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2,076 results on '"Boraschi A"'

52. Towards bio-compatible magnetic nanoparticles: Immune-related effects, in-vitro internalization, and in-vivo bio-distribution of zwitterionic ferrite nanoparticles with unexpected renal clearance

Author

Ferretti, Anna M., Usseglio, Sandro, Mondini, Sara, Drago, Carmelo, La Mattina, Rosa, Chini, Bice, Verderio, Claudia, Leonzino, Marianna, Cagnoli, Cinzia, Joshi, Pooja, Boraschi, Diana, Italiani, Paola, Li, Yang, Swartzwelter, Benjamin J., Sironi, Luigi, Gelosa, Paolo, Castiglioni, Laura, Guerrini, Uliano, and Ponti, Alessandro

Published
2021
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53. Dynamic and Multi-phase Contrast-Enhanced CT Scan

Author

Boraschi, Piero, Tarantini, Gaia, Pacciardi, Federica, Donati, Francescamaria, Radu-Ionita, Florentina, editor, Pyrsopoulos, Nikolaos T., editor, Jinga, Mariana, editor, Tintoiu, Ion C., editor, Sun, Zhonghua, editor, and Bontas, Ecaterina, editor

Published
2020
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54. Computed Tomography and Magnetic Resonance Enterography: From Protocols to Diagnosis.

Author

Maino, Cesare, Mariani, Ilaria, Drago, Silvia Girolama, Franco, Paolo Niccolò, Giandola, Teresa Paola, Donati, Francescamaria, Boraschi, Piero, and Ippolito, Davide

Subjects
INFLAMMATORY bowel diseases, CROHN'S disease, COMPUTED tomography, MAGNETIC resonance, IONIZING radiation
Abstract

Both Magnetic Resonance Enterography (MRE) and Computed Tomography Enterography (CTE) are crucial imaging modalities in the diagnosis and treatment of inflammatory bowel disease (IBD). CTE is often used in acute scenarios, such as when complications (such as abscesses, perforations, or bowel obstructions) are suspected. It can also help determine the degree and extent of pathological processes. Although CTE is rapid, generally accessible, and offers precise images that are useful in emergencies, it does expose patients to ionizing radiation. Nevertheless, MRE is very useful in assessing perianal illness and the small intestine, and it is frequently used in patients who need repeated follow-ups or are pregnant to minimize radiation exposure. Moreover, MRE can demonstrate oedema, fistulas, abscesses, and the thickening of the bowel wall. In addition, MRE offers superior soft tissue contrast resolution without ionizing radiation, which helps identify complications such as fistulas and abscesses. With their respective advantages and disadvantages, both approaches play essential roles in assessing IBD. The primary goal of this review is to provide an overview of the technical specifications, benefits, drawbacks, and imaging findings of CTE and MRE. [ABSTRACT FROM AUTHOR]

Published
2024
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55. De Novo Kaposi Sarcoma in an HIV‐Negative Liver Transplant Recipient With Ulcerative Colitis and Primary Sclerosing Cholangitis.

Author

Ramakrishnan, Pavithra, Amin, Khalid, Gaertner, Wolfgang, Aby, Elizabeth S., and Boraschi, Piero

Subjects
INFLAMMATORY bowel diseases, ULCERATIVE colitis, KAPOSI'S sarcoma, LIVER transplantation, TRANSPLANTATION of organs, tissues, etc.
Abstract

De novo or viral reactivation cancers are a major cause of morbidity and mortality in the solid organ transplant (SOT) population. Primary sclerosing cholangitis (PSC) is an aggressive disease which can lead to cholestatic liver damage and cirrhosis. PSC often cooccurs with inflammatory bowel disease (IBD). Here, we describe the case of a 28‐year‐old male with PSC along with poorly controlled IBD who underwent a liver transplant and developed colonic Kaposi sarcoma (KS). Our case highlights the importance of adequate pretransplant screening for endemic viruses, high clinical suspicion for KS in the setting of difficult‐to‐control colitis, and early multidisciplinary involvement. [ABSTRACT FROM AUTHOR]

Published
2024
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56. Safety of Zein Nanoparticles on Human Innate Immunity and Inflammation.

Author

Corteggio, Annunziata, Heinzl, Tommaso, Boraschi, Diana, Voci, Silvia, Gagliardi, Agnese, Cosco, Donato, and Italiani, Paola

Subjects
NATURAL immunity, BIOPOLYMERS, IMMUNE system, TISSUE engineering, INFLAMMATION
Abstract

In recent years, natural polymers have attracted great interest for the development of release systems for vaccine formulations and drug delivery. Zein, a hydrophobic proline-rich protein mixture obtained from maize, is one of the most widely used polymers, very promising for applications in tissue engineering and the parenteral delivery of bioactive agents. Still, we have a limited understanding of the interaction between zein particles and the human immune system, in particular innate immunity/inflammation, which is the first line of defense of our body. Assessing the immune safety of nanoparticles is of central importance for ensuring that nano-formulations for medical use do not cause adverse effects on human health. Here, we evaluated the capacity of zein nanoparticles to induce/modulate the innate/inflammatory response, the development of innate memory, and the macrophage polarization by using reliable in vitro systems based on human primary monocytes and monocyte-derived macrophages. We observed that zein nanoparticles do not influence any of these aspects of the innate immune/inflammatory response, suggesting its safety and its potential efficiency as a nanocarrier for drug or antigen delivery. [ABSTRACT FROM AUTHOR]

Published
2024
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57. Scoping Review with Topic Modeling on the Diagnostic Criteria for Degenerative Cervical Myelopathy.

