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Dive into the research topics where Abdul-Mehdi S. Ali is active.

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Featured researches published by Abdul-Mehdi S. Ali.


Pharmacology, Biochemistry and Behavior | 2009

Learning deficits in C57BL/6J mice following perinatal arsenic exposure: Consequence of lower corticosterone receptor levels?

Ebany J. Martinez-Finley; Abdul-Mehdi S. Ali; Andrea M. Allan

Most studies on arsenic as a drinking water contaminant have focused on its carcinogenic potential but a few suggest that arsenic can adversely affect cognitive development. One parameter of the hypothalamic-pituitary-adrenal axis, the corticosterone receptor (CR) has been shown to be altered by arsenic. These receptors are found throughout the central nervous system, particularly in the hippocampus, an area of the brain of central importance for learning and memory. We examined the impact of perinatal exposure to 50 parts per billion (ppb) sodium arsenate on CRs and learning and memory behavior in the C57BL/6J mouse. Measurements of CRs revealed that arsenic-exposed offspring have significantly lower levels of these receptors in the nucleus than controls. Exposed offspring showed longer latency to approach a novel object than controls in an object recognition task. In the 8-way radial arm maze, arsenic offspring had a significant increase in the number of entry errors compared to controls. Results suggest that moderate exposures to perinatal arsenic can significantly reduce CR levels in the hippocampus and can have adverse effects on learning and memory behavior.


Environmental Forensics | 2011

Mercury in Natural Waters: A Mini-Review

Aliyar Mousavi; Rose D. Chávez; Abdul-Mehdi S. Ali; Stephen E. Cabaniss

Mercury in fish is a concern as for human health. Understanding mercury toxicity, however, requires an understanding of mercury speciation. Monomethylmercury is known to be the most concerning mercury species. This mini-review first covers an introductory toxicology of mercury. As human exposure to monomethylmercury is mainly through fish and as monomethylmercury concentrations in fish are related to inorganic mercury loads, health and environmental preventive regulations concerning mercury in natural waters are addressed. Further, mercury geochemistry in natural waters is briefly reviewed, and the biogeochemical processes which affect mercury toxicity in natural waters are discussed.


Environmental Science & Technology | 2015

Elevated Concentrations of U and Co-occurring Metals in Abandoned Mine Wastes in a Northeastern Arizona Native American Community

Johanna M. Blake; Sumant Avasarala; Kateryna Artyushkova; Abdul-Mehdi S. Ali; Adrian J. Brearley; Christopher Shuey; Wm. Paul Robinson; Christopher Nez; Sadie Bill; Johnnye Lewis; Chris Hirani; Juan S. Lezama Pacheco; José M. Cerrato

The chemical interactions of U and co-occurring metals in abandoned mine wastes in a Native American community in northeastern Arizona were investigated using spectroscopy, microscopy and aqueous chemistry. The concentrations of U (67-169 μg L(-1)) in spring water samples exceed the EPA maximum contaminant limit of 30 μg L(-1). Elevated U (6,614 mg kg(-1)), V (15,814 mg kg(-1)), and As (40 mg kg(-1)) concentrations were detected in mine waste solids. Spectroscopy (XPS and XANES) solid analyses identified U (VI), As (-I and III) and Fe (II, III). Linear correlations for the release of U vs V and As vs Fe were observed for batch experiments when reacting mine waste solids with 10 mM ascorbic acid (∼pH 3.8) after 264 h. The release of U, V, As, and Fe was at least 4-fold lower after reaction with 10 mM bicarbonate (∼pH 8.3). These results suggest that U-V mineral phases similar to carnotite [K2(UO2)2V2O8] and As-Fe-bearing phases control the availability of U and As in these abandoned mine wastes. Elevated concentrations of metals are of concern due to human exposure pathways and exposure of livestock currently ingesting water in the area. This study contributes to understanding the occurrence and mobility of metals in communities located close to abandoned mine waste sites.


