238 results on '"Reddam A"'
Search Results
2. Reliability, validity and distribution of the Spanish female sexual function index in women with relapsing multiple sclerosis
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Sara Gil-Perotin, Salma Reddam, Cristina González-Mingot, Anna Gil-Sánchez, Inés González-Suarez, Silvia Peralta, Patricia Escrivá, Lucas Barea-Moya, and Beatriz Sánchez-Sánchez
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Female sexual function index ,Sexual health ,Factor analysis ,Multiple sclerosis ,Psychometric validation ,Sexual dysfunction ,Gynecology and obstetrics ,RG1-991 ,Public aspects of medicine ,RA1-1270 - Abstract
Abstract Background The Female Sexual Function Index (FSFI) is a widely recognized tool for assessing sexual dysfunction (SD). However, its validation for Spanish women suffering from multiple sclerosis (MS) has not yet been conducted. Aim The study aimed to examine the psychometric properties of the 19-item Spanish version of the FSFI (svFSFI) in women with relapsing MS. Method A total of 137 women with relapsing MS from three Spanish centers participated in the study and completed the svFSFI. The psychometric properties of the questionnaire were evaluated. The prevalence of SD in the study cohort was determined, and its association with clinical and sociodemographic variables was analyzed using bi- and multivariate regression analyses. Results The svFSFI demonstrated excellent test-retest reliability and substantial-to-excellent internal consistency in the context of relapsing MS. There was significant convergent validity in the intercorrelations of domains. Discriminant validity showed differences in SD between women with high and low neurological disability, as measured by the Expanded Disability Status Scale (EDSS) scores. An exploratory factor analysis indicated a five-factor structure for the svFSFI. The prevalence of SD in the MS cohort was found to be 42.6%, with the ‘desire’ and ‘arousal’ domains being the most affected. Factors such as EDSS score, fatigue, depression, and having a stable partner were found to influence the total svFSFI score. Conclusion The study validates the svFSFI as a reliable and valid instrument for evaluating sexual dysfunction in Spanish women with MS.
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- 2023
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3. Tris(1,3-dichloro-2-propyl) phosphate disrupts the trajectory of cytosine methylation within developing zebrafish embryos.
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Avila-Barnard, Sarah, Dasgupta, Subham, Cheng, Vanessa, Reddam, Aalekhya, Wiegand, Jenna, and Volz, David
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Cytosine methylation ,Embryo ,TDCIPP ,Zebrafish ,Animals ,Cytosine ,DNA Methylation ,Flame Retardants ,Organophosphates ,Organophosphorus Compounds ,Phosphates ,Thymine DNA Glycosylase ,Zebrafish - Abstract
Tris (1,3-dichloro-2-propyl) phosphate (TDCIPP) is an organophosphate ester-based flame retardant widely used within the United States. Within zebrafish, initiation of TDCIPP exposure at 0.75 h post-fertilization (hpf) reliably disrupts cytosine methylation from cleavage (2 hpf) through early-gastrulation (6 hpf). Therefore, the objective of this study was to determine whether TDCIPP-induced effects on cytosine methylation persist beyond 6 hpf. First, we exposed embryos to vehicle or TDCIPP from 0.75 hpf to 6, 24, or 48 hpf, and then conducted bisulfite amplicon sequencing of a target locus (lmo7b) using genomic DNA derived from whole embryos. Within both vehicle- and TDCIPP-treated embryos, CpG methylation was similar at 6 hpf and CHG/CHH methylation were similar at 24 and 48 hpf (relative to 6 hpf). However, relative to 6 hpf within the same treatment, CpG methylation was lower within vehicle-treated embryos at 48 hpf and TDCIPP-treated embryos at 24 and 48 hpf - an effect that was driven by acceleration of CpG hypomethylation. Similar to our previous findings with DNA methyltransferase, we found that, even at high μM concentrations, TDCIPP had no effect on zebrafish and human thymine DNA glycosylase activity (a key enzyme that decreases CpG methylation), suggesting that TDCIPP-induced effects on CpG methylation are not driven by direct interaction with thymine DNA glycosylase. Finally, using 5-methylcytosine (5-mC)-specific whole-mount immunochemistry and automated imaging, we found that exposure to TDCIPP increased 5-mC abundance within the yolk of blastula-stage embryos, suggesting that TDCIPP may impact cytosine methylation of maternally loaded mRNAs during the maternal-to-zygotic transition. Overall, our findings suggest that TDCIPP disrupts the trajectory of cytosine methylation during zebrafish embryogenesis, effects which do not appear to be driven by direct interaction of TDCIPP with key enzymes that regulate cytosine methylation.
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- 2022
4. Reliability, validity and distribution of the Spanish female sexual function index in women with relapsing multiple sclerosis
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Gil-Perotin, Sara, Reddam, Salma, González-Mingot, Cristina, Gil-Sánchez, Anna, González-Suarez, Inés, Peralta, Silvia, Escrivá, Patricia, Barea-Moya, Lucas, and Sánchez-Sánchez, Beatriz
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- 2023
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5. Partial dust removal in vehicles does not mitigate human exposure to organophosphate esters
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Reddam, Aalekhya, Herkert, Nicholas, Stapleton, Heather M, and Volz, David C
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Environmental Sciences ,Pollution and Contamination ,Vaccine Related ,China ,Dust ,Environmental Exposure ,Environmental Monitoring ,Esters ,Flame Retardants ,Humans ,Organophosphates ,Organophosphate esters ,Silicone wristband ,TDCIPP ,Car interiors ,Chemical Sciences ,Biological Sciences ,Toxicology ,Biological sciences ,Chemical sciences ,Environmental sciences - Abstract
Organophosphate esters (OPEs) have been detected within car interior dust, suggesting that the indoor microenvironment of vehicles may represent a potential route of human exposure to OPEs. We recently showed that people with longer commutes are exposed to higher concentrations of tris(1,3-dichloro-2-isopropyl)phosphate (TDCIPP) - a widely used OPE - and other studies have suggested that dust removal may lead to lower exposure to chemicals. Therefore, the overall objective of this study was to determine if a decrease in interior car dust results in mitigation of personal OPE exposure. Participants (N = 49) were asked to wear silicone wristbands, and a subset of them wiped interior parts at the front of their vehicles prior to one study week (N = 25) or both study weeks (N = 11). There were no significant differences in total OPE concentrations (77.79-13,660 ng/g) nor individual OPE concentrations (0.04-4852.81 ng/g) across the different wiping groups nor in relation to participant residence ZIP codes and AC/Heater usage. These findings suggest that higher exposure to TDCIPP for participants with longer commutes may be independent of dust located on interior parts at the front of the vehicle. Therefore, our study demonstrates that there is a need for research on the potential contribution of other sources of TDCIPP exposure within car interiors.
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- 2022
6. Predictive value of individual serum neurofilament light chain levels in short-term disease activity in relapsing multiple sclerosis
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Luis Solís-Tarazona, Lars Lau Raket, Javier Cabello-Murgui, Salma Reddam, Silvia Navarro-Quevedo, and Sara Gil-Perotin
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multiple sclerosis ,biomarker ,relapse ,Z-score ,RMS ,Neurology. Diseases of the nervous system ,RC346-429 - Abstract
BackgroundThe assessment of serum neurofilament light chain (sNFL) has emerged as a diagnostic and prognostic tool in monitoring multiple sclerosis (MS). However, the application of periodic measurement in daily practice remains unclear.ObjectiveTo evaluate the predictive value of individual sNFL levels in determining disease activity in patients with relapsing MS (RMS).MethodsIn this two-year prospective study, 129 RMS patients underwent quarterly sNFL assessments and annual MRI scans. The study analyzed the correlation between individual NFL levels and past, current, and future disease activity. Group-level Z-scores were employed as a comparative measure.ResultsAmong the 37 participants, a total of 61 episodes of disease activity were observed. sNFL levels proved valuable in distinct ways; they were confirmatory of previous and current clinical and/or radiological activity and demonstrated a high negative predictive value for future 90 days activity. Interestingly, Z-scores marginally outperformed sNFL levels in terms of predictive accuracy, indicating the potential for alternative approaches in disease activity assessment. In our cohort, sNFL cut-offs of 10.8 pg./mL (sensitivity 27%, specificity 90%) and 14.3 pg./mL (sensitivity 15%, specificity 95%) correctly identified 7 and 4 out of 26 cases of radiological activity within 90 days, respectively, with 14 and 15% false negatives. When using lower cut-off values, individuals with sNFL levels below 5 pg/mL (with a sensitivity of 92%, specificity of 25%, and negative predictive value of 94%) were less likely to experience radiological activity within the next 3 months.ConclusionIndividual sNFL levels may potentially confirm prior or current disease activity and predict short-term future radiological activity in RMS. These findings underscore its periodic measurement as a valuable tool in RMS management and decision-making, enhancing the precision of clinical evaluation in routine practice.
