15 results on '"Leon-Velarde, Fabiola"'
Search Results
2. The role of menopause in the development of chronic mountain sickness.
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Leon-Velarde, Fabiola and Ramos, Marco Antonio
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MOUNTAIN sickness , *MENOPAUSE , *PHYSIOLOGY - Abstract
Investigates the role of menopause in the appearance of the physiopathological sequence that leads to chronic mountain sickness in a high-altitude female population. Comparison of blood oxygen saturation and erythrocytosis in the hematocrit of menopausal and premenopausal women; Scoring of signs of chronic mountain sickness.
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- 1997
3. Genome-Wide Epigenetic Signatures of Adaptive Developmental Plasticity in the Andes.
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Childebayeva, Ainash, Goodrich, Jaclyn M, Leon-Velarde, Fabiola, Rivera-Chira, Maria, Kiyamu, Melisa, Brutsaert, Tom D, Dolinoy, Dana C, and Bigham, Abigail W
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DNA methylation , *NATURAL selection , *ERYTHROCYTES , *HYPOXIA-inducible factors , *ALTITUDES , *EPIGENETICS , *EPIGENOMICS , *PHENOTYPIC plasticity - Abstract
High-altitude adaptation is a classic example of natural selection operating on the human genome. Physiological and genetic adaptations have been documented in populations with a history of living at high altitude. However, the role of epigenetic gene regulation, including DNA methylation, in high-altitude adaptation is not well understood. We performed an epigenome-wide DNA methylation association study based on whole blood from 113 Peruvian Quechua with differential lifetime exposures to high altitude (>2,500) and recruited based on a migrant study design. We identified two significant differentially methylated positions (DMPs) and 62 differentially methylated regions (DMRs) associated with high-altitude developmental and lifelong exposure statuses. DMPs and DMRs were found in genes associated with hypoxia-inducible factor pathway, red blood cell production, blood pressure, and others. DMPs and DMRs associated with fractional exhaled nitric oxide also were identified. We found a significant association between EPAS1 methylation and EPAS1 SNP genotypes, suggesting that local genetic variation influences patterns of methylation. Our findings demonstrate that DNA methylation is associated with early developmental and lifelong high-altitude exposures among Peruvian Quechua as well as altitude-adaptive phenotypes. Together these findings suggest that epigenetic mechanisms might be involved in adaptive developmental plasticity to high altitude. Moreover, we show that local genetic variation is associated with DNA methylation levels, suggesting that methylation associated SNPs could be a potential avenue for research on genetic adaptation to hypoxia in Andeans. [ABSTRACT FROM AUTHOR]
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- 2021
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4. Association of EGLN1 gene with high aerobic capacity of Peruvian Quechua at high altitude.
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Brutsaert, Tom D., Kiyamu, Melisa, Revollendo, Gianpietro Elias, Isherwood, Jenna L., Lee, Frank S., Rivera-Ch, Maria, Leon-Velarde, Fabiola, Ghosh, Sudipta, and Bigham, Abigail W.
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AEROBIC capacity , *NATURAL selection , *ALTITUDES , *ANALYSIS of covariance , *GENES - Abstract
Highland native Andeans have resided at altitude for millennia. They display high aerobic capacity (VO2max) at altitude, which may be a reflection of genetic adaptation to hypoxia. Previous genomewide (GW) scans for natural selection have nominated Egl-9 homolog 1 gene (EGLN1) as a candidate gene. The encoded protein, EGLN1/PHD2, is an O2 sensor that controls levels of the Hypoxia Inducible Factor-a (HIF-a), which regulates the cellular response to hypoxia. From GW association and analysis of covariance performed on a total sample of 429 Peruvian Quechua and 94 US lowland referents, we identified 5 EGLN1 SNPs associated with higher VO2max (L·min-1 and mL·min-1·kg-1) in hypoxia (rs1769793, rs2064766, rs2437150, rs2491403, rs479200). For 4 of these SNPs, Quechua had the highest frequency of the advantageous (high VO2max) allele compared with 25 diverse lowland comparison populations from the 1000 Genomes Project. Genotype effects were substantial, with high versus low VO2max genotype categories differing by ~11% (e.g., for rs1769793 SNP genotype TT = 34.2 mL·min-1·kg-1 vs. CC = 30.5 mL·min-1·kg-1). To guard against spurious association, we controlled for population stratification. Findings were replicated for EGLN1 SNP rs1769793 in an independent Andean sample collected in 2002. These findings contextualize previous reports of natural selection at EGLN1 in Andeans, and support the hypothesis that natural selection has increased the frequency of an EGLN1 causal variant that enhances O2 delivery or use during exercise at altitude in Peruvian Quechua. [ABSTRACT FROM AUTHOR]
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- 2019
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5. The catalytic role of a research university and international partnerships in building research capacity in Peru: A bibliometric analysis.
