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1. P1257: SMART101 DONOR T-LYMPHOID PROGENITORS TO ACCELERATE IMMUNE RECONSTITUTION POST-HAPLOIDENTICAL PERIPHERAL BLOOD STEM CELL TRANSPLANTATION WITH POST-TRANSPLANT CYCLOPHOSPHAMIDE: SI101-02 PHASE I/II

Author

Fabio Ciceri, Régis Peffault de Latour, Raynier Devillier, Patrizia Chiusolo, Aurelie Bauquet, Laura Simons, Pierre Heimendinger, Pierre Gaudeaux, Olivier Negre, Tayebeh-Shabi Soheili, Juliette Paillet, Isabelle Andre, Sebastien Oster, Marina Cavazzana, and Frederic Lehmann

Subjects
Diseases of the blood and blood-forming organs, RC633-647.5
Published
2023
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2. P1403: SI101-01 PHASE I/II STUDY EVALUATING SAFETY AND EFFICACY OF ALLOGENEIC SMART101 T-LYMPHOID PROGENITOR INJECTION TO ACCELERATE IMMUNE RECONSTITUTION AFTER T-CELL DEPLETED ALLOGENEIC HSCT

Author

Jaap Jan Boelens, Muhammad Umair Mushtaq, Joseph Mcguirk, Aurelie Bauquet, Laura Simons, Pierre Heimendinger, Pierre Gaudeaux, Isabelle Andre, Juliette Paillet, Olivier Negre, Tayebeh-Shabi Soheili, Sebastien Oster, Marcel R.M. van den Brink, Frederic Lehmann, Marina Cavazzana, and Miguel-Angel Perales

Subjects
Diseases of the blood and blood-forming organs, RC633-647.5
Published
2023
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3. T-Cell Progenitors As A New Immunotherapy to Bypass Hurdles of Allogeneic Hematopoietic Stem Cell Transplantation

Author

Pierre Gaudeaux, Ranjita Devi Moirangthem, Aurélie Bauquet, Laura Simons, Akshay Joshi, Marina Cavazzana, Olivier Nègre, Shabi Soheili, and Isabelle André

Subjects
allogeneic hematopoietic stem cell transplantation, T-cells, immune reconstitution, T-cell progenitors, immunotherapy, thymus, Immunologic diseases. Allergy, RC581-607
Abstract

Allogeneic hematopoietic stem cell transplantation (HSCT) is the treatment of preference for numerous malignant and non-malignant hemopathies. The outcome of this approach is significantly hampered by not only graft-versus-host disease (GvHD), but also infections and relapses that may occur because of persistent T-cell immunodeficiency following transplantation. Reconstitution of a functional T-cell repertoire can take more than 1 year. Thus, the major challenge in the management of allogeneic HSCT relies on the possibility of shortening the window of immune deficiency through the acceleration of T-cell recovery, with diverse, self-tolerant, and naïve T cells resulting from de novo thymopoiesis from the donor cells. In this context, adoptive transfer of cell populations that can give rise to mature T cells faster than HSCs while maintaining a safety profile compatible with clinical use is of major interest. In this review, we summarize current advances in the characterization of thymus seeding progenitors, and their ex vivo generated counterparts, T-cell progenitors. Transplantation of the latter has been identified as a worthwhile approach to shorten the period of immune deficiency in patients following allogeneic HSCT, and to fulfill the clinical objective of reducing morbimortality due to infections and relapses. We further discuss current opportunities for T-cell progenitor-based therapy manufacturing, including iPSC cell sources and off-the-shelf strategies. These opportunities will be analyzed in the light of results from ongoing clinical studies involving T-cell progenitors.