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- 2024
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7. Inhalation of two Prop 65-listed chemicals within vehicles may be associated with increased cancer risk
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Reddam, Aalekhya and Volz, David C
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Environmental Sciences ,Pollution and Contamination ,Commerce ,Management ,Tourism and Services ,Cancer ,2.2 Factors relating to the physical environment ,Aetiology ,Good Health and Well Being ,Benzene ,Dust ,Environmental Exposure ,Formaldehyde ,Humans ,Neoplasms ,Risk Assessment ,Transportation ,Inhalation ,Vehicle ,Human ,Cancer risk - Abstract
Chemicals are listed on California's Proposition 65 (Prop 65) for their potential to cause cancer, birth defects or other reproductive harm, and certain chemicals from this list are often detected within interior vehicle dust and air. Therefore, this study examined the potential risk associated with five Prop 65-listed chemicals detected within vehicle interiors: benzene, formaldehyde, di (2-ethylhexyl) phthalate (DEHP), dibutyl phthalate (DBP), and tris(1,3-dichloro-2-propyl)phosphate (TDCIPP). Exposure estimates based on time spent within a vehicle were derived from a meta-analysis of estimated concentrations from the literature. Regulatory levels established by the California Office of Environmental Health Hazard Assessment (OEHHA) were then used to generate percent reference doses (%RfDs) for chemical-specific daily doses as well as determine the probability of risk (exceedance probability) as a function of %RfD for each chemical-specific daily dose. Based on our meta-analysis, benzene and formaldehyde were detected in vehicle interior air whereas DEHP, DBP and TDCIPP were detected in vehicle interior dust. Benzene and formaldehyde were the only two chemicals with an estimated %RfD > 100 across any of the commute times. For commute times of 20 min or longer, the %RfD was > 100 for maximum exposures based on the "maximum allowable daily level" for benzene, and for 95th-percentile exposures based on the "no significant risk level" for benzene and formaldehyde. Furthermore, the probability of exceeding 100% RfD was highest for cancer risks associated with benzene, followed by cancer risks associated with formaldehyde and the risk of reproductive and developmental toxicity associated with benzene. Lastly, within the entire state of California, the percent of commuters with a 10% probability of exceeding cancer risk associated with benzene or formaldehyde exposure was 78% and 63%, respectively. Overall, our study raises concerns about the potential risk associated with inhalation of benzene and formaldehyde for people who spend a significant amount of time in their vehicles, an issue that is especially pertinent to traffic-congested areas where people have longer commutes.
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- 2021
8. Integrating Biophysical Parameters Into the Identification of Soil Map and Pedological Characteristics: Application to the Western High Atlas Mountains, Morocco
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Labbaci, Adnane, Moukrim, Said, Laaribiya, Said, Reddam, Ouafae Abdelouahab, Pisello, Anna Laura, Editorial Board Member, Hawkes, Dean, Editorial Board Member, Bougdah, Hocine, Editorial Board Member, Rosso, Federica, Editorial Board Member, Abdalla, Hassan, Editorial Board Member, Boemi, Sofia-Natalia, Editorial Board Member, Mohareb, Nabil, Editorial Board Member, Mesbah Elkaffas, Saleh, Editorial Board Member, Bozonnet, Emmanuel, Editorial Board Member, Pignatta, Gloria, Editorial Board Member, Mahgoub, Yasser, Editorial Board Member, De Bonis, Luciano, Editorial Board Member, Kostopoulou, Stella, Editorial Board Member, Pradhan, Biswajeet, Editorial Board Member, Abdul Mannan, Md., Editorial Board Member, Alalouch, Chaham, Editorial Board Member, Gawad, Iman O., Editorial Board Member, Nayyar, Anand, Editorial Board Member, Amer, Mourad, Series Editor, Ergüler, Zeynal Abiddin, editor, Hadji, Riheb, editor, Chaminé, Helder I., editor, Rodrigo-Comino, Jesús, editor, Kallel, Amjad, editor, Merkel, Broder, editor, Eshagh, Mehdi, editor, Chenchouni, Haroun, editor, Grab, Stefan, editor, Karakus, Murat, editor, Khomsi, Sami, editor, Knight, Jasper, editor, Bezzeghoud, Mourad, editor, Barbieri, Maurizio, editor, Panda, Sandeep, editor, Benim, Ali Cemal, editor, and El-Askary, Hesham, editor
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- 2023
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9. Improving the rigor and utility of botanical toxicity studies: Recommended resources
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Patel, Deval, Sorkin, Barbara C., Mitchell, Constance A., Embry, Michelle R., Rina-Kong, Sharline, Adams, Rebecca E., DeTemple, Emily R., Reddam, Aalekhya, Gafner, Stefan, Kelber, Olaf, Rider, Cynthia V., Oketch-Rabah, Hellen, Roe, Amy L., Marles, Robin J., Dever, Joseph, and Dentali, Steven
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- 2023
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10. Utilizing systems biology to reveal cellular responses to peroxisome proliferator-activated receptor γ ligand exposure.
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Cheng, Vanessa, Reddam, Aalekhya, Bhatia, Anil, Hur, Manhoi, Kirkwood, Jay S, and Volz, David C
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Ciglitazone ,GW 9662 ,HepG2 cells ,PPARγ ,Systems biology ,Human Genome ,Genetics ,Nutrition ,Biotechnology ,Underpinning research ,Aetiology ,2.1 Biological and endogenous factors ,1.1 Normal biological development and functioning ,Cancer ,Generic health relevance ,Metabolic and endocrine ,PPAR gamma - Abstract
Peroxisome proliferator-activated receptor γ (PPARγ) is a nuclear receptor that, upon activation by ligands, heterodimerizes with retinoid X receptor (RXR), binds to PPAR response elements (PPREs), and activates transcription of downstream genes. As PPARγ plays a central role in adipogenesis, fatty acid storage, and glucose metabolism, PPARγ-specific pharmaceuticals (e.g., thiazolidinediones) have been developed to treat Type II diabetes and obesity within human populations. However, to our knowledge, no prior studies have concurrently assessed the effects of PPARγ ligand exposure on genome-wide PPARγ binding as well as effects on the transcriptome and lipidome within human cells at biologically active, non-cytotoxic concentrations. In addition to quantifying concentration-dependent effects of ciglitazone (a reference PPARγ agonist) and GW 9662 (a reference PPARγ antagonist) on human hepatocarcinoma (HepG2) cell viability, PPARγ abundance in situ, and neutral lipids, HepG2 cells were exposed to either vehicle (0.1% DMSO), ciglitazone, or GW 9662 for up to 24 h, and then harvested for 1) chromatin immunoprecipitation-sequencing (ChIP-seq) to identify PPARγ-bound regions across the entire genome, 2) mRNA-sequencing (mRNA-seq) to identify potential impacts on the transcriptome, and 3) lipidomics to identify potential alterations in lipid profiles. Following exposure to ciglitazone and GW 9662, we found that PPARγ levels were not significantly different after 2-8 h of exposure. While ciglitazone and GW 9662 resulted in a concentration-dependent increase in neutral lipids, the magnitude and localization of PPARγ-bound regions across the genome (as identified by ChIP-seq) did not vary by treatment. However, mRNA-seq and lipidomics revealed that exposure of HepG2 cells to ciglitazone and GW 9662 resulted in significant, treatment-specific effects on the transcriptome and lipidome. Overall, our findings suggest that exposure of human cells to PPARγ ligands at biologically active, non-cytotoxic concentrations results in toxicity that may be driven by a combination of both PPARγ-dependent and PPARγ-independent mechanisms.