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Belter, Christopher W., Garcia, Patricia J., Livinski, Alicia A., Leon-Velarde, Fabiola, Weymouth, Kristen H., and Glass, Roger I.
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LABORATORIES , *UNIVERSITY research , *SCIENCE & state , *MEDICAL research , *MIDDLE-income countries - Abstract
Objective: In Peru, the past three decades have witnessed impressive growth in biomedical research catalyzed from a single research university and its investigators who secured international partnerships and funding. We conducted a bibliometric analysis of publications by Peruvian authors to understand the roots of this growth and the spread of research networks within the country. Methods: For 1997–2016, publications from Web of Science with at least one author affiliated with a Peruvian institution were examined by year, author affiliations, funding agencies, co-authorship linkages, and research topics. Results: From 1997–2016, the annual number of publications from Peru increased 9-fold from 75 to 672 totaling 6032. Of these, 56% of the articles had co-authors from the US, 13% from the UK, 12% from Brazil, and 10% from Spain. Universidad Peruana Cayetano Heredia (UPCH) was clearly the lead research institution noted on one-third of publications. Of the 20 most published authors, 15 were Peruvians, 14 trained at some point at UPCH, and 13 received advanced training abroad. Plotting co-authorships documented the growth of institutional collaborations, the robust links between investigators and some lineages of mentorship. Conclusions: This analysis suggests that international training of Peruvian physician-scientists who built and sustained longstanding international partnerships with funding accelerated quality research on diseases of local importance. The role of a single research university, UPCH, was critical to advance a culture of biomedical research. Increased funding from the Peruvian Government and its Council for Science, Technology and Innovation will be needed to sustain this growth in the future. Middle-income countries might consider the Peruvian experience where long-term research and training partnerships yielded impressive advances to address key health priorities of the country. [ABSTRACT FROM AUTHOR]
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- 2019
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6. The catalytic role of a research university and international partnerships in building research capacity in Peru: A bibliometric analysis.
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Belter, Christopher W., Garcia, Patricia J., Livinski, Alicia A., Leon-Velarde, Fabiola, Weymouth, Kristen H., and Glass, Roger I.
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BIBLIOMETRICS , *UNIVERSITY research , *SCIENCE databases , *MIDDLE-income countries , *WEB databases - Abstract
Objective: In Peru, the past three decades have witnessed impressive growth in biomedical research catalyzed from a single research university and its investigators who secured international partnerships and funding. We conducted a bibliometric analysis of publications by Peruvian authors to understand the roots of this growth and the spread of research networks within the country. Methods: For 1997–2016, publications from Web of Science with at least one author affiliated with a Peruvian institution were examined by year, author affiliations, funding agencies, co-authorship linkages, and research topics. Results: From 1997–2016, the annual number of publications from Peru increased 9-fold from 75 to 672 totaling 6032. Of these, 56% of the articles had co-authors from the US, 13% from the UK, 12% from Brazil, and 10% from Spain. Universidad Peruana Cayetano Heredia (UPCH) was clearly the lead research institution noted on one-third of publications. Of the 20 most published authors, 15 were Peruvians, 14 trained at some point at UPCH, and 13 received advanced training abroad. Plotting co-authorships documented the growth of institutional collaborations, the robust links between investigators and some lineages of mentorship. Conclusions: This analysis suggests that international training of Peruvian physician-scientists who built and sustained longstanding international partnerships with funding accelerated quality research on diseases of local importance. The role of a single research university, UPCH, was critical to advance a culture of biomedical research. Increased funding from the Peruvian Government and its Council for Science, Technology and Innovation will be needed to sustain this growth in the future. Middle-income countries might consider the Peruvian experience where long-term research and training partnerships yielded impressive advances to address key health priorities of the country. Author summary: One measure of a country's productivity in biomedical research is through an analysis of the publications in the peer reviewed literature. We have searched the Web of Science database of English language biomedical publications with a Peruvian author to examine the growth in the number of publications over the period 1997–2016, the most productive research institutions in the country, the distribution of foreign coauthors, and the diversity of topics of research. In the past 2 decades, the number of publications has increased 9-fold with the extensive engagement with foreign co-authors and funding, a growing diversity of topics expanding from infectious diseases to the NCDs, and with one third of all publications coming from a single research university. The early overseas training of a group of young Peruvian physician-scientists in the 1960s led them to establish a unique research university, Universidad Peruano Cayetano Heredia that seeded this new direction and engagement in research, and the seeding of researchers to other institutions in the country working on specific research challenges. The Peruvian experience provides a model for other countries seeking to expand their footprint in research while laying out the need for greater investment by the government to secure and expand these gains while retaining outstanding scientists who have been able to identify through research new ways to address the nation's priority problems in health. The use of bibliometric analyses can provide important insights in the growth of biomedical research in a country providing policy makers with evidence for making decisions on the future funding of research. [ABSTRACT FROM AUTHOR]
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- 2019
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7. LINE-1 and EPAS1 DNA methylation associations with high-altitude exposure.