Neurotoxicology and Teratology | 2015

Prenatal arsenic exposure alters the programming of the glucocorticoid signaling system during embryonic development

Katharine Caldwell; Matthew T. Labrecque; Benjamin R. Solomon; Abdul-Mehdi S. Ali; Andrea M. Allan

The glucocorticoid system, which plays a critical role in a host of cellular functions including mood disorders and learning and memory, has been reported to be disrupted by arsenic. In previous work we have developed and characterized a prenatal moderate arsenic exposure (50ppb) model and identified several deficits in learning and memory and mood disorders, as well as alterations within the glucocorticoid receptor signaling system in the adolescent mouse. In these present studies we assessed the effects of arsenic on the glucocorticoid receptor (GR) pathway in both the placenta and the fetal brain in response at two critical periods, embryonic days 14 and 18. The focus of these studies was on the 11β-hydroxysteroid dehydrogenase enzymes (11β-HSD1 and 11β-HSD2) which play a key role in glucorticoid synthesis, as well as the expression and set point of the GR negative feedback regulation. Negative feedback regulation is established early in development. At E14 we found arsenic exposure significantly decreased expression of both protein and message in brain of GR and the 11β-HSD1, while 11β-HSD2 enzyme protein levels were increased but mRNA levels were decreased in the brain. These changes in brain protein continued into the E18 time point, but mRNA levels were no longer significantly altered. Placental HSD11B2 mRNA was not altered by arsenic treatment but protein levels were elevated at E14. GR placental protein levels were decreased at E18 in the arsenic exposed condition. This suggests that arsenic exposure may alter GR expression levels as a consequence of a prolonged developmental imbalance between 11β-HSD1 and 11β-HSD2 protein expression despite decreased 11HSDB2 mRNA. The suppression of GR and the failure to turn down 11β-HSD2 protein expression during fetal development may lead to an altered set point for GR signaling throughout adulthood. To our knowledge, these studies are the first to demonstrate that gestational exposure to moderate levels of arsenic results in altered fetal programming of the glucocorticoid system.


American Mineralogist | 2011

Methods to analyze metastable and microparticulate hydrated and hydrous iron sulfate minerals

B. C. Hyde; Penelope L. King; M. D. Dyar; Michael Spilde; Abdul-Mehdi S. Ali

Abstract We evaluate analytical methods for characterizing hydrated and hydrous iron sulfate minerals (HHIS) that are typically metastable in air or vacuum, commonly form micrometer-sized particles, and contain multi-valent and light elements (Fe2+, Fe3+, OH−, and H2O) that may be challenging to quantify. We synthesized or obtained HHIS-szomolnokite, melanterite, rhomboclase, schwertmannite, ferricopiapite, paracoquimbite, and jarosite-as well as Fe-oxides. These nominally pure samples were characterized with X‑ray diffraction (XRD), and then used to evaluate bulk analyses obtained from combined inductively coupled plasma, optical emission spectroscopy (ICP-OES), ion chromatography (IC), Mössbauer spectroscopy, and mass spectrometry. Integrated bulk analyses showed excellent agreement with the nominal formulas for the minerals. Because HHIS commonly form micro-sized particles-for example, HHIS found in acid mine drainage (AMD) environments and in martian meteorites-it is necessary to develop micro-analytical techniques. Microscopic mid-infrared spectroscopy allows the analyst to successfully discriminate among HHIS with minimal sample preparation on the small scale (-40 × 40 μm). For chemical analysis, electron probe microanalysis (EPMA) is preferred for samples that can be mounted, polished, coated, and that are stable under high vacuum; however, few HHIS meet those criteria. To characterize HHIS compositions, we show that multiple low-vacuum scanning electron microscopy (SEM) analyses of the same uncoated, unpolished mineral are required. Analysis of each mineral shows linear trends on ternary diagrams of 5×Fe-SO4-O (where oxygen is in O, OH, and H2O) that may be used to narrow down the HHIS mineralogy. Low-vacuum SEM also provides invaluable information about the geochemical and textural context of the samples. Our study provides protocols for microanalysis of these challenging, fine-grained, and metastable HHIS that may also be applied to other mineral groups.


Environmental Science & Technology | 2016

Spectroscopic Investigation of Interfacial Interaction of Manganese Oxide with Triclosan, Aniline, and Phenol

Nabil Shaikh; Saru Taujale; Huichun Zhang; Kateryna Artyushkova; Abdul-Mehdi S. Ali; José M. Cerrato

