorism-related Inhalational Anthrax in an Elderly Woman, Connecticut, 2001

Author

Kevin S. Griffith, Paul S. Mead, Gregory L. Armstrong, John A. Painter, Katherine A. Kelley, Alex R. Hoffmaster, Donald Mayo, Diane Barden, Renee Ridzon, Umesh D. Parashar, Eyasu Habtu Teshale, Jen Williams, Stephanie Noviello, Joseph F. Perz, Eric E. Mast, David L. Swerdlow, and James L. Hadler

Subjects

Bacillus anthracis, bioterrorism, Connecticut, inhalational anthrax, postal facilities, research, Medicine, Infectious and parasitic diseases, RC109-216

Abstract

On November 20, 2001, inhalational anthrax was confirmed in an elderly woman from rural Connecticut. To determine her exposure source, we conducted an extensive epidemiologic, environmental, and laboratory investigation. Molecular subtyping showed that her isolate was indistinguishable from isolates associated with intentionally contaminated letters. No samples from her home or community yielded Bacillus anthracis, and she received no first-class letters from facilities known to have processed intentionally contaminated letters. Environmental sampling in the regional Connecticut postal facility yielded B. anthracis spores from 4 (31%) of 13 sorting machines. One extensively contaminated machine primarily processes bulk mail. A second machine that does final sorting of bulk mail for her zip code yielded B. anthracis on the column of bins for her carrier route. The evidence suggests she was exposed through a cross-contaminated bulk mail letter. Such cross-contamination of letters and postal facilities has implications for managing the response to future B. anthracis–contaminated mailings.

Published

2003

44. Anthrax Postexposure Prophylaxis in Postal Workers, Connecticut, 2001

Author

Jennifer L. Williams, Stephanie S. Noviello, Kevin S. Griffith, Heather Wurtzel, Jennifer Hamborsky, Joseph F. Perz, Ian T. Williams, James L. Hadler, David L. Swerdlow, and Renee Ridzon

Subjects

adverse effects, Anthrax, Bacillus anthracis, ciprofloxacin, Connecticut, doxycycline, Medicine, Infectious and parasitic diseases, RC109-216

Abstract

After inhalational anthrax was diagnosed in a Connecticut woman on November 20, 2001, postexposure prophylaxis was recommended for postal workers at the regional mail facility serving the patient’s area. Although environmental testing at the facility yielded negative results, subsequent testing confirmed the presence of Bacillus anthracis. We distributed questionnaires to 100 randomly selected postal workers within 20 days of initial prophylaxis. Ninety-four workers obtained antibiotics, 68 of whom started postexposure prophylaxis and 21 discontinued. Postal workers who stopped or never started taking prophylaxis cited as reasons disbelief regarding anthrax exposure, problems with adverse events, and initial reports of negative cultures. Postal workers with adverse events reported predominant symptoms of gastrointestinal distress and headache. The influence of these concerns on adherence suggests that communication about risks of acquiring anthrax, education about adverse events, and careful management of adverse events are essential elements in increasing adherence.

Published

2002

45. Cutting Edge: Polymicrobial Sepsis Has the Capacity to Reinvigorate Tumor-Infiltrating CD8 T Cells and Prolong Host Survival

Author

Vladimir P. Badovinac, Isaac J. Jensen, Thomas S. Griffith, and Derek B. Danahy

Subjects

business.industry, medicine.medical_treatment, Immunology, Cancer, medicine.disease, Malignancy, Blockade, Sepsis, 03 medical and health sciences, 0302 clinical medicine, Cytokine, medicine, Cancer research, Immunology and Allergy, Cytotoxic T cell, business, Receptor, CD8, 030215 immunology

Abstract

Malignancy increases sepsis incidence 10-fold and elevates sepsis-associated mortality. Advances in treatment have improved survival of cancer patients shortly after sepsis, but there is a paucity of information on how sepsis impacts cancer growth, development, and prognosis. To test this, cecal ligation and puncture surgery was performed on B16 melanoma-bearing mice to show that sepsis has detrimental effects in hosts with advanced tumors, leading to increased mortality. Surprisingly, mice experiencing cecal ligation and puncture–induced sepsis earlier during tumor development exhibited CD8 T cell–dependent attenuation of tumor growth. Sepsis-resistant CD8 tumor-infiltrating T cells showed increased in vivo activation, effector IFN-γ cytokine production, proliferation, and expression of activation/inhibitory PD-1/LAG-3 receptors because of a sepsis-induced liberation of tumor Ags. Sepsis-reinvigorated CD8 tumor-infiltrating T cells were also amenable to (anti–PD-L1/LAG-3) checkpoint blockade therapy, further prolonging cancer-associated survival in sepsis survivors. Thus, sepsis has the capacity to improve tumor-specific CD8 T cell responses, leading to better cancer prognosis and increased survival.