Published
2022
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4. Signature for Pain Recovery IN Teens (SPRINT): protocol for a multisite prospective signature study in chronic musculoskeletal pain

Author

Fiona Campbell, Jennifer Stinson, Sara E Williams, Christopher D King, Laura Simons, Massieh Moayedi, Robert C Coghill, Martin S Angst, Nima Aghaeepour, Brice Gaudilliere, Marina López-Solà, Marie-Eve Hoeppli, Emma Biggs, Ed Ganio, Kenneth R Goldschneider, Danielle Ruskin, Elliot J Krane, Suellen Walker, Gillian Rush, and Marissa Heirich

Subjects
Medicine
Published
2022
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5. Evidence of Chronic Complement Activation in Asymptomatic Pediatric Brain Injury Patients: A Pilot Study

Author

Scott A. Holmes, Joud Mar’i, Jordan Lemme, Anne Margarette Maallo, Alyssa Lebel, Laura Simons, Michael J. O’Brien, David Zurakowski, Rami Burnstein, and David Borsook

Subjects
inflammation, brain injury, pediatrics, Pediatrics, RJ1-570
Abstract

Physical insult from a mild Traumatic Brain Injury (mTBI) leads to changes in blood flow in the brain and measurable changes in white matter, suggesting a physiological basis for chronic symptom presentation. Post-traumatic headache (PTH) is frequently reported by persons after an mTBI that may persist beyond the acute period (>3 months). It remains unclear whether ongoing inflammation may contribute to the clinical trajectory of PTH. We recruited a cohort of pediatric subjects with PTH who had an acute or a persistent clinical trajectory, each around the 3-month post-injury time point, as well as a group of age and sex-matched healthy controls. We collected salivary markers of mRNA expression as well as brain imaging and psychological testing. The persistent PTH group showed the highest levels of psychological burden and pain symptom reporting. Our data suggest that the acute and persistent PTH cohort had elevated levels of complement factors relative to healthy controls. The greatest change in mRNA expression was found in the acute-PTH cohort wherein the complement cascade and markers of vascular health showed a prominent role for C1Q in PTH pathophysiology. These findings (1) underscore a prolonged engagement of what is normally a healthy response and (2) show that a persistent PTH symptom trajectory may parallel a poorly regulated inflammatory response.

Published
2022
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6. Concise Review: Boosting T‐Cell Reconstitution Following Allogeneic Transplantation—Current Concepts and Future Perspectives

Author

Laura Simons, Marina Cavazzana, and Isabelle André

Subjects
Cellular therapy, Hematopoietic stem cell transplantation, Immunodeficiency, Immune reconstitution, T‐cell, Thymus, Medicine (General), R5-920, Cytology, QH573-671
Abstract

Abstract Allogeneic hematopoietic stem cell transplantation (HSCT) is the treatment of choice for a large number of malignant and nonmalignant (inherited) diseases of the hematopoietic system. Nevertheless, non‐HLA identical transplantations are complicated by a severe T‐cell immunodeficiency associated with a high rate of infection, relapse and graft‐versus‐host disease. Initial recovery of T‐cell immunity following HSCT relies on peripheral expansion of memory T cells mostly driven by cytokines. The reconstitution of a diverse, self‐tolerant, and naive T‐cell repertoire, however, may take up to 2 years and crucially relies on the interaction of T‐cell progenitors with the host thymic epithelium, which may be altered by GvHD, age or transplant‐related toxicities. In this review, we summarize current concepts to stimulate reconstitution of a peripheral and polyclonal T‐cell compartment following allogeneic transplantation such as graft manipulation (i.e., T‐cell depletion), transfusion of ex vivo manipulated donor T cells or the exogenous administration of cytokines and growth factors to stimulate host‐thymopoiesis with emphasis on approaches which have led to clinical trials. Particular attention will be given to the development of cellular therapies such as the ex vivo generation of T‐cell precursors to fasten generation of a polyclonal and functional host‐derived T‐cell repertoire. Having been tested so far only in preclinical mouse models, clinical studies are now on the way to validate the efficacy of such T‐cell progenitors in enhancing immune reconstitution following HSCT in various clinical settings. Stem Cells Translational Medicine 2019;00:1–8

Published
2019
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7. Subclinical post-traumatic stress symptomology and brain structure in youth with chronic headaches