We investigated the reaction of manganese oxide [MnOx(s)] with phenol, aniline, and triclosan in batch experiments using X-ray photoelectron spectroscopy (XPS), Raman spectroscopy, and aqueous chemistry measurements. Analyses of XPS high-resolution spectra suggest that the Mn(III) content increased 8-10% and the content of Mn(II) increased 12-15% in the surface of reacted MnOx(s) compared to the control, indicating that the oxidation of organic compounds causes the reduction of MnOx(s). Fitting of C 1s XPS spectra suggests an increase in the number of aromatic and aliphatic bonds for MnOx(s) reacted with organic compounds. The presence of 2.7% Cl in the MnOx(s) surface after reaction with triclosan was detected by XPS survey scans, while no Cl was detected in MnOx-phenol, MnOx-aniline, and MnOx-control. Raman spectra confirm the increased intensity of carbon features in MnOx(s) samples that reacted with organic compounds compared to unreacted MnOx(s). These spectroscopy results indicate that phenol, aniline, triclosan, and related byproducts are associated with the surface of MnOx(s)-reacted samples. The results from this research contribute to a better understanding of interactions between MnOx(s) and organic compounds that are relevant to natural and engineered environments.


Toxicology reports | 2015

Sex-dependent effects of developmental arsenic exposure on methylation capacity and methylation regulation of the glucocorticoid receptor system in the embryonic mouse brain

Andrea M. Allan; Alexander K. Hafez; Matthew T. Labrecque; Elizabeth R. Solomon; M. Nabil Shaikh; Xianyun Zheng; Abdul-Mehdi S. Ali

Previously we have shown that prenatal moderate arsenic exposure (50 ppb) disrupts glucocorticoid receptor (GR) programming and that these changes continue into adolescence in males. However, it was not clear what the molecular mechanisms were promoting these GR programming changes or if these changes occurred in arsenic-exposed females. In the present studies, we assessed the effects of arsenic on protein and mRNA of the glucocorticoid receptor (GR) and 11β-hydroxysteroid dehydrogenase (Hsd) isozymes and compared the levels of methylation within the promoters of the Nr3c1 and Hsd11b1 genes in female fetal brain at embryonic days (E) 14 and 18. Prenatal arsenate exposure produced sex specific effects on the glucocorticoid system. Compared to males, females were resistant to arsenic induced changes in GR, 11β-Hsd-1 and 11β-Hsd-2 protein levels despite observed elevations in Nr3c1 and Hsd11b2 mRNA. This sex-specific effect was not due to differences in the methylation of the GR promoter as methylation of the Nr3c1 gene was either unchanged (region containing the egr-1 binding site) or similarly reduced (region containing the SP-1 transcription factor binding site) in both males and females exposed to arsenic. Arsenic did produce sex and age-specific changes in the methylation of Hsd11b1 gene, producing increased methylation in females at E14 and decreased methylation at E18.These changes were not attributed to changes in DNMT levels. Since arsenate metabolism could interfere with the generation of methyl donor groups, we assessed glutathione (GSH), S-adenosylmethionine (SAM) and As 3 methyltransferase (As3MT). Exposed males and females had similar levels of As3MT and SAM; however, females had higher levels of GSH/GSSH. It is possible that this greater anti-oxidative capacity within the females provides protection against low to moderate arsenate. Our data suggest that the GR signaling system in female offspring was not as affected by prenatal arsenic and predicts that female arsenic-exposed mice should have normal GR feedback regulation.


BioMed Research International | 2012

Five hundred years of mercury exposure and adaptation.

Guido Lombardi; Antonio Lanzirotti; Clifford Qualls; Francisco Socola; Abdul-Mehdi S. Ali; Otto Appenzeller

Mercury is added to the biosphere by anthropogenic activities raising the question of whether changes in the human chromatin, induced by mercury, in a parental generation could allow adaptation of their descendants to mercury. We review the history of Andean mining since pre-Hispanic times in Huancavelica, Peru. Despite the persistent degradation of the biosphere today, no overt signs of mercury toxicity could be discerned in present day inhabitants. However, mercury is especially toxic to the autonomic nervous system (ANS). We, therefore, tested ANS function and biologic rhythms, under the control of the ANS, in 5 Huancavelicans and examined the metal content in their hair. Mercury levels varied from none to 1.014 ppm, significantly less than accepted standards. This was confirmed by microfocused synchrotron X-ray fluorescence analysis. Biologic rhythms were abnormal and hair growth rate per year, also under ANS control, was reduced (P < 0.001). Thus, evidence of mercurys toxicity in ANS function was found without other signs of intoxication. Our findings are consistent with the hypothesis of partial transgenerational inheritance of tolerance to mercury in Huancavelica, Peru. This would generally benefit survival in the Anthropocene, the man-made world, we now live in.