Author

Matsoukas, Stavros, Zipser, Carl Moritz, Zipser-Mohammadzada, Freschta, Kheram, Najmeh, Boraschi, Andrea, Jiang, Zhilin, Tetreault, Lindsay, Fehlings, Michael G., Davies, Benjamin M., and Margetis, Konstantinos

Subjects
MAGNETIC resonance imaging, INTERVERTEBRAL disk, SPINAL cord injuries, DIAGNOSTIC imaging, DATABASES
Abstract

Study Design: This study is a scoping review. Objective: There is a broad variability in the definition of degenerative cervical myelopathy (DCM) and no standardized set of diagnostic criteria to date. Methods: We interrogated the Myelopathy.org database, a hand-indexed database of primary clinical studies conducted exclusively on DCM in humans between 2005-2021. The DCM inclusion criteria used in these studies were inputted into 3 topic modeling algorithms: Hierarchical Dirichlet Process (HDP), Latent Dirichlet Allocation (LDA), and BERtopic. The emerging topics were subjected to manual labeling and interpretation. Results: Of 1676 reports, 120 papers (7.16%) had well-defined inclusion criteria and were subjected to topic modeling. Four topics emerged from the HDP model: disturbance from extremity weakness and motor signs; fine-motor and sensory disturbance of upper extremity; a combination of imaging and clinical findings is required for the diagnosis; and "reinforcing" (or modifying) factors that can aid in the diagnosis in borderline cases. The LDA model showed the following topics: disturbance to the patient is required for the diagnosis; reinforcing factors can aid in the diagnosis in borderline cases; clinical findings from the extremities; and a combination of imaging and clinical findings is required for the diagnosis. BERTopic identified the following topics: imaging abnormality, typical clinical features, range of objective criteria, and presence of clinical findings. Conclusions: This review provides quantifiable data that only a minority of past studies in DCM provided meaningful inclusion criteria. The items and patterns found here are very useful for the development of diagnostic criteria for DCM. [ABSTRACT FROM AUTHOR]

Published
2024
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58. Cerebrospinal fluid pressure dynamics reveal signs of effective spinal canal narrowing in ambiguous spine conditions

Author

Najmeh Kheram, Nikolai Pfender, Andrea Boraschi, Mazda Farshad, Vartan Kurtcuoglu, Armin Curt, Martin Schubert, and Carl M. Zipser

Subjects
degenerative cervical myelopathy, spinal cord compression, cerebrospinal fluid pressure, craniospinal compliance, bedside diagnostics, spinal canal, Neurology. Diseases of the nervous system, RC346-429
Abstract

Spinal canal narrowing with consecutive spinal cord compression is considered a key mechanism in degenerative cervical myelopathy (DCM). DCM is a common spine condition associated with progressive neurological disability, and timely decompressive surgery is recommended. However, the clinical and radiological diagnostic workup is often ambiguous, challenging confident proactive treatment recommendations. Cerebrospinal fluid pressure dynamics (CSFP) are altered by spinal canal narrowing. Therefore, we aim to explore the potential value of bedside CSFP assessments for qualitative and quantitative assessment of spinal canal narrowing in DCM. In this prospective case series, seven patients with DCM underwent bedside lumbar puncture with measurement of CSFP dynamics and routine CSF analysis (NCT02170155). The patients were enrolled when standard diagnostic algorithms did not permit a clear treatment decision. Measurements include baseline CSFP, cardiac-driven CSFP peak-to-trough amplitude (CSFPp), and the Queckenstedt's test (firm pressure on jugular veins) in neutral and reclined head position. From the Queckenstedt's test, proxies for craniospinal elastance (i.e., relative pulse pressure coefficient; RPPC-Q) were calculated analogously to infusion testing. CSFP metrics were deemed suspicious of canal narrowing when numbers were lower than the minimum value from a previously tested elderly spine-healthy cohort (N = 14). Mean age was 56 ± 13 years (range, 38–75; 2F); symptom severity was mostly mild to moderate (mean mJOA, 13.5 ± 2.6; range, 9–17). All the patients showed some extent of cervical stenosis in the MRI of unclear significance (5/7 following decompressive cervical spine surgery with an adjacent level or residual stenosis). Baseline CSFP was normal except for one patient (range, 4.7–17.4 mmHg). Normal values were found for CSFPp (0.4–1.3 mmHg) and the Queckenstedt's test in normal head positioning (9.-25.3 mmHg). During reclination, the Queckenstedt's test significantly decreased in one, and CSFPp in another case (>50% compared to normal position). RPPC-Q (0.07–0.19) aligned with lower values from spine-healthy (0.10–0.44). Routine CSF examinations showed mild total protein elevation (mean, 522 ± 108 mg/ml) without further evidence for the disturbed blood brain barrier. Intrathecal CSFP measurements allow discerning disturbed from normal CSFP dynamics in this population. Prospective longitudinal studies should further evaluate the diagnostic utility of CSFP assessments in DCM.

Published
2022
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59. The SARS-CoV-2 Nucleoprotein Induces Innate Memory in Human Monocytes

Author

Patricia Urbán, Paola Italiani, Diana Boraschi, and Sabrina Gioria

Subjects
SARS-CoV-2, nucleoprotein, innate immunity, innate memory, monocytes, cytokines, Immunologic diseases. Allergy, RC581-607
Abstract

The interaction of SARS-CoV-2 with the human immune system is at the basis of the positive or negative outcome of the infection. Monocytes and macrophages, which are major innate immune/inflammatory effector cells, are not directly infected by SARS-CoV-2, however they can react to the virus and mount a strong reaction. Whether this first interaction and reaction may bias innate reactivity to re-challenge, a phenomenon known as innate memory, is currently unexplored and may be part of the long-term sequelae of COVID-19. Here, we have tested the capacity of SARS-CoV-2 and some of its proteins to induce innate memory in human monocytes in vitro. Our preliminary results show that the Spike protein subunits S1 and S2 and the entire heat-inactivated virus have no substantial effect. Conversely, monocytes pre-exposed to the nucleocapsid N protein react to subsequent viral or bacterial challenges with an increased production of anti-inflammatory IL-1Ra, a response profile suggesting a milder response to new infections.

Published
2022
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63. What Is IL-1 for? The Functions of Interleukin-1 Across Evolution

Author

Diana Boraschi

Subjects
interleukin-1, inflammation, innate immunity, adaptive immunity, evolution, Immunologic diseases. Allergy, RC581-607
Abstract

Interleukin-1 is a cytokine with potent inflammatory and immune-amplifying effects, mainly produced by macrophages during defensive reactions. In mammals, IL-1 is a superfamily of eleven structurally similar proteins, all involved in inflammation or its control, which mainly act through binding to specific receptors on the plasma membrane of target cells. IL-1 receptors are also a family of ten structurally similar transmembrane proteins that assemble in heterocomplexes. In addition to their innate immune/inflammatory effects, the physiological role of IL-1 family cytokines seems to be linked to the development of adaptive immunity in vertebrates. We will discuss why IL-1 developed in vertebrates and what is its physiological role, as a basis for understanding when and how it can be involved in the initiation and establishment of pathologies.