Published

2019

46. Binary State Start‐Up Demonstration Tests

Author

William S. Griffith and Michelle L. DePoy Smith

Subjects

Computer science, Binary number, State (computer science), Start up, Algorithm

Published

2019

47. Multistate Start‐Up Demonstration Tests

Author

William S. Griffith and Michelle L. DePoy Smith

Subjects

Computer science, Start up, Reliability engineering

Published

2019

48. Autoimmunity increases susceptibility to and mortality from sepsis

Author

Isaac J. Jensen, Patrick W. McGonagill, Ashutosh K. Mangalam, Thomas S. Griffith, Vladimir P. Badovinac, and Samantha N. Jensen

Subjects

Adult, Male, Encephalomyelitis, Autoimmune, Experimental, Multiple Sclerosis, Adolescent, medicine.medical_treatment, Immunology, Datasets as Topic, medicine.disease_cause, Pneumococcal Infections, Autoimmunity, Sepsis, Mice, Young Adult, Risk Factors, Streptococcus pneumoniae, Prevalence, Retrospective analysis, medicine, Animals, Humans, Immunology and Allergy, Aged, Retrospective Studies, Aged, 80 and over, Autoimmune disease, Immune status, business.industry, Multiple sclerosis, Incidence (epidemiology), Experimental autoimmune encephalomyelitis, General Medicine, Middle Aged, medicine.disease, Patient population, Cytokine, Female, Disease Susceptibility, business

Abstract

We recently demonstrated how sepsis influences the subsequent development of experimental autoimmune encephalomyelitis (EAE) presented a conceptual advance in understanding the postsepsis chronic immunoparalysis state. However, the reverse scenario (autoimmunity prior to sepsis) defines a high-risk patient population whose susceptibility to sepsis remains poorly defined. In this study, we present a retrospective analysis of University of Iowa Hospital and Clinics patients demonstrating increased sepsis prevalence among multiple sclerosis (MS), relative to non-MS, patients. To interrogate how autoimmune disease influences host susceptibility to sepsis, well-established murine models of MS and sepsis and EAE and cecal ligation and puncture, respectively, were used. EAE, relative to non-EAE, mice were highly susceptible to sepsis-induced mortality with elevated cytokine storms. These results were further recapitulated in LPS and Streptococcus pneumoniae sepsis models. This work highlights both the relevance of identifying highly susceptible patient populations and expands the growing body of literature that host immune status at the time of septic insult is a potent mortality determinant.

Published

2021

49. From Capital Surges to Drought: Seeking Stability for Emerging Economies

Author

R. Ffrench-Davis, S. Griffith-Jones

Published

2003

50. Sepsis and multiple sclerosis: Causative links and outcomes

Author

Isaac J. Jensen, Thomas S. Griffith, Suzana Stanisavljević, Vladimir P. Badovinac, and Đorđe Miljković

Subjects

Multiple Sclerosis, Neuroimmunomodulation, Secondary infection, Immunology, Gut flora, medicine.disease_cause, Article, Autoimmunity, Sepsis, 03 medical and health sciences, 0302 clinical medicine, Immune system, Brain-Gut Axis, medicine, Immunology and Allergy, Animals, Humans, 030304 developmental biology, 0303 health sciences, biology, business.industry, Multiple sclerosis, biology.organism_classification, medicine.disease, 3. Good health, Review article, Gastrointestinal Microbiome, Organ Specificity, Immune System, Disease Susceptibility, business, Cytokine storm, 030217 neurology & neurosurgery, Biomarkers

Abstract

Sepsis is a life-threatening condition characterized by an acute cytokine storm followed by prolonged dysfunction of the immune system in the survivors. Post-septic lymphopenia and functional deficits of the remaining immune cells lead to increased susceptibility to secondary infections and other morbid conditions causing late death in the patients. This state of post-septic immunoparalysis may also influence disorders stemming from inappropriate or overactive immune responses, such as autoimmune and immunoinflammatory diseases, including multiple sclerosis. In addition, ongoing autoimmunity likely influences the susceptibility to and outcome of sepsis. This review article addresses the bidirectional relationship between sepsis and multiple sclerosis, with a focus on the immunologic mechanisms of the interaction and potential directions for future studies.

Published

2021