Search

Your search keyword '"Zanderigo, Francesca"' showing total 359 results
Start Over Author "Zanderigo, Francesca"
359 results on '"Zanderigo, Francesca"'

1. Synthesis and Preclinical Evaluation of 22-[18F]Fluorodocosahexaenoic Acid as a Positron Emission Tomography Probe for Monitoring Brain Docosahexaenoic Acid Uptake Kinetics.

Author

Duro, Marlon, Van Valkenburgh, Juno, Ingles, Diana, Tran, Jenny, Cai, Zhiheng, Ebright, Brandon, Wang, Shaowei, Kerman, Bilal, Galvan, Jasmin, Hwang, Sung Hee, Sta Maria, Naomi, Zanderigo, Francesca, Croteau, Etienne, Cunnane, Stephen, Rapoport, Stanley, Louie, Stan, Jacobs, Russell, Yassine, Hussein, and Chen, Kai

Subjects
docosahexaenoic acid, incorporation coefficient, polyunsaturated fatty acid, positron emission tomography, radiofluorination, Humans, Mice, Animals, Docosahexaenoic Acids, Apolipoprotein E4, Brain, Positron-Emission Tomography, Biological Transport, Alzheimer Disease
Abstract

Docosahexaenoic acid [22:6(n-3), DHA], a polyunsaturated fatty acid, has an important role in regulating neuronal functions and in normal brain development. Dysregulated brain DHA uptake and metabolism are found in individuals carrying the APOE4 allele, which increases the genetic risk for Alzheimers disease (AD), and are implicated in the progression of several neurodegenerative disorders. However, there are limited tools to assess brain DHA kinetics in vivo that can be translated to humans. Here, we report the synthesis of an ω-radiofluorinated PET probe of DHA, 22-[18F]fluorodocosahexaenoic acid (22-[18F]FDHA), for imaging the uptake of DHA into the brain. Using the nonradiolabeled 22-FDHA, we confirmed that fluorination of DHA at the ω-position does not significantly alter the anti-inflammatory effect of DHA in microglial cells. Through dynamic PET-MR studies using mice, we observed the accumulation of 22-[18F]FDHA in the brain over time and estimated DHAs incorporation coefficient (K*) using an image-derived input function. Finally, DHA brain K* was validated using intravenous administration of 15 mg/kg arecoline, a natural product known to increase the DHA K* in rodents. 22-[18F]FDHA is a promising PET probe that can reveal altered lipid metabolism in APOE4 carriers, AD, and other neurologic disorders. This new probe, once translated into humans, would enable noninvasive and longitudinal studies of brain DHA dynamics by guiding both pharmacological and nonpharmacological interventions for neurodegenerative diseases.

Published
2023

2. Radiosynthesis of 20-[18F]fluoroarachidonic acid for PET-MR imaging: Biological evaluation in ApoE4-TR mice.

Author

Van Valkenburgh, Juno, Duro, Marlon, Burnham, Erica, Chen, Quan, Wang, Shaowei, Tran, Jenny, Kerman, Bilal, Liu, Xiaodan, Sta Maria, Naomi, Zanderigo, Francesca, Croteau, Etienne, Rapoport, Stanley, Cunnane, Stephen, Jacobs, Russell, Yassine, Hussein, Chen, Kai, and Hwang, Sung Hee

Subjects
ApoE4, Arachidonic acid, Brain imaging, Fatty acid, PET-MR, Animals, Mice, Humans, Apolipoprotein E4, Magnetic Resonance Imaging, Brain, Astrocytes, Positron-Emission Tomography, Alzheimer Disease, Mice, Transgenic
Abstract

Dysreglulated brain arachidonic acid (AA) metabolism is involved in chronic inflammation and is influenced by apolipoprotein E4 (APOE4) genotype, the strongest genetic risk factor of late-onset Alzheimers disease (AD). Visualization of AA uptake and distribution in the brain can offer insight into neuroinflammation and AD pathogenesis. Here we present a novel synthesis and radiosynthesis of 20-[18F]fluoroarachidonic acid ([18F]-FAA) for PET imaging using a convergent route and a one-pot, single-purification radiolabeling procedure, and demonstrate its brain uptake in human ApoE4 targeted replacement (ApoE4-TR) mice. By examining p38 phosphorylation in astrocytes, we found that fluorination of AA at the ω-position did not significantly alter its biochemical role in cells. The brain incorporation coefficient (K*) of [18F]-FAA was estimated via multiple methods by using an image-derived input function from the right ventricle of the heart as a proxy of the arterial input function and brain tracer concentrations assessed by dynamic PET-MR imaging. This new synthetic approach should facilitate the practical [18F]-FAA production and allow its translation into clinical use, making investigations of dysregulation of lipid metabolism more feasible in the study of neurodegenerative diseases.