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Childebayeva, Ainash, Jones, Tamara R., Goodrich, Jaclyn M., Leon-Velarde, Fabiola, Rivera-Chira, Maria, Kiyamu, Melisa, Brutsaert, Tom D., Dolinoy, Dana C., and Bigham, Abigail W.
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- 2019
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8. Increased Cardiometabolic Risk and Worsening Hypoxemia at High Altitude.
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Miele, Catherine H., Schwartz, Alan R., Gilman, Robert H., Luu Pham, Wise, Robert A., Davila-Roman, Victor G., Jun, Jonathan C., Polotsky, Vsevolod Y., Miranda, J. Jaime, Leon-Velarde, Fabiola, and Checkley, William
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HYPOXEMIA , *METABOLIC syndrome , *CARDIOVASCULAR diseases risk factors , *MOUNTAIN sickness , *PHYSIOLOGICAL effects of altitudes , *INSULIN resistance - Abstract
Metabolic syndrome, insulin resistance, diabetes, and dyslipidemia are associated with an increased risk of cardiovascular disease. While excessive erythrocytosis is associated with cardiovascular complications, it is unclear how worsening hypoxemia of any degree affects cardiometabolic risk factors in high-altitude populations. We studied the relationship between daytime resting oxyhemoglobin saturation and cardiometabolic risk factors in adult participants living in Puno, Peru (3825 m above sea level). We used multivariable logistic regression models to study the relationship between having a lower oxyhemoglobin saturation and markers of cardiometabolic risk. Nine hundred and fifty-four participants (mean age 55 years, 52% male) had information available on pulse oximetry and markers of cardiometabolic risk. Average oxyhemoglobin saturation was 90% (interquartile range 88%-92%) and 43 (4.5%) had excessive erythrocytosis. Older age, decreased height-adjusted lung function, and higher body mass index (BMI) were associated with having an oxyhemoglobin saturation ≤85%. When adjusting for age, sex, socioeconomic status, having excessive erythrocytosis, and site, we found that each 5% decrease in oxyhemoglobin saturation was associated with a higher adjusted odds of metabolic syndrome (OR = 1.35, 95% CI: 1.07-1.72, p < 0.04), insulin resistance as defined by homeostasis model assessment-insulin resistance (HOMA-IR) >2 mass units (OR = 1.29, 95% CI: 1.00-1.67, p < 0.05), hemoglobin A1c ≥6.5% (OR = 1.66, 95% CI: 1.09-2.51, p < 0.04), and high sensitivity C-reactive protein (hs-CRP) ≥3 mg/L (OR = 1.46, 95% CI: 1.09-1.96, p < 0.01). In high-altitude populations in Puno, Peru, a higher BMI and lower pulmonary function were associated with lower resting daytime oxyhemoglobin saturation. Lower resting oxyhemoglobin saturation, in turn, was associated with higher odds of having multiple unfavorable cardiometabolic factors. Worsening hypoxia of any degree in high-altitude dwellers may be an independent risk factor for cardiovascular disease. [ABSTRACT FROM AUTHOR]
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- 2016
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9. Long-Term Chronic Intermittent Hypobaric Hypoxia in Rats Causes an Imbalance in the Asymmetric Dimethylarginine/Nitric Oxide Pathway and ROS Activity: A Possible Synergistic Mechanism for Altitude Pulmonary Hypertension?
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Lüneburg, Nicole, Siques, Patricia, Brito, Julio, Arriaza, Karem, Pena, Eduardo, Klose, Hans, Leon-Velarde, Fabiola, and Böger, Rainer H.