Author

Jillian Vinall Miller, Quinn Andre, Inge Timmers, Laura Simons, Nivez Rasic, Catherine Lebel, and Melanie Noel

Subjects
Brain, Headache, Pain, PTSD, Post-traumatic stress symptoms, Trauma, Computer applications to medicine. Medical informatics, R858-859.7, Neurology. Diseases of the nervous system, RC346-429
Abstract

Background/aims: Post-traumatic stress symptoms (PTSS) and chronic pain often co-occur at high rates in youth. PTSS may alter brain structure thereby contributing to headache chronicity. This study examined whether PTSS and altered limbic circuitry were associated with headache frequency in youth. Methods: Thirty youth aged 10–18 years with chronic headaches and 30 age- and sex-matched controls underwent a 3T MRI scan. Volumes of the hippocampus and amygdala were obtained from T1-weighted images. Mean fractional anisotropy (FA, an index of white matter structure) axial and radial diffusivity values of the cingulum and uncinate fasciculus were extracted from diffusion-weighted images. Youth reported on their headaches daily, for one-month, and self-reported pubertal status, emotion regulation, adverse childhood experiences (ACEs) and PTSS using validated measures. Volumes of the hippocampus and amygdala and diffusivity values of the cingulum and uncinate were compared between patients and controls. Hierarchical linear regressions were used to examine the association between PTSS, subcortical volumes and/or diffusivity values and headache frequency. Results: Mean FA values of the cingulum were higher in patients compared to controls (P = 0.02, Cohen’s d = 0.69). Greater PTSS (P = 0.04), smaller amygdala volumes (P = 0.01) and lower FA of the cingulum (P = 0.04) were associated with greater headache frequency, after accounting for age, puberty, pain duration, emotion regulation, and ACEs (Adjusted R2 ≥ 0.15). Headache frequency was associated with increases in radial diffusivity (P = 0.002, Adjusted R2 = 0.59), as opposed to axial diffusivity (n.s.). Conclusions: PTSS, smaller amygdalar volume, and poorer cingulum structural connectivity were associated with headache frequency in youth, and may underlie headache chronicity.

Published
2021
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8. Humoral Responses and Chronic GVHD Exacerbation after COVID-19 Vaccination Post Allogeneic Stem Cell Transplantation

Author

Caroline Pabst, Louise Benning, Nora Liebers, Maike Janssen, Leandra Caille, Claudius Speer, Lixiazi He, Maria-Luisa Schubert, Laura Simons, Ute Hegenbart, Stefan Schönland, Aleksandar Radujkovic, Michael Schmitt, Paul Schnitzler, Carsten Müller-Tidow, Sascha Dietrich, Peter Dreger, and Thomas Luft

Subjects
allogeneic stem cell transplantation, COVID-19, cGVHD, humoral responses, immunosuppression, Medicine
Abstract

The COVID-19 pandemic threatens patients with a compromised immune and endothelial system, including patients who underwent allogeneic stem cell transplantation (alloSCT). Thus, there is an unmet need for optimizing vaccination management in this high-risk cohort. Here, we monitored antibodies against SARS-CoV-2 spike protein (anti-S1) in 167 vaccinated alloSCT patients. Humoral immune responses were detectable in 81% of patients after two vaccinations with either mRNA-, vector-based, or heterologous regimens. Age, B-cell counts, time interval from vaccination, and the type of vaccine determined antibody titres in patients without systemic immunosuppression (sIS). Similar to a healthy control cohort, mRNA vaccine-based regimens induced higher titres than vector-based vaccines. Patients on two or more immunosuppressants rarely developed immunity. In contrast, 62% and 45% of patients without or on only one immunosuppressant, respectively, showed a strong humoral vaccination response (titre > 100). Exacerbation of cGVHD upon vaccination was observed in 6% of all patients and in 22% of patients receiving immunosuppression for cGVHD. cGVHD exacerbation and low antibody titres were both associated with higher angiopoietin-2 (ANG2) serum levels. In conclusion, mRNA-based vaccines elicit strong humoral responses in alloSCT patients in the absence of double sIS. Biomarkers such as ANG2 might help with weighing cGVHD risk versus beneficial responses.