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- 2021
11. Longer commutes are associated with increased human exposure to tris(1,3-dichloro-2-propyl) phosphate
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Reddam, Aalekhya, Tait, George, Herkert, Nicholas, Hammel, Stephanie C, Stapleton, Heather M, and Volz, David C
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Transportation ,Logistics and Supply Chains ,Built Environment and Design ,Commerce ,Management ,Tourism and Services ,Adolescent ,Adult ,Dust ,Environmental Exposure ,Environmental Monitoring ,Esters ,Flame Retardants ,Humans ,Middle Aged ,Organophosphates ,Phosphates ,Transportation ,Young Adult ,Organophosphate esters ,Silicone wristband ,Tris(1 ,3-dichloro-2-propyl) phosphate ,Human exposure ,Environmental Sciences - Abstract
Organophosphate esters (OPEs) are a class of semi-volatile organic compounds (SVOCs) used as flame retardants, plasticizers, and anti-foaming agents. Due to stringent flammability standards in vehicles and the ability of OPEs to migrate out of end-use products, elevated concentrations of OPEs have been found in car dust samples around the world. As many residents of Southern California spend a significant amount of time in their vehicles, there is potential for increased exposure to OPEs associated with longer commute times. As approximately 70% of the University of California, Riverside's undergraduate population commutes, the objective of this study was to use silicone wristbands to monitor personal exposure to OPEs and determine if exposure was associated with commute time in a subset of these students. Participants were asked to wear wristbands for five continuous days and complete daily surveys about the amount of time spent commuting. Data were then used to calculate a participant-specific total commute score. Components of Firemaster 550 (triphenyl phosphate, or TPHP, and isopropylated triaryl phosphate isomers) and Firemaster 600 (TPHP and tert-butylated triaryl phosphate isomers) - both widely used commercial flame retardant formulations - were strongly correlated with other OPEs detected within participant wristbands. Moreover, the concentration of tris(1,3-dichloro-2-propyl) phosphate (TDCIPP) was significantly correlated with the concentration of several Firemaster 500 components and tris(2-chloroisopropyl) phosphate (TCIPP). Finally, out of all OPEs measured, TDCIPP was significantly and positively correlated with total commute score, indicating that longer commutes are associated with increased human exposure to TDCIPP. Overall, our findings raise concerns about the potential for chronic TDCIPP exposure within vehicles and other forms of transportation, particularly within densely populated and traffic-congested areas such as Southern California.
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- 2020
12. High-content screening in zebrafish identifies perfluorooctanesulfonamide as a potent developmental toxicant
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Dasgupta, Subham, Reddam, Aalekhya, Liu, Zekun, Liu, Jinyong, and Volz, David C
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Medical Biotechnology ,Biomedical and Clinical Sciences ,Digestive Diseases ,Liver Disease ,Prevention ,Good Health and Well Being ,Animals ,Embryo ,Nonmammalian ,Embryonic Development ,Fluorocarbons ,Hazardous Substances ,RNA ,Messenger ,Sulfonamides ,Toxicity Tests ,Water Pollutants ,Chemical ,Zebrafish ,Zebrafish Proteins ,PFAS ,Perfluorooctanesulfonamide ,Embryonic development ,Hepatotoxicity ,Environmental Sciences - Abstract
Per- and polyfluoroalkyl substances (PFASs) have been used for decades within industrial processes and consumer products, resulting in frequent detection within the environment. Using zebrafish embryos, we screened 38 PFASs for developmental toxicity and revealed that perfluorooctanesulfonamide (PFOSA) was the most potent developmental toxicant, resulting in elevated mortality and developmental abnormalities following exposure from 6 to 24 h post fertilization (hpf) and 6 to 72 hpf. PFOSA resulted in a concentration-dependent increase in mortality and abnormalities, with surviving embryos exhibiting a >12-h delay in development at 24 hpf. Exposures initiated at 0.75 hpf also resulted in a concentration-dependent delay in epiboly, although these effects were not driven by a specific sensitive window of development. We relied on mRNA-sequencing to identify the potential association of PFOSA-induced developmental delays with impacts on the embryonic transcriptome. Relative to stage-matched vehicle controls, these data revealed that pathways related to hepatotoxicity and lipid transport were disrupted in embryos exposed to PFOSA from 0.75 to 14 hpf and 0.75 to 24 hpf. Therefore, we measured liver area as well as neutral lipids in 128-hpf embryos exposed to vehicle (0.1% DMSO) or PFOSA from 0.75 to 24 hpf and clean water from 24 to 128 hpf, and showed that PFOSA exposure from 0.75 to 24 hpf resulted in a decrease in liver area and increase in yolk sac neutral lipids at 128 hpf. Overall, our findings show that early exposure to PFOSA adversely impacts embryogenesis, an effect that may lead to altered lipid transport and liver development.
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- 2020
13. Integrating Biophysical Parameters Into the Identification of Soil Map and Pedological Characteristics: Application to the Western High Atlas Mountains, Morocco
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Labbaci, Adnane, primary, Moukrim, Said, additional, Laaribiya, Said, additional, and Reddam, Ouafae Abdelouahab, additional
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- 2023
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14. Prenatal exposure to polybrominated diphenyl ethers and birth outcomes
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Reddam, Aalekhya, Sjödin, Andreas, Cowell, Whitney, Jones, Richard, Wang, Shuang, Perera, Frederica, Herbstman, Julie B., and Kupsco, Allison
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- 2023
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15. Patient's perspective in clinical practice to assess and predict disability in multiple sclerosis
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S. Gil-Perotin, L. Bernad, S. Reddam, C. Ferrer-Pardo, S. Navarro-Quevedo, and L. Solís-Tarazona
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Medicine ,Science - Abstract
Abstract The information provided by a person with multiple sclerosis (MS) may anticipate changes in the course of the disease. To explore the role of a set of standardized patient-reported outcomes (PRO) in predicting disability progression in MS an observational study was conducted in two cohorts of 30 and 86 persons with progressive MS (pwPMS) and relapsing MS (pwRMS), respectively. The associations between baseline clinical, biochemical variables and results on MS quality of life scale (MusiQol), Modified Fatigue Impact Scale (MFIS) and Beck Depression Inventory II (BDI-II) were analyzed. The progression of disability after 2 years of follow-up in pwRMS was investigated. We show that PRO differentiated pwRMS and pwPMS cohorts with lower MusiQoL and higher MFIS and BDI-II scores in the latter. Only MFIS was correlated with disability in pwRMS and high scores in the physical MFIS domain associated with worse performance in 9HPT, and a trend in T25FW and SDMT. Instead, the cognitive MFIS domain was correlated with CHI3L1 in cerebrospinal fluid, a biomarker of progression. At the end of the study, global MFIS and BDI-II were found to be independent risk factors for disability independent of relapse. Although all PRO measures explored were altered in pwPMS, baseline MFIS discriminated current and prospective disability in pwRMS, identifying patients at risk of progression.
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- 2022
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16. mRNA-Sequencing Identifies Liver as a Potential Target Organ for Triphenyl Phosphate in Embryonic Zebrafish
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Reddam, Aalekhya, Mitchell, Constance A, Dasgupta, Subham, Kirkwood, Jay S, Vollaro, Alyssa, Hur, Manhoi, and Volz, David C
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Medical Biochemistry and Metabolomics ,Biomedical and Clinical Sciences ,Prevention ,Liver Disease ,Digestive Diseases ,triphenyl phosphate ,heart ,liver ,betaine ,osmoregulation ,zebrafish ,Pharmacology and Pharmaceutical Sciences ,Toxicology ,Pharmacology and pharmaceutical sciences - Abstract
Triphenyl phosphate (TPHP) is a commonly used organophosphate flame retardant and plasticizer in the United States. Using zebrafish as a model, the overall objective of this study was to identify potential organs that might be targeted by TPHP during embryonic development. Based on mRNA-sequencing, TPHP exposure from 24 to 30 h post fertilization (hpf) and 24 to 48 hpf significantly affected the abundance of 305 and 274 transcripts, respectively, relative to vehicle (0.1% DMSO) controls. In addition to minor effects on cardiotoxicity- and nephrotoxicity-related pathways, ingenuity pathway analysis (IPA) of significantly affected transcripts within 30- and 48-hpf embryos revealed that hepatotoxicity-related pathways were strongly affected following exposure to TPHP-alone. Moreover, although pretreatment with fenretinide (a retinoic acid receptor agonist) mitigated TPHP-induced pericardial edema and liver enlargement at 72 and 128 hpf, respectively, IPA revealed that fenretinide was unable to block TPHP-induced effects on cardiotoxicity-, nephrotoxicity-, and hepatotoxicity-related pathways at 48 hpf, suggesting that TPHP-induced effects on the transcriptome were not associated with toxicity later in development. In addition, based on Oil Red O staining, we found that exposure to TPHP nearly abolished neutral lipids from the embryonic head and trunk and, based on metabolomics, significantly decreased the total abundance of metabolites-including betaine, a known osmoprotectant-at 48 and 72 hpf. Overall, our data suggest that, in addition to the heart, TPHP exposure during early development results in adverse effects on the liver, lipid utilization, and osmoregulation within embryonic zebrafish.