Published
2022
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64. Data on body mass, glucose tolerance and bone phenotype of mice with osteogenesis imperfecta on long-term low-fat and high-fat diets

Author

Josephine T. Tauer, Iris Boraschi-Diaz, and Svetlana V. Komarova

Subjects
Animal model, Glucose intolerance, Osteogenesis imperfecta, Body mass, Bone phenotype, High-fat diet, Computer applications to medicine. Medical informatics, R858-859.7, Science (General), Q1-390
Abstract

Male and female mice with a dominant severe bone fragility disorder, osteogenesis imperfecta, and their wild-type littermates (FVB background) were challenged with a long-term (26 weeks) high-fat diet to evaluate the development of obesity and glucose intolerance. Here we present data for the measurements of body mass, the outcome of glucose tolerance tests during the long-term diet, as well as organ weights and bone phenotype at the end of the study. Interpretation of the data and further in-depth analysis can be found in the article “Male but not female mice with severe osteogenesis imperfecta are partially protected from high-fat diet-induced obesity.” by Tauer JT, Boraschi-Diaz I, Al Rifai O, Rauch F, Ferron M, Komarova SV, published in Molecular Genetics and Metabolism. The data presented here demonstrate individual mouse outcomes of long-term diet experiments that can be reused for comparative studies of diet-induced changes in wild-type mice on different backgrounds and different mouse models of osteogenesis imperfecta.

Published
2022
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65. Helicobacter pylori Infection of Primary Human Monocytes Boosts Subsequent Immune Responses to LPS

Author

Tobias Frauenlob, Theresa Neuper, Muamera Mehinagic, Hieu-Hoa Dang, Diana Boraschi, and Jutta Horejs-Hoeck

Subjects
monocytes, innate memory, innate immunity, Helicobacter pylori, chronic gastric inflammation, primary myeloid immune cells, Immunologic diseases. Allergy, RC581-607
Abstract

Infection with Helicobacter pylori (H. pylori) affects almost half of the world’s population and is a major cause of stomach cancer. Although immune cells react strongly to this gastric bacterium, H. pylori is still one of the rare pathogens that can evade elimination by the host and cause chronic inflammation. In the present study, we characterized the inflammatory response of primary human monocytes to repeated H. pylori infection and their responsiveness to an ensuing bacterial stimulus. We show that, although repeated stimulations with H. pylori do not result in an enhanced response, H. pylori-primed monocytes are hyper-responsive to an Escherichia coli-lipopolysaccharide (LPS) stimulation that takes place shortly after infection. This hyper-responsiveness to bacterial stimuli is observed upon infection with viable H. pylori only, while heat-killed H. pylori fails to boost both cytokine secretion and STAT activation in response to LPS. When the secondary challenge occurs several days after the primary infection with live bacteria, H. pylori-infected monocytes lose their hyper-responsiveness. The observation that H. pylori makes primary human monocytes more susceptible to subsequent/overlapping stimuli provides an important basis to better understand how H. pylori can maintain chronic inflammation and thus contribute to gastric cancer progression.

Published
2022
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66. Insights Into the Low Rate of In-Pump Thrombosis With the HeartMate 3: Does the Artificial Pulse Improve Washout?

Author

Peng Fang, Jianjun Du, Andrea Boraschi, Silvia Bozzi, Alberto Redaelli, Marianne Schmid Daners, Vartan Kurtcuoglu, Filippo Consolo, and Diane de Zélicourt

Subjects
left ventricular assist device (LVAD), computational fluid dynamics (CFD), HeartMate 3 (HM3), pump thrombosis, washout, rotational speed modulation, Diseases of the circulatory (Cardiovascular) system, RC666-701
Abstract

While earlier studies reported no relevant effect of the HeartMate 3 (HM3) artificial pulse (AP) on bulk pump washout, its effect on regions with prolonged residence times remains unexplored. Using numerical simulations, we compared pump washout in the HM3 with and without AP with a focus on the clearance of the last 5% of the pump volume. Results were examined in terms of flush-volume (Vf, number of times the pump was flushed with new blood) to probe the effect of the AP independent of changing flow rate. Irrespective of the flow condition, the HM3 washout scaled linearly with flush volume up to 70% washout and slowed down for the last 30%. Flush volumes needed to washout 95% of the pump were comparable with and without the AP (1.3–1.4 Vf), while 99% washout required 2.1–2.2 Vf with the AP vs. 2.5 Vf without the AP. The AP enhanced washout of the bend relief and near-wall regions. It also transiently shifted or eliminated stagnation regions and led to rapid wall shear stress fluctuations below the rotor and in the secondary flow path. Our results suggest potential benefits of the AP for clearance of fluid regions that might elicit in-pump thrombosis and provide possible mechanistic rationale behind clinical data showing very low rate of in-pump thrombosis with the HM3. Further optimization of the AP sequence is warranted to balance washout efficacy while limiting blood damage.

Published
2022
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68. Altered maternal metabolism during mild gestational hyperglycemia as a predictor of adverse perinatal outcomes: A comprehensive analysis