Published
2022
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9. Isolating Brain Regions Implicated in the Affective Components of Neuropathic Pain

Author

Natalia I. Lopez, Scott Holmes, Nadia Barakat, Alyssa Lebel, Laura Simons, and David Borsook

Subjects
Medicine (General), R5-920, Therapeutics. Pharmacology, RM1-950
Abstract

Introduction/Aim: The psychosocial factors implicated in neuropathic pain are profound. Pain symptoms can lead to prolonged manifestations of affective and other psychological disorders (e.g., negative mood; avoidance behaviors). In this investigation, we sought to (1) evaluate the extent to which psychological factors are elevated in an acute neuropathic pain cohort, and (2) evaluate brain changes implicated in the affective components of acute neuropathic pain. Methods: Participants included ankle sprain patients with acute neuropathic pain (n = 24, Age = 16.1 years, SD = 4.1), and age- and gender-matched healthy controls (n = 12, Age = 16.1, SD = 2.95). Participants were evaluated using self-report questionnaires of psychological and pain-related symptoms: Multidimensional Anxiety Scale for Children-MASC; Children’s Depression Inventory-CDI; Fear of Pain Questionnaire-FOPQ, Functional Disability Inventory-FDI, Pediatric Pain Screening Tool-PPST, and Pain Catastrophizing Scale-PCS. Cortical thickness and sub-cortical volumes were extracted from Freesurfer. Results: The neuropathic pain cohort exhibited elevated scores on the CDI, FOPQ, FDI, PPST, and PCS relative to controls (p

Published
2019
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10. Signature for Pain Recovery IN Teens (SPRINT): protocol for a multisite prospective signature study in chronic musculoskeletal pain

Author

Laura Simons, Massieh Moayedi, Robert C Coghill, Jennifer Stinson, Martin S Angst, Nima Aghaeepour, Brice Gaudilliere, Christopher D King, Marina López-Solà, Marie-Eve Hoeppli, Emma Biggs, Ed Ganio, Sara E Williams, Kenneth R Goldschneider, Fiona Campbell, Danielle Ruskin, Elliot J Krane, Suellen Walker, Gillian Rush, and Marissa Heirich

Subjects
Adolescent, National Institutes of Health (U.S.), Musculoskeletal Pain, Humans, Multicenter Studies as Topic, Pain Management, General Medicine, Prospective Studies, Chronic Pain, United States
Abstract

IntroductionCurrent treatments for chronic musculoskeletal (MSK) pain are suboptimal. Discovery of robust prognostic markers separating patients who recover from patients with persistent pain and disability is critical for developing patient-specific treatment strategies and conceiving novel approaches that benefit all patients. Given that chronic pain is a biopsychosocial process, this study aims to discover and validate a robust prognostic signature that measures across multiple dimensions in the same adolescent patient cohort with a computational analysis pipeline. This will facilitate risk stratification in adolescent patients with chronic MSK pain and more resourceful allocation of patients to costly and potentially burdensome multidisciplinary pain treatment approaches.Methods and analysisHere we describe a multi-institutional effort to collect, curate and analyse a high dimensional data set including epidemiological, psychometric, quantitative sensory, brain imaging and biological information collected over the course of 12 months. The aim of this effort is to derive a multivariate model with strong prognostic power regarding the clinical course of adolescent MSK pain and function.Ethics and disseminationThe study complies with the National Institutes of Health policy on the use of a single internal review board (sIRB) for multisite research, with Cincinnati Children’s Hospital Medical Center Review Board as the reviewing IRB. Stanford’s IRB is a relying IRB within the sIRB. As foreign institutions, the University of Toronto and The Hospital for Sick Children (SickKids) are overseen by their respective ethics boards. All participants provide signed informed consent. We are committed to open-access publication, so that patients, clinicians and scientists have access to the study data and the signature(s) derived. After findings are published, we will upload a limited data set for sharing with other investigators on applicable repositories.Trial registration numberNCT04285112.