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- 2019
17. Diphenyl Phosphate-Induced Toxicity During Embryonic Development
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Mitchell, Constance A, Reddam, Aalekhya, Dasgupta, Subham, Zhang, Sharon, Stapleton, Heather M, and Volz, David C
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Animals ,Biphenyl Compounds ,Embryonic Development ,Flame Retardants ,Humans ,Phosphates ,Environmental Sciences - Abstract
Diphenyl phosphate (DPHP) is an aryl phosphate ester (APE) used as an industrial catalyst and chemical additive and is the primary metabolite of flame retardant APEs, including triphenyl phosphate (TPHP). Minimal DPHP-specific toxicity studies have been published despite ubiquitous exposure within human populations following metabolism of TPHP and other APEs. Therefore, the objective of this study was to determine the potential for DPHP-induced toxicity during embryonic development. Using zebrafish as a model, we found that DPHP significantly increased the distance between the sinus venosus and bulbus arteriosis (SV-BA) at 72 h postfertilization (hpf) following initiation of exposure before and after cardiac looping. Interestingly, pretreatment with d-mannitol mitigated DPHP-induced effects on SV-BA length despite the absence of DPHP effects on pericardial area, suggesting that DPHP-induced cardiac defects are independent of pericardial edema formation. Using mRNA-sequencing, we found that DPHP disrupts pathways related to mitochondrial function and heme biosynthesis; indeed, DPHP significantly decreased hemoglobin levels in situ at 72 hpf following exposure from 24 to 72 hpf. Overall, our findings suggest that, similar to TPHP, DPHP impacts cardiac development, albeit the potency of DPHP is significantly less than TPHP within developing zebrafish.
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- 2019
18. Ciglitazone—a human PPARγ agonist—disrupts dorsoventral patterning in zebrafish
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Cheng, Vanessa, Dasgupta, Subham, Reddam, Aalekhya, and Volz, David C
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Biochemistry and Cell Biology ,Biomedical and Clinical Sciences ,Biological Sciences ,Diabetes ,Genetics ,Pediatric ,Underpinning research ,1.1 Normal biological development and functioning ,Generic health relevance ,PPAR gamma ,Ciglitazone ,Dorsoventral patterning ,Zebrafish ,Embryo ,PPARγ ,Medical and Health Sciences - Abstract
Peroxisome proliferator-activated receptor γ (PPARγ) is a ligand-activated transcription factor that regulates lipid/glucose homeostasis and adipocyte differentiation. While the role of PPARγ in adipogenesis and diabetes has been extensively studied, little is known about PPARγ function during early embryonic development. Within zebrafish, maternally-loaded pparγ transcripts are present within the first 6 h post-fertilization (hpf), and de novo transcription of zygotic pparγ commences at ~48 hpf. Since maternal pparγ transcripts are elevated during a critical window of cell fate specification, the objective of this study was to test the hypothesis that PPARγ regulates gastrulation and dorsoventral patterning during zebrafish embryogenesis. To accomplish this objective, we relied on (1) ciglitazone as a potent PPARγ agonist and (2) a splice-blocking, pparγ-specific morpholino to knockdown pparγ. We found that initiation of ciglitazone-a potent human PPARγ agonist-exposure by 4 hpf resulted in concentration-dependent effects on dorsoventral patterning in the absence of epiboly defects during gastrulation, leading to ventralized embryos by 24 hpf. Interestingly, ciglitazone-induced ventralization was reversed by co-exposure with dorsomorphin, a bone morphogenetic protein signaling inhibitor that induces strong dorsalization within zebrafish embryos. Moreover, mRNA-sequencing revealed that lipid- and cholesterol-related processes were affected by exposure to ciglitazone. However, pparγ knockdown did not block ciglitazone-induced ventralization, suggesting that PPARγ is not required for dorsoventral patterning nor involved in ciglitazone-induced toxicity within zebrafish embryos. Our findings point to a novel, PPARγ-independent mechanism of action and phenotype following ciglitazone exposure during early embryonic development.
- Published
- 2019
19. Synthesis of Fe, Mn and Cu modified TiO2 photocatalysts for photodegradation of Orange II
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Abdelouahab Reddam, Hanae, Elmail, Rachad, Lloria, Sara Cerro, Monrós Tomás, Guillermo, Reddam, Zinab Abdelouahab, and Coloma-Pascual, Fernando
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- 2020
- Full Text
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20. Patient's perspective in clinical practice to assess and predict disability in multiple sclerosis
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Gil-Perotin, S., Bernad, L., Reddam, S., Ferrer-Pardo, C., Navarro-Quevedo, S., and Solís-Tarazona, L.
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- 2022
- Full Text
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21. Synthesis of Fe, Mn and Cu modified TiO2 photocatalysts for photodegradation of Orange II
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Hanae Abdelouahab Reddam, Rachad Elmail, Sara Cerro Lloria, Guillermo Monrós Tomás, Zinab Abdelouahab Reddam, and Fernando Coloma-Pascual
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Fotocatálisis ,Óxido de titanio ,Sol-gel ,Impreganación ,Naranja II ,Clay industries. Ceramics. Glass ,TP785-869 - Abstract
The residual dyes from different sources are considered a wide variety of organic pollutants introduced into the natural water resources. One of the main sources with severe pollution problems worldwide is the textile industry and its dye-containing wastewaters. The aim of this study was the photocatalytic degradation of the azoic dye “Orange II” using Mn, Cu and Fe modified titania. The catalysts were prepared by two different methods, sol–gel and an impregnation method in a commercial titania (Degussa P25), after drying the samples were calcined at 400 °C. The samples were characterized by BET method for surface area measurement (SBET), XRD, Raman spectroscopy, XPS, UV–vis spectroscopy by diffuse reflectance technique and its photocatalytic activity was evaluated in the degradation of the azo dye Orange II in aqueous solutions using the Langmuir–Hinshelwood model. The catalysts prepared by sol–gel method exhibit a larger surface area than the prepared by impregnation and the introduction of the oxides leads to a slight reduction of SBET. The sol–gel samples show lower photoactivity than the impregnated samples due to the presence of both anatase and rutile phases in these powders, the phase junction anatase–rutile facilitate transfer of the photogenerated electron from the conduction band of the rutile phase to the trapping sites on the anatase surface and prevents the electron–hole recombination and allows the holes generated to move to the surface of the catalyst. XRD, Raman, XPS and UV–Vis data show that the metallic cations are incorporated in the titania lattice in greater extend in SG samples while remain dispersed on the surface in impregnated samples. Although the entrance of metallic cations in solid solution enhance the photocatalytic activity due to the enhanced formation of electrons–hole pairs, at a high doping content, a large number of structural defects are induced serving as a recombination center of electron–hole pairs and sol–gel samples show higher photoactivity than impregnated samples, except in the case of Fe modified samples that shows the higher red shift with Eg = 1.8 eV and compensate the induced recombination center of electron–hole pairs. Resumen: Los tintes orgánicos residuales de la industria textil suponen una amplia variedad de contaminantes orgánicos introducidos en los recursos hídricos naturales. Una de las fuentes principales con graves problemas de contaminación en todo el mundo es la industria textil y las aguas residuales que contienen estos tintes. El objetivo de este estudio fue la degradación fotocatalítica del tinte azoico «Naranja II» utilizando óxido de titanio modificado con Mn, Cu y Fe. Los catalizadores se prepararon mediante dos métodos diferentes, sol-gel y un método de impregnación en un óxido de titanio comercial (Degussa P25), después de secar las muestras se calcinaron a 400 °C. Las muestras se caracterizaron por el método BET para la medida de la superficie específica (SBET), XRD, espectroscopia Raman, XPS, espectroscopia UV-vis mediante la técnica de reflectancia difusa y se evaluó su actividad fotocatalítica en la degradación del colorante azoico Orange II en soluciones acuosas utilizando el modelo de Langmuir-Hinshelwood. Los catalizadores preparados por el método sol-gel presentan una superficie específica mayor que la preparada por impregnación y la introducción de los óxidos conduce a una ligera reducción de la SBET. Las muestras de sol-gel muestran una fotoactividad más baja que las muestras impregnadas debido a la presencia de anatasa y rutilo en estos polvos, la unión de fase anatasa-rutilo facilita la transferencia del electrón fotogenerado de la banda de conducción de la fase rutilo a los sitios de captura en la superficie de anatasa y evita la recombinación de los pares electrón-hueco permitiendo que los huecos generados se muevan hacia la superficie del catalizador. Los datos de XRD, Raman, XPS y UV-Vis muestran que los cationes metálicos se incorporan en la red de óxido de titanio con mayor amplitud en las muestras SG, mientras que permanecen dispersos en la superficie en muestras impregnadas. Aunque la entrada de cationes metálicos en solución sólida mejora la actividad fotocatalítica debido a la más fácil producción de pares electrón-hueco, con un alto contenido de dopante, se inducen una gran cantidad de defectos estructurales que sirven como centro de recombinación de pares electrón-hueco. Las muestras sol-gel muestran una fotoactividad más alta que las muestras impregnadas, excepto en el caso de muestras modificadas con Fe que muestran un mayor desplazamiento al rojo con Eg = 1.8 eV y compensan el centro de recombinación inducida de pares electrón-hueco.