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PULMONARY hypertension , *NITRIC-oxide synthases , *HYPOXEMIA , *REACTIVE oxygen species , *ARGININE , *ASYMMETRY (Chemistry) , *INFLUENCE of altitude , *HYPOBARIC chambers - Abstract
Chronic intermittent hypoxia (CIH) and chronic hypoxia (CH) are associated with high-altitude pulmonary hypertension (HAPH). Asymmetric dimethylarginine (ADMA), a NO synthase (NOS) inhibitor, may contribute to HAPH. This study assessed changes in the ADMA/NO pathway and the underlying mechanisms in rat lungs following exposure to CIH or CH simulated in a hypobaric chamber at 428 Torr. Twenty-four adult Wistar rats were randomly assigned to three groups: CIH2x2 (2 days of hypoxia/2 days of normoxia), CH, and NX (permanent normoxia), for 30 days. All analyses were performed in whole lung tissue. L-Arginine and ADMA were analyzed using LC-MS/MS. Under both hypoxic conditions right ventricular hypertrophy was observed (p<0.01) and endothelial NOS mRNA increased (p<0.001), but the phosphorylated/nonphosphorylated vasodilator-stimulated phosphoprotein (VASP) ratio was unchanged. ADMA increased (p<0.001), whereas dimethylarginine dimethylaminohydrolase (DDAH) activity decreased only under CH (p<0.05). Although arginase activity increased (p<0.001) and L-arginine exhibited no changes, the L-arginine/ADMA ratio decreased significantly (p<0.001). Moreover, NOX4 expression increased only under CH (p<0.01), but malondialdehyde (MDA) increased (up to 2-fold) equally in CIH2x2 and CH (p<0.001). Our results suggest that ADMA and oxidative stress likely reduce NO bioavailability under altitude hypoxia, which implies greater pulmonary vascular reactivity and tone, despite the more subdued effects observed under CIH. [ABSTRACT FROM AUTHOR]
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- 2016
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10. Andean and Tibetan patterns of adaptation to high altitude.
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Bigham, Abigail W., Wilson, Megan J., Julian, Colleen G., Kiyamu, Melisa, Vargas, Enrique, Leon‐Velarde, Fabiola, Rivera‐Chira, Maria, Rodriquez, Carmelo, Browne, Vaughn A., Parra, Esteban, Brutsaert, Tom D., Moore, Lorna G., and Shriver, Mark D.
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INFLUENCE of altitude , *PHYSIOLOGICAL adaptation , *NATURAL selection , *TIBETANS , *HEMOGLOBINS , *SINGLE nucleotide polymorphisms , *REGRESSION analysis , *GENETICS - Abstract
Objectives High-altitude hypoxia, or decreased oxygen levels caused by low barometric pressure, challenges the ability of humans to live and reproduce. Despite these challenges, human populations have lived on the Andean Altiplano and the Tibetan Plateau for millennia and exhibit unique circulatory, respiratory, and hematological adaptations to life at high altitude. We and others have identified natural selection candidate genes and gene regions for these adaptations using dense genome scan data. One gene previously known to be important in cellular oxygen sensing, egl nine homolog 1 ( EGLN1), shows evidence of positive selection in both Tibetans and Andeans. Interestingly, the pattern of variation for this gene differs between the two populations. Continued research among Tibetan populations has identified statistical associations between hemoglobin concentration and single nucleotide polymorphism ( SNP) genotype at EGLN1 and a second gene, endothelial PAS domain protein 1 ( EPAS1). Methods To measure for the effects of EGLN1 and EPAS1 altitude genotypes on hemoglobin concentration among Andean highlanders, we performed a multiple linear regression analysis of 10 candidate SNPs in or near these two genes. Results Our analysis did not identify significant associations between EPAS1 or EGLN1 SNP genotypes and hemoglobin concentration in Andeans. Conclusions These results contribute to our understanding of the unique set of adaptations developed in different highland groups to the hypoxia of high altitude. Overall, the results provide key insights into the patterns of geneticadaptation to high altitude in Andean and Tibetan populations. Am. J. Hum. Biol. 25:190-197, 2013. © 2013 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]
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- 2013
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11. A Genomewide Admixture Mapping Panel for Hispanic/Latino Populations.