Author

Rudge, M.V., Calderon, I.M.P., Barbosa, A.P., Abbade, J., Costa, R.A.A., Magalhães, C.G., Salvadori, D.F., Gelaleti, R., Hallur, R.L.S., Marcondes, J.P., Floriano, J.F., Reyes, D.R.A., Sobrevia, L., Prudêncio, C.B., Pículo, F., Marini, G., Vesentini, G., Morceli, G., Negrato, C.A., Prazeres, H.D., Molina, S., Arantes, M., Cavassini, A.C., Kerche, L., De Luca, A.K.C., Corrêa-Silva, S., Bevilacqua, E., Moreli, J.B., Pietro, L., Daher, S., Fabio, S., Honorio-França, A.C., Queiroz, A.A., Hara, C.C.P., Boraschi, C.A.L., Pauletti, T.A.V.L., Jovanovic, L., Dias, A., Atallah, A.N., Ramos, M.D., Brasil, M.A.M., Rudge, C.V.C., Tristão, A., Del Nero, U., Mendonça, M., Witkin, S.S., Sartorão Filho, C.I., Nunes, S.K., Pinheiro, F.A., Quiroz, S.V., Pascon, T., Caldeirão, T.D., Oliveira, A.P., Nicolosi, B.F., Bolognani, C.V., Fagundes, D.L.G., Llanos, I.C.F., Vernini, J.M., Reis, L.B.S.M., Sirimarco, M.P., Basso, N.M., Maquesim, N.A.Q., Silva, S.A.L.C., Silva, S.C., Scudeller, T.T., Ayach, W., Almeida, A.P.M., Nicolosi, B.F.C.A., Lima, C.P., Luminoso, D., Vasconcellos, F.C., Ferraz, G.A.R., Migiolaro, H., Camargo, L.P., Macedo, M.L.S., Rodrigues, M.R.K., Anézio, P.H.O., Rudge, Marilza Vieira Cunha, Barbosa, Angélica Mercia Pascon, Sobrevia, Luis, Gelaleti, Rafael Bottaro, Hallur, Raghavendra Lakshmana Shetty, Marcondes, João Paulo Castro, Salvadori, Daisy Maria Fávero, Prudêncio, Caroline Baldini, Magalhães, Claudia Garcia, Costa, Roberto, Abbade, Joelcio Francisco, Corrente, José Eduardo, and Calderon, Iracema de Mattos Paranhos

Published
2020
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71. Influence of age on the relation between body position and noninvasively acquired intracranial pulse waves

Author

Boraschi, Andrea; https://orcid.org/0000-0002-2908-5234, Hafner, Matthias, Spiegelberg, Andreas; https://orcid.org/0000-0002-3812-3191, Kurtcuoglu, Vartan; https://orcid.org/0000-0003-2665-0995, Boraschi, Andrea; https://orcid.org/0000-0002-2908-5234, Hafner, Matthias, Spiegelberg, Andreas; https://orcid.org/0000-0002-3812-3191, and Kurtcuoglu, Vartan; https://orcid.org/0000-0003-2665-0995

Abstract

The capacitive measurement of the head’s dielectric properties has been recently proposed as a noninvasive method for deriving surrogates of craniospinal compliance (CC), a parameter used in the evaluation of space-occupying neurological disorders. With the higher prevalence of such disorders in the older compared to the younger population, data on the head’s dielectric properties of older healthy individuals would be of particularly high value before assessing pathologic changes. However, so far only measurements on young volunteers (< 30 years) were reported. In the present study, we have investigated the capacitively obtained electric signal known as W in older healthy individuals. Thirteen healthy subjects aged > 60 years were included in the study. W was acquired in the resting state (supine horizontal position), and during head-up and head-down tilting. AMP, the peak-to-valley amplitude of W related to cardiac action, was extracted from W. AMP was higher in this older cohort compared to the previously investigated younger one (0°: 5965 ± 1677 arbitrary units (au)). During head-up tilting, AMP decreased (+ 60°: 4446 ± 1620 au, P < 0.001), whereas it increased during head-down tilting (− 30°: 7600 ± 2123 au, P < 0.001), as also observed in the younger cohort. Our observation that AMP, a metric potentially reflective of CC, is higher in the older compared to the younger cohort aligns with the expected decrease of CC with age. Furthermore, the robustness of AMP is reinforced by the consistent relative changes observed during tilt testing in both cohorts.

Published
2024

72. Scoping Review with Topic Modeling on the Diagnostic Criteria for Degenerative Cervical Myelopathy

Author

Matsoukas, Stavros; https://orcid.org/0000-0001-5902-0637, Zipser, Carl Moritz, Zipser-Mohammadzada, Freschta; https://orcid.org/0000-0002-1829-804X, Kheram, Najmeh, Boraschi, Andrea; https://orcid.org/0000-0002-2908-5234, Jiang, Zhilin, Tetreault, Lindsay; https://orcid.org/0000-0001-8435-4292, Fehlings, Michael G; https://orcid.org/0000-0002-5722-6364, Davies, Benjamin M; https://orcid.org/0000-0003-0591-5069, Margetis, Konstantinos; https://orcid.org/0000-0002-3715-8093, Matsoukas, Stavros; https://orcid.org/0000-0001-5902-0637, Zipser, Carl Moritz, Zipser-Mohammadzada, Freschta; https://orcid.org/0000-0002-1829-804X, Kheram, Najmeh, Boraschi, Andrea; https://orcid.org/0000-0002-2908-5234, Jiang, Zhilin, Tetreault, Lindsay; https://orcid.org/0000-0001-8435-4292, Fehlings, Michael G; https://orcid.org/0000-0002-5722-6364, Davies, Benjamin M; https://orcid.org/0000-0003-0591-5069, and Margetis, Konstantinos; https://orcid.org/0000-0002-3715-8093

Abstract

STUDY DESIGN: This study is a scoping review. OBJECTIVE: There is a broad variability in the definition of degenerative cervical myelopathy (DCM) and no standardized set of diagnostic criteria to date. METHODS: We interrogated the Myelopathy.org database, a hand-indexed database of primary clinical studies conducted exclusively on DCM in humans between 2005-2021. The DCM inclusion criteria used in these studies were inputted into 3 topic modeling algorithms: Hierarchical Dirichlet Process (HDP), Latent Dirichlet Allocation (LDA), and BERtopic. The emerging topics were subjected to manual labeling and interpretation. RESULTS: Of 1676 reports, 120 papers (7.16%) had well-defined inclusion criteria and were subjected to topic modeling. Four topics emerged from the HDP model: disturbance from extremity weakness and motor signs; fine-motor and sensory disturbance of upper extremity; a combination of imaging and clinical findings is required for the diagnosis; and "reinforcing" (or modifying) factors that can aid in the diagnosis in borderline cases. The LDA model showed the following topics: disturbance to the patient is required for the diagnosis; reinforcing factors can aid in the diagnosis in borderline cases; clinical findings from the extremities; and a combination of imaging and clinical findings is required for the diagnosis. BERTopic identified the following topics: imaging abnormality, typical clinical features, range of objective criteria, and presence of clinical findings. CONCLUSIONS: This review provides quantifiable data that only a minority of past studies in DCM provided meaningful inclusion criteria. The items and patterns found here are very useful for the development of diagnostic criteria for DCM.