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- 2020
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22. Hydrogen Storage Using Platinum‐Supported Ceria Dispersed on Activated Carbon.
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Wahby, Anass, Abdelouahab‐Reddam, Zinab, El Mail, Rachad, Silvestre‐Albero, Joaquín, and Sepúlveda‐Escribano, Antonio
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- *
CHEMICAL processes , *ACTIVATED carbon , *HYDROGEN storage , *CERIUM oxides , *DOPING agents (Chemistry) , *PLATINUM , *PLATINUM nanoparticles - Abstract
In the current work, carbon materials were used in the hydrogen adsorption process, specifically as carbons doped with platinum dispersed on ceria. The textural characterization results of the prepared samples and the starting carbon showed the presence of both micro‐ and mesopores. On the other hand, it has been observed that the specific areas were inversely proportional to the CeO2 loading. In addition, the amount of adsorbed hydrogen increased after doping the carbon with platinum and, even more, when the carbon was doped with Pt dispersed on ceria (2.2 mg/g at 25°C and 30 bar). However, there was a ceria optimum from which the adsorption capacity decreased (10% wt). The results of temperature‐programmed desorption (TPD) of hydrogen indicated a high affinity between Pt and H2 that enhanced H2 adsorption process by establishing chemical bonds between the metal particles and H2. Precisely, the presence of metallic Pt particles dispersed on ceria considerably promotes the spillover process of hydrogen on carbon. This can be confirmed by hydrogen adsorption–desorption isotherms, that showed that complete desorption of chemisorbed hydrogen required an increase of temperature. [ABSTRACT FROM AUTHOR]
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- 2024
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23. Morphometric mapping of the macrostructural abnormalities of midsagittal corpus callosum in Wilson’s disease
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Albert Stezin, Venkateswara Reddy Reddam, Shantala Hegde, Ravi Yadav, Jitender Saini, and Pramod Kumar Pal
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cognitive dysfunction ,corpus callosum ,magnetic resonance imaging ,mmse ,white matter ,wilson disease ,Neurology. Diseases of the nervous system ,RC346-429 - Abstract
BACKGROUND AND PURPOSE: The corpus callosum (CC) consists of topographically arranged white matter (WM) fibers. Previous studies have indicated the CC to be discretely involved in WD. In this study, we strived to characterize the macrostructural properties of the CC using midsagittal cross-sectional area and thickness profile measurements. MATERIALS AND METHODS: This study was performed using archived magnetic resonance imaging (MRI) scans of 14 patients with WD and 14 age- and gender-matched healthy controls. Using an automated software pipeline for morphometric profiling, the midsagittal CC was segmented into five sub-regions (CC1–5) according to the Hofer–Frahm scheme. The mean thickness and area of different CC segments and their clinical and cognitive correlates were identified. RESULTS: The mean area was significantly different only in CC2 segment (94.2 ± 25.5 vs. 118.6 ± 19.7 mm2, corrected P < 0.05). The mean thickness was significantly different in CC1 (5.06 ± 1.15 vs. 6.93 ± 0.89 mm, corrected P < 0.05), CC2 (3.73 ± 0.96 vs. 4.87 ± 1.01 mm, corrected P < 0.05), and CC3 segments (3.42 ± 0.84 vs. 3.94 ± 0.72 mm, corrected P < 0.05). The age at onset of neurological symptoms and MMSE score was significantly correlated with the morphometric changes of CC1 and CC2 segments. CONCLUSION: Morphological changes of the CC are discrete in WD. Morphometric loss of CC was associated with an earlier onset of neurological symptoms and cognitive dysfunction in WD.
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- 2021
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24. Utilizing systems biology to reveal cellular responses to peroxisome proliferator-activated receptor γ ligand exposure
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Vanessa Cheng, Aalekhya Reddam, Anil Bhatia, Manhoi Hur, Jay S. Kirkwood, and David C. Volz
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PPARγ ,Ciglitazone ,GW 9662 ,HepG2 cells ,Systems biology ,Toxicology. Poisons ,RA1190-1270 - Abstract
Peroxisome proliferator-activated receptor γ (PPARγ) is a nuclear receptor that, upon activation by ligands, heterodimerizes with retinoid X receptor (RXR), binds to PPAR response elements (PPREs), and activates transcription of downstream genes. As PPARγ plays a central role in adipogenesis, fatty acid storage, and glucose metabolism, PPARγ-specific pharmaceuticals (e.g., thiazolidinediones) have been developed to treat Type II diabetes and obesity within human populations. However, to our knowledge, no prior studies have concurrently assessed the effects of PPARγ ligand exposure on genome-wide PPARγ binding as well as effects on the transcriptome and lipidome within human cells at biologically active, non-cytotoxic concentrations. In addition to quantifying concentration-dependent effects of ciglitazone (a reference PPARγ agonist) and GW 9662 (a reference PPARγ antagonist) on human hepatocarcinoma (HepG2) cell viability, PPARγ abundance in situ, and neutral lipids, HepG2 cells were exposed to either vehicle (0.1% DMSO), ciglitazone, or GW 9662 for up to 24 h, and then harvested for 1) chromatin immunoprecipitation-sequencing (ChIP-seq) to identify PPARγ-bound regions across the entire genome, 2) mRNA-sequencing (mRNA-seq) to identify potential impacts on the transcriptome, and 3) lipidomics to identify potential alterations in lipid profiles. Following exposure to ciglitazone and GW 9662, we found that PPARγ levels were not significantly different after 2–8 h of exposure. While ciglitazone and GW 9662 resulted in a concentration-dependent increase in neutral lipids, the magnitude and localization of PPARγ-bound regions across the genome (as identified by ChIP-seq) did not vary by treatment. However, mRNA-seq and lipidomics revealed that exposure of HepG2 cells to ciglitazone and GW 9662 resulted in significant, treatment-specific effects on the transcriptome and lipidome. Overall, our findings suggest that exposure of human cells to PPARγ ligands at biologically active, non-cytotoxic concentrations results in toxicity that may be driven by a combination of both PPARγ-dependent and PPARγ-independent mechanisms.