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Mao, Xianyun, Bigham, Abigail W., Mei, Rui, Gutierrez, Gerardo, Weiss, Ken M., Brutsaert, Tom D., Leon-Velarde, Fabiola, Moore, Lorna G., Vargas, Enrique, McKeigue, Paul M., Shriver, Mark D., and Parra, Esteban J.
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HISPANIC Americans , *GENEALOGY , *DISEASE risk factors - Abstract
Admixture mapping (AM) is a promising method for the identification of genetic risk factors for complex traits and diseases showing prevalence differences among populations. Efficient application of this method requires the use of a genomewide panel of ancestry-informative markers (AIMs) to infer the population of origin of chromosomal regions in admixed individuals. Genomewide AM panels with markers showing high frequency differences between West African and European populations are already available for disease-gene discovery in African Americans. However, no such a map is yet available for Hispanic/Latino populations, which are the result of two-way admixture between Native American and European populations or of three-way admixture of Native American, European, andWest African populations. Here, we report a genomewide AM panel with 2,120 AIMs showing high frequency differences between Native American and European populations. The average intermarker genetic distance is ∼1.7 cM. The panel was identified by genotyping, with the Affymetrix GeneChip Human Mapping 500K array, a population samplewith European ancestry, a Mesoamerican sample comprising Maya and Nahua from Mexico, and a South American sample comprising Aymara/Quechua from Bolivia and Quechua from Peru. The main criteria for marker selection were both high information content for Native American/European ancestry (measured as the standardized variance of the allele frequencies, also known as ''f value") and small frequency differences between the Mesoamerican and South American samples. This genomewide AM panel will make it possible to apply AM approaches in many admixed populations throughout the Americas. [ABSTRACT FROM AUTHOR]
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- 2007
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12. The AndeanEGLN1 adaptive allele could be a loss of function variant that increases HIF1-α in skeletal muscle.
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Brutsaert, Tom D., Kiyamu, Melissa, Revollendo, Gianpietro Elias, Isherwood, Jenna L., Lee, Frank S., Rivera-Ch, Maria, Leon-Velarde, Fabiola, Ghosh, Sudipta, and Bigham, Abigail W.
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SKELETAL muscle , *ALLELES , *PULMONARY gas exchange - Published
- 2020
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13. Plasma catecholamines and blood volume in native Andeans during hypoxia and normoxia.
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Gamboa, Alfredo, Gamboa, Jorge L., Holmes, Courtney, Sharabi, Yehonatan, Leon-Velarde, Fabiola, Fischman, Gary J., Appenzeller, Otto, and Goldstein, David S.
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HYPOXEMIA , *CATECHOLAMINES , *BLOOD volume , *HEMATOCRIT , *MOUNTAIN sickness , *POLYCYTHEMIA , *NORADRENALINE , *DOPAMINE - Abstract
Plasma catechols and blood volume were measured in 20 male, native high-altitude residents of Cerro de Pasco, Peru (4338 m), while hypoxic and subsequently while normoxic at sea level. Ten subjects were healthy controls,with hematocrits lower than 61%, and ten had chronic mountain sickness (CMS), a syndrome of maladaptation to altitude, characterized by polycythemia (hematocrit > 61%), profound hypoxemia, and neurologic symptoms. The main aim of the study was to evaluate the chronic effects of hypoxia on plasma catechols and on blood volume, by studying these parameters during hypoxia at high altitude (HA) and shortly after exposure to normoxia at sea level (SL). Subjects were first studied at HA in their habitual hypoxic environment, and measurements were repeated within 4 hours of arrival at SL (Lima, Peru, 150 m). All subjects had higher plasma norepinephrine (NE), dopamine (DA), and dihydroxyphenylglycol (DHPG) levels in HA (NE in controls and CMS: 414±47 and 514±35 pg/mL; DA: 9±1 and 13±1 pg/mL, DHPG: 817±48 and 972±77 pg/mL) than at SL (NE: 164±9 and 243±28 pg/mL; DA: 4±0.5 and 5±1 pg/mL DHPG: 502±23 and 649±39 pg/mL). Group differences were statistically significant only for NE in the CMS group. Plasma volume was higher in HA in both groups (p<0.05); red cell volume was higher in HA only in the CMS group. The results indicate sympathetic nervous stimulation by chronic ambient hypoxia at altitude in Andean natives, independent of maladaptation to their native environment. [ABSTRACT FROM AUTHOR]
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- 2006
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14. Blood lead levels in Peruvian adults are associated with proximity to mining and DNA methylation.