Published
2024

76. Methodological Approaches To Assess Innate Immunity and Innate Memory in Marine Invertebrates and Humans

Author

Manon Auguste, Daniela Melillo, Annunziata Corteggio, Rita Marino, Laura Canesi, Annalisa Pinsino, Paola Italiani, and Diana Boraschi

Subjects
innate immunity, innate memory, invertebrates, humans, in vivo, in vitro, Toxicology. Poisons, RA1190-1270
Abstract

Assessing the impact of drugs and contaminants on immune responses requires methodological approaches able to represent real-life conditions and predict long-term effects. Innate immunity/inflammation is the evolutionarily most widespread and conserved defensive mechanism in living organisms, and therefore we will focus here on immunotoxicological methods that specifically target such processes. By exploiting the conserved mechanisms of innate immunity, we have examined the most representative immunotoxicity methodological approaches across living species, to identify common features and human proxy models/assays. Three marine invertebrate organisms are examined in comparison with humans, i.e., bivalve molluscs, tunicates and sea urchins. In vivo and in vitro approaches are compared, highlighting common mechanisms and species-specific endpoints, to be applied in predictive human and environmental immunotoxicity assessment. Emphasis is given to the 3R principle of Replacement, Refinement and Reduction of Animals in Research and to the application of the ARRIVE guidelines on reporting animal research, in order to strengthen the quality and usability of immunotoxicology research data.

Published
2022
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78. Mechanisms and Barriers in Cancer Nanomedicine: Addressing Challenges, Looking for Solutions *

Author

Anchordoquy, Thomas J., primary, Barenholz, Yechezkel, additional, Boraschi, Diana, additional, Chorny, Michael, additional, Decuzzi, Paolo, additional, Dobrovolskaia, Marina A., additional, Farhangrazi, Z. Shadi, additional, Farrell, Dorothy, additional, Gabizon, Alberto, additional, Ghandehari, Hamidreza, additional, Godin, Biana, additional, La-Beck, Ninh M., additional, Ljubimova, Julia, additional, Moghimi, S. Moein, additional, Pagliaro, Len, additional, Park, Ji-Ho, additional, Peer, Dan, additional, Ruoslahti, Erkki, additional, Serkova, Natalie J., additional, and Simberg, Dmitri, additional

Published
2021
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80. Innate Memory Reprogramming by Gold Nanoparticles Depends on the Microbial Agents That Induce Memory

Author

Benjamin J. Swartzwelter, Sara Michelini, Tobias Frauenlob, Francesco Barbero, Alessandro Verde, Anna Chiara De Luca, Victor Puntes, Albert Duschl, Jutta Horejs-Hoeck, Paola Italiani, and Diana Boraschi

Subjects
innate immunity, innate memory, nanoparticles, microbial agents, monocytes, Immunologic diseases. Allergy, RC581-607
Abstract

Innate immune memory, the ability of innate cells to react in a more protective way to secondary challenges, is induced by exposure to infectious and other exogeous and endogenous agents. Engineered nanoparticles are particulate exogenous agents that, as such, could trigger an inflammatory reaction in monocytes and macrophages and could therefore be also able to induce innate memory. Here, we have evaluated the capacity of engineered gold nanoparticles (AuNPs) to induce a memory response or to modulate the memory responses induced by microbial agents. Microbial agents used were in soluble vs. particulate form (MDP and the gram-positive bacteria Staphylococcus aureus; β-glucan and the β-glucan-producing fungi C. albicans), and as whole microrganisms that were either killed (S. aureus, C. albicans) or viable (the gram-negative bacteria Helicobacter pylori). The memory response was assessed in vitro, by exposing human primary monocytes from 2-7 individual donors to microbial agents with or without AuNPs (primary response), then resting them for 6 days to allow return to baseline, and eventually challenging them with LPS (secondary memory response). Primary and memory responses were tested as production of the innate/inflammatory cytokine TNFα and other inflammatory and anti-inflammatory factors. While inactive on the response induced by soluble microbial stimuli (muramyl dipeptide -MDP-, β-glucan), AuNPs partially reduced the primary response induced by whole microorganisms. AuNPs were also unable to directly induce a memory response but could modulate stimulus-induced memory in a circumscribed fashion, limited to some agents and some cytokines. Thus, the MDP-induced tolerance in terms of TNFα production was further exacerbated by co-priming with AuNPs, resulting in a less inflammatory memory response. Conversely, the H. pylori-induced tolerance was downregulated by AuNPs only relative to the anti-inflammatory cytokine IL-10, which would lead to an overall more inflammatory memory response. These effects of AuNPs may depend on a differential interaction/association between the reactive particle surfaces and the microbial components and agents, which may lead to a change in the exposure profiles. As a general observation, however, the donor-to-donor variability in memory response profiles and reactivity to AuNPs was substantial, suggesting that innate memory depends on the individual history of exposures.

Published
2021
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81. SERS Sensing of Bacterial Endotoxin on Gold Nanoparticles

Author

Alessandro Verde, Maria Mangini, Stefano Managò, Chiara Tramontano, Ilaria Rea, Diana Boraschi, Paola Italiani, and Anna Chiara De Luca

Subjects
SERS, gold nanoparticles, LPS, biosensor, inflammation, innate immunity, Immunologic diseases. Allergy, RC581-607
Abstract

Engineered gold nanoparticles (AuNPs) find application in several fields related to human activities (i.e., food and cosmetic industry or water purification) including medicine, where they are employed for diagnosis, drug delivery and cancer therapy. As for any material/reagent for human use, the safety of AuNPs needs accurate evaluation. AuNPs are prone to contamination by bacterial endotoxin (lipopolysaccharide, LPS), a potent elicitor of inflammatory responses in mammals. It is therefore important, when assessing AuNP immunosafety and immune-related effects, to discriminate between inflammatory effects intrinsic to the NPs from those caused by an undeliberate and undetected LPS contamination. Detection of LPS contamination in AuNP preparations poses different problems when using the current LPS detection assays, given the general interference of NPs, similar to other particulate agents, with the assay reagents and endpoints. This leads to time-consuming search for optimal assay conditions for every NP batch, with unpredictable results, and to the use in parallel of different assays, each with its weaknesses and unpredictability. Thus, the development of highly sensitive, quantitative and accurate assays able to detect of LPS on AuNPs is very important, in view of their medical applications. Surface-enhanced Raman spectroscopy (SERS) is a label-free, sensitive, chemical-specific, nondestructive and fast technique that can be used to directly obtain molecular fingerprint information and a quantitative analysis of LPS adsorbed on AuNPs. Within this study, we describe the use of SERS for the label-free identification and quantitative evaluation - down to few attograms - of the LPS adsorbed on the surface of 50 nm AuNPs. We thus propose SERS as an efficient tool to detect LPS on the AuNP surface, and as the basis for the development of a new sensitive and specific LPS-detection sensor based on the use of AuNPs and SERS.