Published
2022

11. Considering Precision and Utility When we Talk About Pain. Comment on Cohen et al

Author

Graham L. Moseley, Neil Pearson, Roland Reezigt, Victoria J. Madden, Mark R. Hutchinson, Martin Dunbar, Anneke J. Beetsma, Hayley B. Leake, Pete Moore, Laura Simons, Lauren Heathcote, Cormac Ryan, Carolyn Berryman, Amelia K. Mardon, Benedict M. Wand, Moseley, Graham L, Pearson, Neil, Reezigt, Roland, Madden, Victoria J, Hutchinson, Mark R, Dunbar, Martin, Beetsma, Anneke J, Leake, Hayley B, Moore, Pete, Simons, Laura, Heathcote, Lauren, Ryan, Cormac, Berryman, Carolyn, Mardon, Amelia K, Wand, Benedict M, Neuromechanics, AMS - Rehabilitation & Development, and Healthy Ageing, Allied Health Care and Nursing

Subjects
pain medicine, pijn, Anesthesiology and Pain Medicine, talking, Neurology, Humans, Pain, pain, Neurology (clinical), praten, comment, pain treatment, commentaar
Abstract

We applaud many of the sentiments put forward by Cohen et al in their critique of language and logic in pain medicine. 8 Pleas to avoid conflation between nociception and pain are not new - “The mislabelling of nociceptors as pain fibres was not an elegant simplification but a most unfortunate trivialisation of pain”29 ; “.. we don't actually have ‘pain receptors’, or ‘pain nerves’ or ‘pain pathways’ or ‘pain centres.’”4 We are among those who see such conflation as contrasting with contemporary understandings of ‘how pain works’ and undermining evidence-based treatment approaches.

Published
2022

15. Ex vivo generated human T-lymphoid progenitors as a tool to accelerate immune reconstitution after partially HLA compatible hematopoietic stem cell transplantation or after gene therapy

Author

Isabelle, André, Laura, Simons, Kuiying, Ma, Ranjita Devi, Moirangthem, Jean-Sébastien, Diana, Elisa, Magrin, Chloé, Couzin, Alessandra, Magnani, and Marina, Cavazzana

Subjects
Mice, Immune Reconstitution, Transplantation Conditioning, T-Lymphocytes, Hematopoietic Stem Cell Transplantation, Animals, Humans, Genetic Therapy
Abstract

Prolonged T-cell immunodeficiency following HLA- incompatible hematopoietic stem cell transplantation (HSCT) represents a major obstacle hampering the more widespread use of this approach. Strategies to fasten T-cell reconstitution in this setting are highly warranted as opportunistic infections and an increased risk of relapse account for high rates of morbidity and mortality especially during early month following this type of HSCT. We have implemented a feeder free cell system based on the use of the notch ligand DL4 and cytokines allowing for the in vitro differentiation of human T-Lymphoid Progenitor cells (HTLPs) from various sources of CD34+ hematopoietic stem and precursor cells (HSPCs). Co- transplantion of human T-lymphoid progenitors (HTLPs) and non- manipulated HSPCs into immunodeficient mice successfully accelerated the reconstitution of a polyclonal T-cell repertoire. This review summarizes preclinical data on the use of T-cell progenitors for treatment of post- transplantation immunodeficiency and gives insights into the development of GMP based protocols for potential clinical applications including gene therapy approaches. Future clinical trials implementing this protocol will aim at the acceleration of immune reconstitution in different clinical settings such as SCID and leukemia patients undergoing allogeneic transplantation. Apart from pure cell-therapy approaches, the combination of DL-4 culture with gene transduction protocols will open new perspectives in terms of gene therapy applications for primary immunodeficiencies.