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- 2021
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25. Predictive value of individual serum neurofilament light chain levels in short-term disease activity in relapsing multiple sclerosis
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Solís-Tarazona, Luis, primary, Raket, Lars Lau, additional, Cabello-Murgui, Javier, additional, Reddam, Salma, additional, Navarro-Quevedo, Silvia, additional, and Gil-Perotin, Sara, additional
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- 2024
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26. 18 Prenatal heat stress and birth outcomes in a rural Ghanaian cohort
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Wylie, Blair, primary, Lee, Alison, additional, Reddam, Aalekhya, additional, Nuhu, Mohammed Mujtaba, additional, Tuholske, Cascade, additional, Seyram, Kaali, additional, Ae-Ngibise, Kennetha A., additional, Medgyesi, Danielle, additional, Boamah, Ellen, additional, Baccarelli, Andrea, additional, Agyei, Oscar, additional, Chillrud, Steven, additional, Poku asante, Kwaku, additional, Jack, Darby, additional, Agyapong, Prince Darko, additional, and Sulemana, Abubakari, additional
- Published
- 2024
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27. Inverse associations of cord blood mitochondrial DNA copy number with childhood adiposity.
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Reddam, Aalekhya, Bloomquist, Tessa R., Covell, Lindsey T., Hu, Heng, Oberfield, Sharon E., Gallagher, Dympna, Miller, Rachel L., Goldsmith, Jeff, Rundle, Andrew G., Baccarelli, Andrea A., Herbstman, Julie B., and Kupsco, Allison
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CORD blood ,MITOCHONDRIAL DNA ,AFRICAN American children ,OBESITY ,ADIPOSE tissues - Abstract
Objective: The objective of this study was to examine associations between umbilical cord mitochondrial DNA copy number (mtDNAcn) and adiposity across childhood. Methods: In a prospective birth cohort of Dominican and African American children from New York City, New York (1998–2006), mtDNAcn was measured in cord blood. Children (N = 336) were evaluated for their height, weight, and bioimpedance at age 5, 7, 9, and 11 years. We used linear mixed‐effects models to assess associations of mtDNAcn tertiles in cord blood with child BMI, BMI z scores, fat mass index, and body fat percentage. Latent class growth models and interactions between mtDNAcn and child age or child age2 were used to assess associations between age and adiposity trajectories. Results: BMI was, on average, 1.5 kg/m2 higher (95% CI: 0.58, 2.5) in individuals with mtDNAcn in the low‐ compared with the middle‐mtDNAcn tertile. Results were similar for BMI z score, fat mass index, and body fat percentage. Moreover, children in the low‐mtDNAcn group had increased odds of being in an "increasing" or "high‐stable" adiposity class. Conclusions: Lower mtDNAcn at birth may predict greater childhood adiposity, highlighting the potential key role of perinatal mitochondrial function in adiposity during development. [ABSTRACT FROM AUTHOR]
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- 2024
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28. Prenatal heat stress and birth outcomes in predominantly rural central Ghana
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Abubakari, Sulemana Watara, primary, Reddam, Aalekhya, additional, Mujtaba, Mohammed Nuhu, additional, Tuholske, Cascade, additional, Kaali, Seyram, additional, Quinn, Ashlinn, additional, Ngibise, Kenneth Ayuurebobi Ae, additional, Wylie, Blair, additional, Medgyesi, Danielle, additional, Kaali, Ellen Boamah, additional, Baccarelli, Andrea, additional, Agyei, Oscar, additional, Chillrud, Steve, additional, Asante, Kwaku Poku, additional, Jack, Darby, additional, Agyapong, Prince, additional, and Lee, Alison, additional
- Published
- 2023
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29. Negative Associations of Cord Blood Mitochondrial DNA Copy Number with Childhood Adiposity Trajectories in Children
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Reddam, Aalekhya, primary, Bloomquist, Tessa R, additional, Hu, Heng, additional, Oberfield, Sharon E, additional, Gallagher, Dympna, additional, Goldsmith, Jeff, additional, Rundle, Andrew G, additional, Baccarelli, Andrea A, additional, Herbstman, Julie B, additional, and Kupsco, Allison, additional
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- 2023
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30. Reliability, Validity and Distribution of the Spanish Female Sexual Function Index in Women with Multiple Sclerosis
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Gil-Perotin, Sara, primary, Reddam, Salma, additional, González-Mingot, Cristina, additional, Gil-Sánchez, Anna, additional, González-Suarez, Inés, additional, Peralta, Silvia, additional, Escrivá, Patricia, additional, Barea-Moya, Lucas, additional, and Sánchez-Sánchez, Beatriz, additional
- Published
- 2023
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31. Abnormal subcortical volumes and cortical thickness in Parkinson's disease with impulse control disorders
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Shweta Prasad, Venkateswara Reddy Reddam, Albert Stezin, Ravi Yadav, Jitender Saini, and Pramod Kumar Pal
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cortical thickness ,impulse control disorder ,parkinson's disease ,subcortical volumetry ,Neurology. Diseases of the nervous system ,RC346-429 - Abstract
Background: The occurrence of impulse control disorders (ICDs) in Parkinson's disease (PD) is frequently attributed to dopamine replacement therapy. However, not all patients who receive medication develop ICDs. Recent imaging studies have suggested specific neuroanatomical abnormalities in patients with PD and ICD. Objectives: This study aims to identify changes in volumes of subcortical structures and cortical thickness specific to patients with PD and ICDs. Methodology: A total of 11 patients with PD and ICD (PDICD(+)), 15 patients with PD without ICD (PDICD(−)), and 15 healthy controls were analyzed in this study. ICDs were diagnosed and quantified using the Questionnaire for Impulsive-Compulsive Disorders in PD-Rating Scale (QUIP-RS). Structural imaging was performed on a 3T scanner; volumes of subcortical structures and cortical thickness were obtained using first in FSL and FreeSurfer. Results: Significant volume loss of the nucleus accumbens was observed in the PDICD(+) group. Several areas of significant cortical thinning were observed in the PDICD(+) group in comparison PDICD(−) group. Thinning of the left middle temporal gyrus, transverse temporal gyrus, and bilateral temporal poles was observed in the PDICD(+) group. No correlations were observed between QUIP-RS scores and areas of cortical thinning. Conclusions: The PDICD(+) group has specific neuroanatomical variations in the nucleus accumbens and temporal lobes, which may contribute to the development of ICD and perhaps predispose a patient to ICDs on exposure to dopamine replacement therapy.
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- 2019
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32. Air pollution and human endogenous retrovirus methylation in the school inner-city asthma intervention study
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Aalekhya Reddam, Valentina Bollati, Haotian Wu, Chiara Favero, Letizia Tarantini, Mirjam Hoxha, Nicole Comfort, Diane R Gold, Wanda Phipatanakul, and Andrea A Baccarelli
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Toxicology - Abstract
Human endogenous retroviruses (HERVs) are transposable genomic elements generally repressed through DNA methylation. HERVs can be demethylated and expressed in response to environmental stimuli. Therefore, more research is needed to understand the influence of environmental exposures on HERV methylation. Air pollutants are commonly linked with global hypomethylation, and as HERVs comprise of nearly 8% of repetitive elements in the human genome, our objective was to examine the association between air pollutant exposure and HERV methylation. We investigated 180 students with asthma participating in the School Inner-City Asthma Intervention Study, which evaluated the efficacy of classroom air filters and school-wide pest management on air pollutant/allergen exposure and asthma. Both air pollutants measured in classrooms and asthma outcomes assessed by surveys were collected pre- and post-intervention. Buccal swabs were also collected pre- and post-intervention, and methylation levels from 9 transposable genomic elements (HERV-E, -FRD, -K, -L, -R, -W, -9, and HRES and LINE1) were measured. Adjusting for relevant covariates, the overall air pollutant mixture was cross-sectionally associated with higher HERV-W and lower HERV-L and LINE1 methylation. Coarse PM was cross-sectionally associated with higher HERV-K methylation and CO2 with lower LINE1 methylation. These results suggest that exposure to air pollutants is associated with HERV-W and HERV-K hypermethylation and HERV-L and LINE1 hypomethylation in children with asthma. Future studies are needed to characterize the links between HERV methylation and possible adverse outcomes.