Published
2021
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83. 100 Years of BCG Immunization: Past, Present, and Future

Author

Aldo Tagliabue, Diana Boraschi, Luciana C. C. Leite, and Stefan H. E. Kaufmann

Subjects
n/a, Medicine
Abstract

The 100th anniversary of the introduction of Bacille–Calmette–Guérin (BCG) as a tuberculosis (TB) vaccine is an occasion warranting further investigation of the early attempts which culminated in the introduction of BCG as a TB vaccine, as well as of subsequent recognition of failures, new findings that broaden its applications, outstanding questions, and approaches towards the development of novel vaccine candidates [...]

Published
2022
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84. Personalised Profiling of Innate Immune Memory Induced by Nano-Imaging Particles in Human Monocytes

Author

Giacomo Della Camera, Mariusz Madej, Anna Maria Ferretti, Rita La Spina, Yang Li, Annunziata Corteggio, Tommaso Heinzl, Benjamin J. Swartzwelter, Gergö Sipos, Sabrina Gioria, Alessandro Ponti, Diana Boraschi, and Paola Italiani

Subjects
innate immunity, innate memory, nanoparticles, imaging materials, monocytes, Immunologic diseases. Allergy, RC581-607
Abstract

Engineered nanoparticles used for medical purposes must meet stringent safety criteria, which include immunosafety, i.e., the inability to activate possibly detrimental immune/inflammatory effects. Even medical nanomaterials devoid of direct immunotoxic or inflammatory effects may have an impact on human health if able to modify innate memory, which is the ability to “prime” future immune responses towards a different, possibly more detrimental reactivity. Although innate memory is usually protective, anomalous innate memory responses may be at the basis of immune pathologies. In this study, we have examined the ability of two nanomaterials commonly used for diagnostic imaging purposes, gold and iron oxide nanoparticles, to induce or modulate innate memory, using an in vitro model based on human primary monocytes. Monocytes were exposed in culture to nanoparticles alone or together with the bacterial agent LPS (priming phase/primary response), then rested for six days (extinction phase), and eventually challenged with LPS (memory/secondary response). The memory response to the LPS challenge was measured as changes in the production of inflammatory (TNFα, IL-6) and anti-inflammatory cytokines (IL-10, IL-1Ra), as compared to unprimed monocytes. The results show that both types of nanoparticles can have an effect in the induction of memory, with changes observed in the cytokine production. By comparing nanomaterials of different shapes (spherical vs. rod-shaped gold particles) and different size (17 vs. 22 nm diameter spherical iron oxide particles), it was evident that innate memory could be differentially induced and modulated depending on size, shape and chemical composition. However, the main finding was that the innate memory effect of the particles was strongly donor-dependent, with monocytes from each donor showing a distinct memory profile upon priming with the same particles, thereby making impossible to draw general conclusions on the particle effects. Thus, in order to predict the effect of imaging nanoparticles on the innate memory of patients, a personalised profiling would be required, able to take in consideration the peculiarities of the individual innate immune reactivity.

Published
2021
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87. Recommendations from the United European Gastroenterology evidence-based guidelines for the diagnosis and therapy of chronic pancreatitis

Author

Löhr, Matthias, Dominguez-Munoz, J. Enrique, Besselink, Marc, Mayerle, Julia, Rosendahl, Jonas, Lerch, Markus M., Akisik, Fatih, Kartalis, Nikolaos, Manfredi, Riccardo, Iglesias-Garcia, Julio, Haas, Stephan L., Keller, Jutta, Boermeester, Marja A., Werner, Jens, Dumonceau, Jean-Marc, Fockens, Paul, Drewes, Asbjørn, Cheyan, Güralp O., Lindkvist, Björn, Drenth, Joost P., Ewald, Nils, Hardt, Philip, de Madaria, Enrique, Gheorghe, Christian, Lindgren, Fredrik, Schneider, Alexander, Witt, Heiko, Bollen, Thomas, Boraschi, Piero, Frøkjær, Jens B., Rudolf, Sasa, Bruno, Marco, Dimcevski, Georg, Giovannini, Marc, Pukitis, Aldis, Petrone, Mariachiara, Oppong, Kofi, Ammori, Basil, Friess, Helmut, Izbiki, Jakob R., Ganeh, Paula, Salvia, Roberto, Sauvanet, Alain, Barbu, Sorin, Lyadov, Vladimir, Deprez, Pierre, Gubergrits, Natalja, Okhlobystiy, Alexey V., Arvanitakis, Marianna, Costamagna, Guido, Pap, Akos, Andersson, Roland, Hauge, Truls, McKay, Colin, Pukitis, Aldos, Regnér, Sara, Dite´, Peter, Olesen, Søren S., Duggan, Sinead, Hopper, Andrew, Phillips, Mary, Shvets, Oleg, Vujasinovic, Miroslav, Czako, Laszlo, Piemonti, Lorenzo, Kocher, Hemant, Rebours, Vinciane, Stimac, Davor, Hegyi, Peter, Drewes, Asbjørn M., Czakó, László, and Löhr, J. Matthias

Published
2018
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90. Personalized risk prediction of postoperative cognitive impairment – rationale for the EU-funded BioCog project

Author

Winterer, G., Androsova, G., Bender, O., Boraschi, D., Borchers, F., Dschietzig, T.B., Feinkohl, I., Fletcher, P., Gallinat, J., Hadzidiakos, D., Haynes, J.D., Heppner, F., Hetzer, S., Hendrikse, J., Ittermann, B., Kant, I.M.J., Kraft, A., Krannich, A., Krause, R., Kühn, S., Lachmann, G., van Montfort, S.J.T., Müller, A., Nürnberg, P., Ofosu, K., Pietsch, M., Pischon, T., Preller, J., Renzulli, E., Scheurer, K., Schneider, R., Slooter, A.J.C., Spies, C., Stamatakis, E., Volk, H.D., Weber, S., Wolf, A., Yürek, F., and Zacharias, N.