Published
2019

17. Generation of adult human T-cell progenitors for immunotherapeutic applications

Author

Laura, Simons, Kuiying, Ma, Corinne, de Chappedelaine, Ranjita Devi, Moiranghtem, Elodie, Elkaim, Juliette, Olivré, Sandrine, Susini, Kevin, Appourchaux, Christian, Reimann, Hanem, Sadek, Olivier, Pellé, Nicolas, Cagnard, Elisa, Magrin, Chantal, Lagresle-Peyrou, Tom, Taghon, Antonio, Rausell, Marina, Cavazzana, and Isabelle, André-Schmutz

Subjects
Mice, T-Lymphocytes, Receptors, Antigen, T-Cell, Animals, Humans, Cell Differentiation, Immunotherapy, Thymus Gland, Cells, Cultured, Article
Published
2017

18. Treatment of Post- HSCT Immunodeficiency By Infusion of Ex Vivo- Generated T Cell Precursors from Adult and Cord Blood Hematopoietic Stem and Progenitor Cells

Author

Kuiying Ma, Elodie Elkaim, Fabien Touzot, Laura Simons, Corinne De La Chappedelaine, Sandrine Susini, Christian Reimann, Marina Cavazzana, and Isabelle André-Schmutz

Subjects
medicine.medical_treatment, T cell, Immunology, Notch signaling pathway, Cell Biology, Hematology, Hematopoietic stem cell transplantation, Biology, Acquired immune system, Biochemistry, Haematopoiesis, medicine.anatomical_structure, T cell differentiation, Cancer research, medicine, Cytotoxic T cell, Progenitor cell
Abstract

Non-HLA identical hematopoietic stem cell transplantation (HSCT) provides a corrective therapy for most life-threatening primary immunodeficiencies (PID) and some malignant hemopathies. Despite advances made, severe complications following the treatment such as the prolonged persistence of T cell immunodeficiency still limit the use of this partially incompatible HSCT. After HSCT, the reconstitution of a functional T cell compartment relies on the availability of T cell precursors to rapidly seed the thymus and differentiate into mature T cells. We have previously demonstrated that an in vitro culture system based on the use of a modified Delta-like-4 (DLL4) Notch ligand and T cell cytokines allows for the effective generation of human T cell precursors from cord blood within 7 days. Moreover, once injected into NOD/SCID/gcko mice, T cell precursors generated in this system were able to colonize the thymus and generate a diversified and functional T-cell compartment. Here, we aimed at testing the capacity of adult HSPCs in this reconstitution system. We found that, like their CB- derived counterparts, T cell precursors generated from adult HPSCs phenotypically resembled thymic CD34+CD7+ cells with high in vitro T-cell differentiation potential. Interestingly, the peak of T cell progenitors for adult HSPCs occurred around day 3, compared to day 7 in CB. At this timepoint, T cell precursors derived from adult HSPC already expressed all critical genes for T cell lineage development, as well as the major chemokine receptors implicated in thymus homing. The introduction of retronectin further improved differentiation and proliferation of T cell progenitors from both HPSC sources in our in vitro system. Comparative molecular analysis of adult- and CB- derived progenitors suggested, that differential requirements for Notch receptor/ligand interactions may explain the differences in kinetics observed during the culture of the two types of HSPC. It remains to be further evaluated, whether targeted modifications of the Notch signaling pathway can improve the outcome of this in vitro T cell differentiation system for adult HPSCs. Overall our results suggest that adult HSPCs, like their CB- derived counterparts, provide an effective source of in vitro cultured T cell progenitors harboring all the necessary requirements for the in vivo -reconstitution of a functional T cell compartment. This is particularly important in the context of future clinical applications in HSCT where adult HSPCs are more available and more frequently used than CB HSPCs. Based on our results, we propose that upon injection into a patient, DLL4- cultured T cell precursors from both HSPC sources could significantly accelerate the reconstitution of the adaptive immune system after a partially HLA-incompatible HSCT. Currently, we are translating these results into a phase I clinical trial including adult and pediatric patients transplanted for malignant hemopathies or PIDs requiring an allogeneic HSCT from a HLA-partially mismatched donors. Disclosures No relevant conflicts of interest to declare.

Published
2015

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