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Childebayeva, Ainash, Goodrich, Jaclyn M., Chesterman, Nathan, Leon-Velarde, Fabiola, Rivera-Ch, Maria, Kiyamu, Melisa, Brutsaert, Tom D., Bigham, Abigail W., and Dolinoy, Dana C.
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DNA methylation , *ADULTS , *MINES & mineral resources , *CARDIOVASCULAR system , *NERVOUS system - Abstract
• Inorganic lead exposure can affect various systems of the body, and especially the nervous system. • Lead exposure can also influence the epigenome, including DNA methylation. • Lead is associated with epigenetic changes in neurological function and metal ion binding genes. • We also found an association between lead and hemoglobin, and lead levels and proximity to mining. Inorganic lead (Pb) is common in the environment, and is toxic to neurological, renal, and cardiovascular systems. Pb exposure influences the epigenome with documented effects on DNA methylation (DNAm). We assessed the impact of low levels of Pb exposure on DNAm among non-miner individuals from two locations in Peru: Lima, the capital, and Cerro de Pasco, a highland mining town, to study the effects of Pb exposure on physiological outcomes and DNAm. Pb levels were measured in whole blood (n = 305). Blood leukocyte DNAm was determined for 90 DNA samples using the Illumina MethylationEPIC chip. An epigenome-wide association study was performed to assess the relationship between Pb and DNAm. Individuals from Cerro de Pasco had higher Pb than individuals from Lima (p-value = 2.00E-16). Males had higher Pb than females (p-value = 2.36E-04). Pb was positively associated with hemoglobin (p-value = 8.60E-04). In Cerro de Pasco, blood Pb decreased with the distance from the mine (p-value = 0.04), and association with soil Pb was approaching significance (p-value = 0.08). We identified differentially methylated positions (DMPs) associated with genes SOX18, ZMIZ1, and KDM1A linked to neurological function. We also found 45 differentially methylated regions (DMRs), seven of which were associated with genes involved in metal ion binding and nine to neurological function and development. Our results demonstrate that even low levels of Pb can have a significant impact on the body including changes to DNAm. We report associations between Pb and hemoglobin, Pb and distance from mining, and between blood and soil Pb. We also report associations between loci- and region-specific DNAm and Pb. [ABSTRACT FROM AUTHOR]
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- 2021
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15. SENP1, but not fetal hemoglobin, differentiates Andean highlanders with chronic mountain sickness from healthy individuals among Andean highlanders.
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Hsieh, Matthew M., Callacondo, David, Rojas-Camayo, Jose, Quesada-Olarte, Jose, Wang, Xunde, Uchida, Naoya, Maric, Irina, Remaley, Alan T., Leon-Velarde, Fabiola, Villafuerte, Francisco C., and Tisdale, John F.
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FETAL hemoglobin , *HYPOXEMIA , *ERYTHROPOIETIN , *BLOOD plasma , *GENOTYPES - Abstract
Chronic mountain sickness (CMS) results from chronic hypoxia. It is unclear why certain highlanders develop CMS. We hypothesized that modest increases in fetal hemoglobin (HbF) are associated with lower CMS severity. In this cross-sectional study, we found that HbF levels were normal (median = 0.4%) in all 153 adult Andean natives in Cerro de Pasco, Peru. Compared with healthy adults, the borderline elevated hemoglobin group frequently had symptoms (headaches, tinnitus, cyanosis, dilatation of veins) of CMS. Although the mean hemoglobin level differed between the healthy (17.1 g/dL) and CMS (22.3 g/dL) groups, mean plasma erythropoietin (EPO) levels were similar (healthy, 17.7 mIU/mL; CMS, 12.02 mIU/mL). Sanger sequencing determined that single-nucleotide polymorphisms in endothelial PAS domain 1 ( EPAS1 ) and egl nine homolog 1 ( EGLN1 ), associated with lower hemoglobin in Tibetans, were not identified in Andeans. Sanger sequencing of sentrin-specific protease 1 ( SENP1 ) and acidic nuclear phosphoprotein 32 family, member D ( ANP32D ), in healthy and CMS individuals revealed that non-G/G genotypes were associated with higher CMS scores. No JAK2 V617F mutation was detected in CMS individuals. Thus, HbF and other classic erythropoietic parameters did not differ between healthy and CMS individuals. However, the non-G/G genotypes of SENP1 appeared to differentiate individuals with CMS from healthy Andean highlanders. [ABSTRACT FROM AUTHOR]
- Published
- 2016
- Full Text
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