Published
2018
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91. Direct LC-MS/MS Analysis of Extra- and Intracellular Glycerophosphoinositol in Model Cancer Cell Lines

Author

Ana Margarida Campos, Genoveffa Nuzzo, Alessia Varone, Paola Italiani, Diana Boraschi, Daniela Corda, and Angelo Fontana

Subjects
inflammation, cancer, mass spectrometry, autocrine and paracrine mechanism, solid phase extraction, second messenger, Immunologic diseases. Allergy, RC581-607
Abstract

Glycerophosphoinositols (GPIs) are water-soluble bioactive phospholipid derivatives of increasing interest as intracellular and paracrine mediators of eukaryotic cell functions. The most representative compound of the family is glycerophosphoinositol (GroPIns), an ubiquitous component of mammalian cells that participates in cell proliferation, cell survival and cell response to stimuli. Levels and activity of this compound vary among cell types and deciphering these functions requires accurate measurements in in vitro and in vivo models. The conventional approaches for the analysis of GroPIns pose several issues in terms of sensitivity and product resolution, especially when the product is in the extracellular milieu. Here we present an UPLC-MS study for the quantitative analysis of this lipid derivative in cells and, for the first time, culture supernatants. The method is based on a solid-phase extraction that allows for fast desalting and analyte concentration. The robustness of the procedure was tested on the simultaneous measurements of intra- and extracellular levels of GroPIns in a number of human cell lines where it has been shown that the non-transformed cells are characterized by high extracellular level of GroPIns, whereas the tumor cells tended to have higher intracellular levels.

Published
2021
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93. Cerebrospinal Fluid Pressure Dynamics as a Bedside Test in Traumatic Spinal Cord Injury to Assess Surgical Spinal Cord Decompression: Safety, Feasibility, and Proof-of-Concept

Author

Kheram, Najmeh, Boraschi, Andrea, Pfender, Nikolai, Friedl, Susanne Gabriele, Rasenack, Maria, Fritz, Benjamin, Kurtcuoglu, Vartan, Schubert, Martin, Curt, Armin, Zipser, Carl M, and University of Zurich

Subjects
spine surgery, cerebrospinal fluid pressure, spinal cord compression, 610 Medicine & health, 10046 Balgrist University Hospital, Swiss Spinal Cord Injury Center, craniospinal compliance, General Medicine, spinal cord injury, 10052 Institute of Physiology, compression biomarker
Abstract

Background Sufficient and timely spinal cord decompression is a critical surgical objective for neurological recovery in spinal cord injury (SCI). Residual cord compression may be associated with disturbed cerebrospinal fluid pressure (CSFP) dynamics. Objectives This study aims to assess whether intrathecal CSFP dynamics in SCI following surgical decompression are feasible and safe, and to explore the diagnostic utility. Methods Prospective cohort study. Bedside lumbar CSFP dynamics and cervical MRI were obtained following surgical decompression in N = 9 with mostly cervical acute-subacute SCI and N = 2 patients with non-traumatic SCI. CSFP measurements included mean CSFP, cardiac-driven CSFP peak-to-valley amplitudes (CSFPp), Valsalva maneuver, and Queckenstedt’s test (firm pressure on jugular veins, QT). From QT, proxies for cerebrospinal fluid pulsatility curve were calculated (ie, relative pulse pressure coefficient; RPPC-Q). CSFP metrics were compared to spine-healthy patients. computer tomography (CT)-myelography was done in 3/8 simultaneous to CSFP measurements. Results Mean age was 45 ± 9 years (range 17-67; 3F), SCI was complete (AIS A, N = 5) or incomplete (AIS B-D, N = 6). No adverse events related to CSFP assessments. CSFP rise during QT was induced in all patients [range 9.6-26.6 mmHg]. However, CSFPp was reduced in 3/11 (0.1-0.3 mmHg), and in 3/11 RPPC-Q was abnormal (0.01-0.05). Valsalva response was reduced in 8/11 (2.6-23.4 mmHg). CSFP dynamics corresponded to CT-myelography. Conclusions Comprehensive bedside lumbar CSFP dynamics in SCI following decompression are safe, feasible, and can reveal distinct patterns of residual spinal cord compression. Longitudinal studies are required to define critical thresholds of impaired CSFP dynamics that may impact neurological recovery and requiring surgical revisions.

Published
2023
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95. Induction of Innate Immune Memory by Engineered Nanoparticles in Monocytes/Macrophages: From Hypothesis to Reality

Author

Paola Italiani, Giacomo Della Camera, and Diana Boraschi

Subjects
innate memory, monocytes, macrophages, nanoparticles, epigenetics, metabolism, Immunologic diseases. Allergy, RC581-607
Abstract

The capacity of engineered nanoparticles to activate cells of the innate immune system, in particular monocytes and macrophages, is considered at the basis of their toxic/inflammatory effects. It is, however, evident that even nanoparticles that do not directly induce inflammatory activation, and are therefore considered as safe, can nevertheless induce epigenetic modifications and affect metabolic pathways in monocytes and macrophages. Since epigenetic and metabolic changes are the main mechanisms of innate memory, we had previously proposed that nanoparticles can induce/modulate innate memory, that is, have the ability of shaping the secondary response to inflammatory challenges. In light of new data, it is now possible to support the original hypothesis and show that different types of nanoparticles can both directly induce innate memory, priming macrophages for a more potent response to subsequent stimuli, and modulate bacteria-induced memory by attenuating the priming-induced enhancement. This evidence raises two important issues. First, in addition to overt toxic/inflammatory effects, we should consider evaluating the capacity to induce innate memory and the related epigenetic and metabolic changes in the immunosafety assessment of nanomaterials, since modulation of innate memory may be at the basis of long-term unwanted immunological effects. The other important consideration is that this capacity of nanomaterials could open a new avenue in immunomodulation and the possibility of using engineered nanomaterials for improving immune responses to vaccines and resistance to infections, and modulate anomalous immune/inflammatory reactions in chronic inflammatory diseases, autoimmunity, and a range of other immune-related pathologies.