Published
2022

12. Manipulation of Dietary DHA does not Alter DHA Brain Uptake Kinetics in Mice Despite Changing Brain and Plasma DHA Levelsvs

Author

Duro, Marlon Vincent V., primary, Van Valkenburgh, Juno S., additional, Abdullah, Laila, additional, Ingles, Diana E., additional, Cai, Zhiheng, additional, Kerman, Bilal Ersen, additional, Wang, Shaowei, additional, Jacobs, Russell E., additional, Sta. Maria, Naomi, additional, Zanderigo, Francesca, additional, Croteau, Etienne, additional, Cunnane, Stephen, additional, Rapoport, Stanley I., additional, Chen, Kai, additional, and Yassine, Hussein N., additional

Published
2023
Full Text
View/download PDF

24. Synthesis and Preclinical Evaluation of 22‑[18F]Fluorodocosahexaenoic Acid as a Positron Emission Tomography Probe for Monitoring Brain Docosahexaenoic Acid Uptake Kinetics.

Author

Duro, Marlon Vincent V., Van Valkenburgh, Juno, Ingles, Diana E., Tran, Jenny, Cai, Zhiheng, Ebright, Brandon, Wang, Shaowei, Kerman, Bilal E., Galvan, Jasmin, Hwang, Sung Hee, Sta Maria, Naomi S., Zanderigo, Francesca, Croteau, Etienne, Cunnane, Stephen C., Rapoport, Stanley I., Louie, Stan G., Jacobs, Russell E., Yassine, Hussein N., and Chen, Kai

Published
2023
Full Text
View/download PDF

25. Guidelines for the content and format of PET brain data in publications and archives: A consensus paper

Author

Knudsen, Gitte M, Ganz, Melanie, Appelhoff, Stefan, Boellaard, Ronald, Bormans, Guy, Carson, Richard E, Catana, Ciprian, Doudet, Doris, Gee, Antony D, Greve, Douglas N, Gunn, Roger N, Halldin, Christer, Herscovitch, Peter, Huang, Henry, Keller, Sune H, Lammertsma, Adriaan A, Lanzenberger, Rupert, Liow, Jeih-San, Lohith, Talakad G, Lubberink, Mark, Lyoo, Chul H, Mann, J John, Matheson, Granville J, Nichols, Thomas E, Nørgaard, Martin, Ogden, Todd, Parsey, Ramin, Pike, Victor W, Price, Julie, Rizzo, Gaia, Rosa-Neto, Pedro, Schain, Martin, Scott, Peter JH, Searle, Graham, Slifstein, Mark, Suhara, Tetsuya, Talbot, Peter S, Thomas, Adam, Veronese, Mattia, Wong, Dean F, Yaqub, Maqsood, Zanderigo, Francesca, Zoghbi, Sami, and Innis, Robert B

Published
2020
Full Text
View/download PDF

32. Brain serotonin 1A receptor binding: relationship to peripheral blood DNA methylation, recent life stress and childhood adversity in unmedicated major depression.

Author

Galfalvy, Hanga, Shea, Eileen, de Vegvar, Jacqueline, Pantazatos, Spiro, Huang, Yung-yu, Burke, Ainsley K., Sublette, M. Elizabeth, Oquendo, Maria A., Zanderigo, Francesca, Miller, Jeffrey M., and Mann, J. John

Subjects
DNA methylation, SEROTONIN receptors, MENTAL depression, POSITRON emission tomography, NEURAL transmission, CD14 antigen
Abstract

Background: Childhood and lifetime adversity may reduce brain serotonergic (5-HT) neurotransmission by epigenetic mechanisms. Aims: We tested the relationships of childhood adversity and recent stress to serotonin 1A (5-HT1A) receptor genotype, DNA methylation of this gene in peripheral blood monocytes and in vivo 5-HT1A receptor binding potential (BPF) determined by positron emission tomography (PET) in 13 a priori brain regions, in participants with major depressive disorder (MDD) and healthy volunteers (controls). Method: Medication-free participants with MDD (n = 192: 110 female, 81 male, 1 other) and controls (n = 88: 48 female, 40 male) were interviewed about childhood adversity and recent stressors and genotyped for rs6295. DNA methylation was assayed at three upstream promoter sites (−1019, −1007, −681) of the 5-HT1A receptor gene. A subgroup (n = 119) had regional brain 5-HT1A receptor BPF quantified by PET. Multi-predictor models were used to test associations between diagnosis, recent stress, childhood adversity, genotype, methylation and BPF. Results: Recent stress correlated positively with blood monocyte methylation at the −681 CpG site, adjusted for diagnosis, and had positive and region-specific correlations with 5-HT1A BPF in participants with MDD, but not in controls. In participants with MDD, but not in controls, methylation at the −1007 CpG site had positive and region-specific correlations with binding potential. Childhood adversity was not associated with methylation or BPF in participants with MDD. Conclusions: These findings support a model in which recent stress increases 5-HT1A receptor binding, via methylation of promoter sites, thus affecting MDD psychopathology. [ABSTRACT FROM AUTHOR]