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- 2023
33. Mitochondrial DNA copy number dynamics and associations with the prenatal environment from birth through adolescence in a population of Dominican and African American children
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Allison Kupsco, Tessa R Bloomquist, Heng Hu, Aalekhya Reddam, Deliang Tang, Jeff Goldsmith, Andrew G Rundle, Andrea A Baccarelli, and Julie B Herbstman
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Molecular Medicine ,Cell Biology ,Molecular Biology - Published
- 2023
34. Inhalation of two Prop 65-listed chemicals within vehicles may be associated with increased cancer risk
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Aalekhya Reddam and David C. Volz
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Benzene ,Formaldehyde ,Inhalation ,Vehicle ,Human ,Cancer risk ,Environmental sciences ,GE1-350 - Abstract
Chemicals are listed on California’s Proposition 65 (Prop 65) for their potential to cause cancer, birth defects or other reproductive harm, and certain chemicals from this list are often detected within interior vehicle dust and air. Therefore, this study examined the potential risk associated with five Prop 65-listed chemicals detected within vehicle interiors: benzene, formaldehyde, di (2-ethylhexyl) phthalate (DEHP), dibutyl phthalate (DBP), and tris(1,3-dichloro-2-propyl)phosphate (TDCIPP). Exposure estimates based on time spent within a vehicle were derived from a meta-analysis of estimated concentrations from the literature. Regulatory levels established by the California Office of Environmental Health Hazard Assessment (OEHHA) were then used to generate percent reference doses (%RfDs) for chemical-specific daily doses as well as determine the probability of risk (exceedance probability) as a function of %RfD for each chemical-specific daily dose. Based on our meta-analysis, benzene and formaldehyde were detected in vehicle interior air whereas DEHP, DBP and TDCIPP were detected in vehicle interior dust. Benzene and formaldehyde were the only two chemicals with an estimated %RfD > 100 across any of the commute times. For commute times of 20 min or longer, the %RfD was > 100 for maximum exposures based on the “maximum allowable daily level” for benzene, and for 95th-percentile exposures based on the “no significant risk level” for benzene and formaldehyde. Furthermore, the probability of exceeding 100% RfD was highest for cancer risks associated with benzene, followed by cancer risks associated with formaldehyde and the risk of reproductive and developmental toxicity associated with benzene. Lastly, within the entire state of California, the percent of commuters with a 10% probability of exceeding cancer risk associated with benzene or formaldehyde exposure was 78% and 63%, respectively. Overall, our study raises concerns about the potential risk associated with inhalation of benzene and formaldehyde for people who spend a significant amount of time in their vehicles, an issue that is especially pertinent to traffic-congested areas where people have longer commutes.
- Published
- 2021
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35. Machine learning detects EEG microstate alterations in patients living with temporal lobe epilepsy
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V, Kiran Raj, Rajagopalan, Shyam Sundar, Bhardwaj, Sujas, Panda, Rajanikant, Reddam, Venkateswara Reddy, Ganne, Chaitanya, Kenchaiah, Raghavendra, Mundlamuri, Ravindranadh C, Kandavel, Thennarasu, Majumdar, Kaushik K, Parthasarathy, Satishchandra, Sinha, Sanjib, and Bharath, Rose Dawn
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- 2018
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36. Shaky and unsteady: Dynamic posturography in essential tremor
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Prasad, Shweta, Velayutham, Selva Ganapathy, Reddam, Venkateswara Reddy, Stezin, Albert, Jhunjhunwala, Ketan, and Pal, Pramod Kumar
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- 2018
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37. Human Exposure and Developmental Effects of Organophosphate Esters
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Reddam, Aalekhya
- Subjects
Environmental science ,Commuting ,Exposure Science ,Organophosphate Esters ,Toxicology ,Vehicles ,Zebarfish - Abstract
Organophosphate esters (OPEs) are a class of semi-volatile organic compounds that are used as flame retardants, plasticizers, and anti-foaming agents. Due to their ubiquitous use and ability to migrate out of end-use products, elevated concentrations of OPEs have been detected within indoor dust samples, a prevalent source for human exposure. Similar to the built environment, organophosphate esters are introduced into vehicles as plasticizers and flame retardants and have the potential to migrate and accumulate within vehicle dust. While human exposure to OPEs via indoor dust is well characterized, more information is needed to address the extent of OPE exposure and subsequent risk with time spent in vehicles and understand mechanisms underlying OPE-specific toxicity during early development. Therefore, the primary objectives of this dissertation are to 1) increase our understanding of the mechanisms of developmental toxicity for triphenyl phosphate (TPHP), a high-production volume OPE, 2) measure human exposure to OPEs within a population that spends a significant amount of time in personal transportation, and 3) calculate the risk associated with ingestion of tris(1,3-dichloro-2-propyl) phosphate (TDCIPP), another high-production volume OPE, within car interiors. For Aim 1, using whole-embryo exposures and a combination of mRNA-sequencing, phenotypic assessments, neutral lipid staining, and metabolomics, TPHP was shown to result in adverse effects on the liver, lipid abundance, and osmoregulation within the developing zebrafish. For Aim 2, using silicone wristbands to monitor personal OPE exposure within a subset of commuter vs. non-commuter undergraduate students at the University of California, Riverside (UCR), we identified that longer commutes were associated with increased TDCIPP exposure. Building on the results of Aim 2, in Aim 3 we demonstrated that a reduction in car dashboard dust does not affect increased TDCIPP exposure as a result of longer time spent in vehicles. Lastly, for Aim 4, a risk assessment identified that the ingestion of TDCIPP from car interior dust does not pose a cancer risk for commuters in California. Overall, our findings contribute to our understanding of human OPE exposure in relation to commute times and how TPHP – a ubiquitous OPE – may alter embryonic development.
- Published
- 2021
38. Longer commutes are associated with increased human exposure to tris(1,3-dichloro-2-propyl) phosphate
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Aalekhya Reddam, George Tait, Nicholas Herkert, Stephanie C. Hammel, Heather M. Stapleton, and David C. Volz
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Environmental sciences ,GE1-350 - Abstract
Organophosphate esters (OPEs) are a class of semi-volatile organic compounds (SVOCs) used as flame retardants, plasticizers, and anti-foaming agents. Due to stringent flammability standards in vehicles and the ability of OPEs to migrate out of end-use products, elevated concentrations of OPEs have been found in car dust samples around the world. As many residents of Southern California spend a significant amount of time in their vehicles, there is potential for increased exposure to OPEs associated with longer commute times. As approximately 70% of the University of California, Riverside’s undergraduate population commutes, the objective of this study was to use silicone wristbands to monitor personal exposure to OPEs and determine if exposure was associated with commute time in a subset of these students. Participants were asked to wear wristbands for five continuous days and complete daily surveys about the amount of time spent commuting. Data were then used to calculate a participant-specific total commute score. Components of Firemaster 550 (triphenyl phosphate, or TPHP, and isopropylated triaryl phosphate isomers) and Firemaster 600 (TPHP and tert-butylated triaryl phosphate isomers) – both widely used commercial flame retardant formulations – were strongly correlated with other OPEs detected within participant wristbands. Moreover, the concentration of tris(1,3-dichloro-2-propyl) phosphate (TDCIPP) was significantly correlated with the concentration of several Firemaster 500 components and tris(2-chloroisopropyl) phosphate (TCIPP). Finally, out of all OPEs measured, TDCIPP was significantly and positively correlated with total commute score, indicating that longer commutes are associated with increased human exposure to TDCIPP. Overall, our findings raise concerns about the potential for chronic TDCIPP exposure within vehicles and other forms of transportation, particularly within densely populated and traffic-congested areas such as Southern California. Keywords: Organophosphate esters, Silicone wristband, Tris(1,3-dichloro-2-propyl) phosphate, Human exposure, Transportation
- Published
- 2020
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39. Environmental Chemical Exposures and Mitochondrial Dysfunction: a Review of Recent Literature
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Aalekhya Reddam, Sarah McLarnan, and Allison Kupsco
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Health Status ,Health, Toxicology and Mutagenesis ,Public Health, Environmental and Occupational Health ,Humans ,Environmental Exposure ,Management, Monitoring, Policy and Law ,Mitochondria ,Nature and Landscape Conservation - Abstract
Purpose of Review Mitochondria play various roles that are important for cell function and survival; therefore, significant mitochondrial dysfunction may have chronic consequences that extend beyond the cell. Mitochondria are already susceptible to damage, which may be exacerbated by environmental exposures. Therefore, the aim of this review is to summarize the recent literature (2012–2022) looking at the effects of six ubiquitous classes of compounds on mitochondrial dysfunction in human populations. Recent Findings The literature suggests that there are a number of biomarkers that are commonly used to identify mitochondrial dysfunction, each with certain advantages and limitations. Classes of environmental toxicants such as polycyclic aromatic hydrocarbons, air pollutants, heavy metals, endocrine-disrupting compounds, pesticides, and nanomaterials can damage the mitochondria in varied ways, with changes in mtDNA copy number and measures of oxidative damage the most commonly measured in human populations. Other significant biomarkers include changes in mitochondrial membrane potential, calcium levels, and ATP levels. Summary This review identifies the biomarkers that are commonly used to characterize mitochondrial dysfunction but suggests that emerging mitochondrial biomarkers, such as cell-free mitochondria and blood cardiolipin levels, may provide greater insight into the impacts of exposures on mitochondrial function. This review identifies that the mtDNA copy number and measures of oxidative damage are commonly used to characterize mitochondrial dysfunction, but suggests using novel approaches in addition to well-characterized ones to create standardized protocols. We identified a dearth of studies on mitochondrial dysfunction in human populations exposed to metals, endocrine-disrupting chemicals, pesticides, and nanoparticles as a gap in knowledge that needs attention.