Published
2020
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96. Profiling the Course of Resolving vs. Persistent Inflammation in Human Monocytes: The Role of IL-1 Family Molecules

Author

Paola Italiani, Ettore Mosca, Giacomo Della Camera, Daniela Melillo, Paola Migliorini, Luciano Milanesi, and Diana Boraschi

Subjects
inflammation, monocytes, macrophages, IL-1 family, in vitro model, Immunologic diseases. Allergy, RC581-607
Abstract

Monocytes and macrophages have a central role in all phases of an inflammatory reaction. To understanding the regulation of monocyte activation during a physiological or pathological inflammation, we propose two in vitro models that recapitulate the different phases of the reaction (recruitment, initiation, development, and resolution vs. persistence of inflammation), based on human primary blood monocytes exposed to sequential modifications of microenvironmental conditions. These models exclusively describe the functional development of blood-derived monocytes that first enter an inflammatory site. All reaction phases were profiled by RNA-Seq, and the two models were validated by studying the modulation of IL-1 family members. Genes were differentially modulated, and distinct clusters were identified during the various phases of inflammation. Pathway analysis revealed that both models were enriched in pathways involved in innate immune activation. We observe that monocytes acquire an M1-like profile during early inflammation, and switch to a deactivated M2-like profile during both the resolving and persistent phases. However, during persistent inflammation they partially maintain an M1 profile, although they lose the ability to produce inflammatory cytokines compared to M1 cells. The production of IL-1 family molecules by ELISA reflected the transcriptomic profiles in the distinct phases of the two inflammatory reactions. Based on the results, we hypothesize that persistence of inflammatory stimuli cannot maintain the M1 activated phenotype of incoming monocytes for long, suggesting that the persistent presence of M1 cells and effects in a chronically inflamed tissue is mainly due to activation of newly incoming cells. Moreover, being IL-1 family molecules mainly expressed and secreted by monocytes during the early stages of the inflammatory response (within 4-14 h), and the rate of their production decreasing during the late phase of both resolving and persistent inflammation, we suppose that IL-1 factors are key regulators of the acute defensive innate inflammatory reaction that precedes establishment of longer-term adaptive immunity, and are mainly related to the presence of recently recruited blood monocytes. The well-described role of IL-1 family cytokines and receptors in chronic inflammation is therefore most likely dependent on the continuous influx of blood monocytes into a chronically inflamed site.

Published
2020
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98. Chemotherapy-Induced Liver Injury in Patients with Colorectal Liver Metastases: Findings from MR Imaging

Author

Francescamaria Donati, Dania Cioni, Salvatore Guarino, Maria Letizia Mazzeo, Emanuele Neri, and Piero Boraschi

Subjects
chemotherapy-associated steatohepatitis, hepatic damage, peliosis, nodular hyperplasia, sinusoidal obstruction syndrome, magnetic resonance imaging, Medicine (General), R5-920
Abstract

Chemotherapy-induced liver injury has been found to be quite common in cancer patients undergoing chemotherapy. Being aware of chemotherapy-induced hepatotoxicity is important for avoiding errors in detecting liver metastases and for defining the most appropriate clinical management strategy. MRI imaging has proven to be a useful troubleshooting tool that helps overcome false negatives in tumor response imaging after chemotherapy due to liver parenchyma changes. The purpose of this review is, therefore, to describe the characteristics of magnetic resonance imaging of the broad spectrum of liver damage induced by systemic chemotherapeutic agents in order to avoid misdiagnoses of liver metastases and disease progression and to define the most appropriate clinical management strategy.

Published
2022
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99. Circulating levels of IL-1 family cytokines and receptors in Alzheimer’s disease: new markers of disease progression?

Author

Paola Italiani, Ilaria Puxeddu, Sabrina Napoletano, Emanuele Scala, Daniela Melillo, Simone Manocchio, Antonella Angiolillo, Paola Migliorini, Diana Boraschi, Emilia Vitale, and Alfonso Di Costanzo

Subjects
Alzheimer’s disease, Mild cognitive impairment, Subjective memory complaints, IL-1 family, Cytokines, Receptors, Neurology. Diseases of the nervous system, RC346-429
Abstract

Abstract Background Although the mechanisms underlying AD neurodegeneration are not fully understood, it is now recognised that inflammation could play a crucial role in the initiation and progression of AD neurodegeneration. A neuro-inflammatory network, based on the anomalous activation of microglial cells, includes the production of a number of inflammatory cytokines both locally and systemically. These may serve as diagnostic markers or therapeutic targets for AD neurodegeneration. Methods We have measured the levels of the inflammation-related cytokines and receptors of the IL-1 family in serum of subjects with AD, compared to mild cognitive impairment (MCI), subjective memory complaints (SMC), and normal healthy subjects (NHS). Using a custom-made multiplex ELISA array, we examined ten factors of the IL-1 family, the inflammation-related cytokines IL-1α, IL-1β, IL-18, and IL-33, the natural inhibitors IL-1Ra and IL-18BP, and the soluble receptors sIL-1R1, sIL-1R2, sIL-1R3, and sIL-1R4. Results The inflammatory cytokines IL-1α and IL-1β, their antagonist IL-1Ra, and their soluble receptor sIL-1R1 were increased in AD. The decoy IL-1 receptor sIL-1R2 was only increased in MCI. IL-33 and its soluble receptor sIL-1R4 were also significantly higher in AD. The soluble form of the accessory receptor for both IL-1 and IL-33 receptor complexes, sIL-1R3, was increased in SMC and even more in AD. Total IL-18 levels were unchanged, whereas the inhibitor IL-18BP was significantly reduced in MCI and SMC, and highly increased in AD. The levels of free IL-18 were significantly higher in MCI. Conclusions AD is characterised by a significant alteration in the circulating levels of the cytokines and receptors of the IL-1 family. The elevation of sIL-1R4 in AD is in agreement with findings in other diseases and can be considered a marker of ongoing inflammation. Increased levels of IL-1Ra, sIL-1R1, sIL-1R4, and IL-18BP distinguished AD from MCI and SMC, and from other inflammatory diseases. Importantly, sIL-1R1, sIL-1R3, sIL-1R4, and IL-18BP negatively correlated with cognitive impairment. A significant elevation of circulating sIL-1R2 and free IL-18, not present in SMC, is characteristic of MCI and disappears in AD, making them additional interesting markers for evaluating progression from MCI to AD.

Published
2018
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