Published
2023
Full Text
View/download PDF

35. Radiosynthesis of 20-[18F]fluoroarachidonic acid for PET-MR imaging: Biological evaluation in ApoE4-TR mice

Author

Van Valkenburgh, Juno, primary, Duro, Marlon Vincent V., additional, Burnham, Erica, additional, Chen, Quan, additional, Wang, Shaowei, additional, Tran, Jenny, additional, Kerman, Bilal E., additional, Hwang, Sung Hee, additional, Liu, Xiaodan, additional, Sta. Maria, Naomi S., additional, Zanderigo, Francesca, additional, Croteau, Etienne, additional, Rapoport, Stanley I., additional, Cunnane, Stephen C., additional, Jacobs, Russell E., additional, Yassine, Hussein N., additional, and Chen, Kai, additional

Published
2022
Full Text
View/download PDF

37. Neuroinflammation and Acute Psychopathology

Author

Mann, J. John, primary, Galfalvy, Hanga, additional, Haghighi, Fatemeh, additional, Underwood, Mark D., additional, Miller, Jeffrey, additional, Sublette, M. Elizabeth, additional, Zanderigo, Francesca, additional, and Lan, Martin, additional

Published
2022
Full Text
View/download PDF

44. Brain 5-HT1A Receptor PET Binding, Cortisol Responses to Stress, and the Familial Transmission of Suicidal Behavior

Author

Melhem, Nadine M, primary, Zhong, Yongqi, additional, Miller, Jeffrey M, additional, Zanderigo, Francesca, additional, Ogden, R Todd, additional, Sublette, M Elizabeth, additional, Newell, Madison, additional, Burke, Ainsley, additional, Keilp, John G, additional, Lesanpezeshki, Mohammad, additional, Bartlett, Elizabeth, additional, Brent, David A, additional, and Mann, J John, additional

Published
2021
Full Text
View/download PDF

50. Nondisplaceable Binding Is a Potential Confounding Factor in 11C-PBR28 Translocator Protein PET Studies.

Author

Laurell, Gjertrud L, Plavén-Sigray, Pontus, Jucaite, Aurelija, Varrone, Andrea, Cosgrove, Kelly P, Svarer, Claus, Knudsen, Gitte M, Ogden, R Todd, Zanderigo, Francesca, Cervenka, Simon, Hillmer, Ansel T, Schain, Martin, Laurell, Gjertrud L, Plavén-Sigray, Pontus, Jucaite, Aurelija, Varrone, Andrea, Cosgrove, Kelly P, Svarer, Claus, Knudsen, Gitte M, Ogden, R Todd, Zanderigo, Francesca, Cervenka, Simon, Hillmer, Ansel T, and Schain, Martin

Abstract

The PET ligand 11C-PBR28 (N-((2-(methoxy-11C)-phenyl)methyl)-N-(6-phenoxy-3-pyridinyl)acetamide) binds to the 18-kDa translocator protein (TSPO), a biomarker of glia. In clinical studies of TSPO, the ligand total distribution volume, VT, is frequently the reported outcome measure. Since VT is the sum of the ligand-specific distribution volume (VS) and the nondisplaceable-binding distribution volume (VND), differences in VND across subjects and groups will have an impact on VTMethods: Here, we used a recently developed method for simultaneous estimation of VND (SIME) to disentangle contributions from VND and VS Data from 4 previously published 11C-PBR28 PET studies were included: before and after a lipopolysaccharide challenge (8 subjects), in alcohol use disorder (14 patients, 15 controls), in first-episode psychosis (16 patients, 16 controls), and in Parkinson disease (16 patients, 16 controls). In each dataset, regional VT estimates were obtained with a standard 2-tissue-compartment model, and brain-wide VND was estimated with SIME. VS was then calculated as VT - VND VND and VS were then compared across groups, within each dataset. Results: A lower VND was found for individuals with alcohol-use disorder (34%, P = 0.00084) and Parkinson disease (34%, P = 0.0032) than in their corresponding controls. We found no difference in VND between first-episode psychosis patients and their controls, and the administration of lipopolysaccharide did not change VNDConclusion: Our findings suggest that in TSPO PET studies, nondisplaceable binding can differ between patient groups and conditions and should therefore be considered.

Published
2021
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results