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- 2022
40. Use of individual measure and Z-scores to monitor disease course in Relapsing Multiple Sclerosis: A 1-year Prospective Study in a Single Center (P5-3.012)
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Solís-Tarazona, Luis Rafael, primary, Reddam, Salma, additional, and Gil-Perotín, Sara, additional
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- 2023
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41. Air Pollution and Human Endogenous Retrovirus Methylation in the School Inner-City Asthma Intervention Study
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Reddam, Aalekhya, primary, Bollati, Valentina, additional, Wu, Haotian, additional, Favero, Chiara, additional, Tarantini, Letizia, additional, Hoxha, Mirjam, additional, Comfort, Nicole, additional, Gold, Diane R, additional, Phipatanakul, Wanda, additional, and Baccarelli, Andrea A, additional
- Published
- 2023
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42. Ciglitazone—a human PPARγ agonist—disrupts dorsoventral patterning in zebrafish
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Vanessa Cheng, Subham Dasgupta, Aalekhya Reddam, and David C. Volz
- Subjects
PPARγ ,Ciglitazone ,Dorsoventral patterning ,Zebrafish ,Embryo ,Medicine ,Biology (General) ,QH301-705.5 - Abstract
Peroxisome proliferator-activated receptor γ (PPARγ) is a ligand-activated transcription factor that regulates lipid/glucose homeostasis and adipocyte differentiation. While the role of PPARγ in adipogenesis and diabetes has been extensively studied, little is known about PPARγ function during early embryonic development. Within zebrafish, maternally-loaded pparγ transcripts are present within the first 6 h post-fertilization (hpf), and de novo transcription of zygotic pparγ commences at ~48 hpf. Since maternal pparγ transcripts are elevated during a critical window of cell fate specification, the objective of this study was to test the hypothesis that PPARγ regulates gastrulation and dorsoventral patterning during zebrafish embryogenesis. To accomplish this objective, we relied on (1) ciglitazone as a potent PPARγ agonist and (2) a splice-blocking, pparγ-specific morpholino to knockdown pparγ. We found that initiation of ciglitazone—a potent human PPARγ agonist—exposure by 4 hpf resulted in concentration-dependent effects on dorsoventral patterning in the absence of epiboly defects during gastrulation, leading to ventralized embryos by 24 hpf. Interestingly, ciglitazone-induced ventralization was reversed by co-exposure with dorsomorphin, a bone morphogenetic protein signaling inhibitor that induces strong dorsalization within zebrafish embryos. Moreover, mRNA-sequencing revealed that lipid- and cholesterol-related processes were affected by exposure to ciglitazone. However, pparγ knockdown did not block ciglitazone-induced ventralization, suggesting that PPARγ is not required for dorsoventral patterning nor involved in ciglitazone-induced toxicity within zebrafish embryos. Our findings point to a novel, PPARγ-independent mechanism of action and phenotype following ciglitazone exposure during early embryonic development.
- Published
- 2019
- Full Text
- View/download PDF
43. Harnessing Extracellular Vesicle’s for Elucidating Racial/Ethnic Disparity in Alzheimer’s Disease and Related Dementia Risk in Light of Air Pollution Exposure
- Author
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Nicholson, Stacia, primary, Herrera-Moreno, José F., additional, Kalia, Vrinda, additional, Reddam, Aalekhya Reddam, additional, Paredes-Céspedes, Diana, additional, Baccarelli, Andrea, additional, and Luchsinger, José A., additional
- Published
- 2022
- Full Text
- View/download PDF
44. Use of individual measure and Z-scores to monitor disease course in Relapsing Multiple Sclerosis: A 1-year Prospective Study in a Single Center (P5-3.012)
- Author
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Luis Rafael Solís-Tarazona, Salma Reddam, and Sara Gil-Perotín
- Published
- 2023
45. Mitochondrial DNA copy number dynamics and associations with the prenatal environment from birth through adolescence in a population of Dominican and African American children
- Author
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Kupsco, Allison, primary, Bloomquist, Tessa R, additional, Hu, Heng, additional, Reddam, Aalekhya, additional, Tang, Deliang, additional, Goldsmith, Jeff, additional, Rundle, Andrew G, additional, Baccarelli, Andrea A, additional, and Herbstman, Julie B, additional
- Published
- 2023
- Full Text
- View/download PDF
46. High performance of Cu/CeO2-Nb2O5 catalysts for preferential CO oxidation and total combustion of toluene
- Author
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Jardim, Erika de Oliveira, Rico-Francés, Soledad, Abdelouahab-Reddam, Zinab, Coloma, Fernando, Silvestre-Albero, Joaquín, Sepúlveda-Escribano, Antonio, and Ramos-Fernandez, Enrique V.
- Published
- 2015
- Full Text
- View/download PDF
47. Effect of the metal precursor on the properties of Pt/CeO2/C catalysts for the total oxidation of ethanol
- Author
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Abdelouahab-Reddam, Z., Mail, R. El, Coloma, F., and Sepúlveda-Escribano, A.
- Published
- 2015
- Full Text
- View/download PDF
48. Platinum supported on highly-dispersed ceria on activated carbon for the total oxidation of VOCs
- Author
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Abdelouahab-Reddam, Z., Mail, R. El, Coloma, F., and Sepúlveda-Escribano, A.
- Published
- 2015
- Full Text
- View/download PDF
49. Análisis y prospectiva del desarrollo turístico en los parques naturales del norte de la Comunitat Valenciana
- Author
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Ouafae Abdelouahab Reddam, Diego López Olivares, and Juan Bautista Ferreres Bonfill
- Subjects
Environmental sciences ,GE1-350 ,Geography (General) ,G1-922 - Abstract
Las nuevas tendencias de la demanda turística en las últimas décadas han supuesto un creciente atractivo de nuevas tipologías turísticas entre ellas el turismo en los parques naturales. Los nuevos usos de los parques deben representar beneficios para la población local pero esos procesos deben ir acompañados de planificaciones de carácter sostenible. Para ello hemos aplicado en esta investigación una metodología Delphi a los parques naturales del interior-norte de la Comunitat Valenciana: Parque Natural de la Sierra de Espadán, Parque Natural del Penyagolosa y Parque Natural de la Tinença de Benifassà.
- Published
- 2017
50. Harnessing Extracellular Vesicle’s for Elucidating Racial/Ethnic Disparity in Alzheimer’s Disease and Related Dementia Risk in Light of Air Pollution Exposure
- Author
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Stacia Nicholson, José F. Herrera-Moreno, Vrinda Kalia, Aalekhya Reddam Reddam, Diana Paredes-Céspedes, Andrea Baccarelli, and José A. Luchsinger
- Subjects
General Earth and Planetary Sciences ,General Environmental Science - Published
- 2022
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