Journal of Exposure Science and Environmental Epidemiology | 2017

Residential proximity to abandoned uranium mines and serum inflammatory potential in chronically exposed Navajo communities

Molly E. Harmon; Johnnye Lewis; Curtis Miller; Joseph Hoover; Abdul-Mehdi S. Ali; Chris Shuey; Miranda Cajero; Selita N. Lucas; Katherine E. Zychowski; Bernadette Pacheco; Esther Erdei; Sandy Ramone; Teddy Nez; Melissa Gonzales; Matthew J. Campen

Members of the Navajo Nation, who possess a high prevalence of cardiometabolic disease, reside near hundreds of local abandoned uranium mines (AUM), which contribute uranium, arsenic and other metals to the soil, water and air. We recently reported that hypertension is associated with mine waste exposures in this population. Inflammation is a major player in the development of numerous vascular ailments. Our previous work establishing that specific transcriptional responses of cultured endothelial cells treated with human serum can reveal relative circulating inflammatory potential in a manner responsive to pollutant exposures, providing a model to assess responses associated with exposure to these waste materials in this population. To investigate a potential link between exposures to AUM and serum inflammatory potential in affected communities, primary human coronary artery endothelial cells were treated for 4 h with serum provided by Navajo study participants (n=145). Endothelial transcriptional responses of intercellular adhesion molecule-1 (ICAM-1), vascular cell adhesion molecule-1 (VCAM-1) and chemokine ligand 2 (CCL2) were measured. These transcriptional responses were then linked to AUM exposure metrics, including surface area-weighted AUM proximity and estimated oral intake of metals. AUM proximity strongly predicted endothelial transcriptional responses to serum including CCL2, VCAM-1 and ICAM-1 (P<0.0001 for each), whereas annual water intakes of arsenic and uranium did not, even after controlling for all major effect modifiers. Inflammatory potential associated with proximity to AUMs, but not oral intake of specific metals, additionally suggests a role for inhalation exposure as a contributor to cardiovascular disease.


Toxicological Sciences | 2018

Respirable Uranyl-Vanadate-Containing Particulate Matter Derived From a Legacy Uranium Mine Site Exhibits Potentiated Cardiopulmonary Toxicity

Katherine E. Zychowski; Vamsi K. Kodali; Molly E. Harmon; Christina R Tyler; Bethany Sanchez; Yoselin Ordonez Suarez; Guy Herbert; Abigail Wheeler; Sumant Avasarala; José M. Cerrato; Nitesh K. Kunda; Pavan Muttil; Chris Shuey; Adrian J. Brearley; Abdul-Mehdi S. Ali; Yan Lin; Mohammad Shoeb; Aaron Erdely; Matthew J. Campen

Exposure to windblown particulate matter (PM) arising from legacy uranium (U) mine sites in the Navajo Nation may pose a human health hazard due to their potentially high metal content, including U and vanadium (V). To assess the toxic impact of PM derived from Claim 28 (a priority U mine) compared with background PM, and consider the putative role of metal species U and V. Two representative sediment samples from Navajo Nation sites (Background PM and Claim 28 PM) were obtained, characterized in terms of chemistry and morphology, and fractioned to the respirable (≤ 10 μm) fraction. Mice were dosed with either PM sample, uranyl acetate, or vanadyl sulfate via aspiration (100 µg), with assessments of pulmonary and vascular toxicity 24 h later. Particulate matter samples were also examined for in vitro effects on cytotoxicity, oxidative stress, phagocytosis, and inflammasome induction. Claim 28 PM10 was highly enriched with U and V and exhibited a unique nanoparticle ultrastructure compared with background PM10. Claim 28 PM10 exhibited enhanced pulmonary and vascular toxicity relative to background PM10. Both U and V exhibited complementary pulmonary inflammatory potential, with U driving a classical inflammatory cytokine profile (elevated interleukin [IL]-1β, tumor necrosis factor-α, and keratinocyte chemoattractant/human growth-regulated oncogene) while V preferentially induced a different cytokine pattern (elevated IL-5, IL-6, and IL-10). Claim 28 PM10 was more potent than background PM10 in terms of in vitro cytotoxicity, impairment of phagocytosis, and oxidative stress responses. Resuspended PM10 derived from U mine waste exhibit greater cardiopulmonary toxicity than background dusts. Rigorous exposure assessment is needed to gauge the regional health risks imparted by these unremediated sites.

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Johnnye Lewis

University of New Mexico

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