Recruiting age influences male and female survival and population persistence in a long-lived tropical seabird

Abstract The lesser prairie-chicken Tympanuchus pallidicinctus has experienced significant declines in distribution and abundance since the early 1900s. A severe and prolonged drought from 2009 to 2013 resulted in further declines in population numbers and despite improved environmental and habitat conditions since 2013, populations of lesser prairie chickens have shown little improvement. To investigate whether breeding season survival of lesser prairie-chickens in eastern New Mexico could be driving this response, we developed the following objectives: 1) estimate male and female breeding-season survival; 2) determine whether male and female survival varies temporally among lekking, nesting, and brood-rearing periods; and 3) determine cause-specific mortality during the breeding season. We captured and radiocollared 76 lesser prairie-chickens (50 male, 26 female) during spring of 2014 and 2015 and estimated their survival throughout the breeding season (15 March–31 August). Male survival was nearly double that of females in both years (0.79–0.81 and 0.38–0.45, respectively). Males had similar survival across all periods (lekking, postlekking, late summer: 0.89–0.95). Females had the greatest period-specific survival during lekking and brood rearing (0.87 ± 0.08 and 0.85 ± 0.10, respectively) relative to the nesting period (0.58 ± 0.11). Mammalian predation was the primary cause of mortality in both years. Our results indicate that in New Mexico 1) lesser prairie-chicken breeding season survival was consistent with geographically similar studies, 2) females have lower survival during the nesting period, and 3) female lesser prairie-chicken survival was lower than male survival regardless of time period. Management actions that provide and protect high-quality nesting habitat may help ensure that female survival is maximized during the nesting period.

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Gonadal sex patterns p21-induced cellular senescence in mouse and human glioblastoma

10.1101/2021.06.02.446756 ◽

2021 ◽

Author(s):

Lauren Broestl ◽

Lucia Grandison ◽

Saraswati Shenoy ◽

Miranda M. Tallman ◽

Gina Rhee ◽

...

Keyword(s):

Sex Differences ◽

Mouse Model ◽

Cell Lines ◽

Cellular Senescence ◽

Therapeutic Response ◽

Cdk Inhibitor ◽

Male And Female ◽

Human Glioblastoma ◽

Female Survival ◽

Worse Prognosis

AbstractMales exhibit higher incidence and worse prognosis for the majority of cancers, including glioblastoma (GBM). Disparate survival may be related to sex-biased responses to treatment, including radiation. Using a mouse model of GBM, we show that female cells are more sensitive to radiation, and that senescence represents a major component of the radiation therapeutic response in both sexes. Correlation analyses revealed that the CDK inhibitor p21 and irradiation induced senescence were differentially regulated between male and female cells. Indeed, female cellular senescence was more sensitive to changes in p21 levels, a finding that was observed in both wildtype and transformed murine astrocytes and patient-derived GBM cell lines. Using a novel Four Core Genotypes model of GBM, we further show that sex differences in p21-induced senescence are patterned by gonadal sex. These data suggest that sex differences in p21 induced senescence contribute to the female survival advantage in GBM.

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Progression of the smoking epidemic in high-income regions and its effects on male-female survival differences: A populations-based analysis

10.21203/rs.2.13968/v2 ◽

2019 ◽

Author(s):

Maarten Wensink ◽

Jesús-Adrián Álvarez ◽

Silvia Rizzi ◽

Fanny Janssen ◽

Rune Lindahl-Jacobsen

Keyword(s):

Sex Differences ◽

North America ◽

Life Expectancy ◽

Time Lag ◽

High Income ◽

Attributable Mortality ◽

Birth Cohorts ◽

Male And Female ◽

Female Survival ◽

Survival Differences

Abstract BackgroundOf all lifestyle behaviours, smoking caused the most deaths in the last century. Because of the time lag between the act of smoking and dying from smoking, and because males generally take up smoking before females do, male and female smoking epidemiology often follows a typical double wave pattern dubbed the ‘smoking epidemic’. How are male and female deaths from this epidemic differentially progressing in high-income regions on a cohort-by-age basis? How have they affected male-female survival differences? MethodsWe used data for the period 1950-2015 from the WHO Mortality Database and the Human Mortality Database on three geographic regions that have progressed most into the smoking epidemic: high-income North America, high-income Europe and high-income Oceania. We examined changes in smoking-attributable mortality fractions as estimated by the Preston-Glei-Wilmoth method by age (ages 50-85) across birth cohorts 1870-1965. We used these to trace sex differences with and without smoking-attributable mortality in period life expectancy between ages 50 and 85. ResultsIn all three high-income regions, smoking explained up to 50% of sex differences in period life expectancy between ages 50 and 85 over the study period. These sex differences have declined since at least 1980, driven by smoking-attributable mortality, which tended to decline in males and increase in females overall. Thus, there was a convergence between sexes across recent cohorts. While smoking-attributable mortality was still increasing for older female cohorts, it was declining for females in the more recent cohorts in the US and Europe, as well as for males in all three regions.ConclusionsThe smoking epidemic contributed substantially to the male-female survival gap and to the recent narrowing of that gap in high-income North America, high-income Europe and high-income Oceania. The precipitous decline in smoking-attributable mortality in recent cohorts bodes somewhat hopeful. Yet, smoking-attributable mortality remains high, and therefore cause for concern.

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Progression of the smoking epidemic in high-income regions and its effects on male-female survival differences: a cohort-by-age analysis of 17 countries.

10.21203/rs.2.13968/v3 ◽

2019 ◽

Author(s):

Maarten Wensink ◽

Jesús-Adrián Álvarez ◽

Silvia Rizzi ◽

Fanny Janssen ◽

Rune Lindahl-Jacobsen

Keyword(s):

Sex Differences ◽

North America ◽

Life Expectancy ◽

Time Lag ◽

High Income ◽

Attributable Mortality ◽

Birth Cohorts ◽

Male And Female ◽

Female Survival ◽

Survival Differences

Abstract Background Of all lifestyle behaviours, smoking caused the most deaths in the last century. Because of the time lag between the act of smoking and dying from smoking, and because males generally take up smoking before females do, male and female smoking epidemiology often follows a typical double wave pattern dubbed the ‘smoking epidemic’. How are male and female deaths from this epidemic differentially progressing in high-income regions on a cohort-by-age basis? How have they affected male-female survival differences? MethodsWe used data for the period 1950-2015 from the WHO Mortality Database and the Human Mortality Database on three geographic regions that have progressed most into the smoking epidemic: high-income North America, high-income Europe and high-income Oceania. We examined changes in smoking-attributable mortality fractions as estimated by the Preston-Glei-Wilmoth method by age (ages 50-85) across birth cohorts 1870-1965. We used these to trace sex differences with and without smoking-attributable mortality in period life expectancy between ages 50 and 85. ResultsIn all three high-income regions, smoking explained up to 50% of sex differences in period life expectancy between ages 50 and 85 over the study period. These sex differences have declined since at least 1980, driven by smoking-attributable mortality, which tended to decline in males and increase in females overall. Thus, there was a convergence between sexes across recent cohorts. While smoking-attributable mortality was still increasing for older female cohorts, it was declining for females in the more recent cohorts in the US and Europe, as well as for males in all three regions.ConclusionsThe smoking epidemic contributed substantially to the male-female survival gap and to the recent narrowing of that gap in high-income North America, high-income Europe and high-income Oceania. The precipitous decline in smoking-attributable mortality in recent cohorts bodes somewhat hopeful. Yet, smoking-attributable mortality remains high, and therefore cause for concern.

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Predation on reproducing wolf spiders: access to information has differential effects on male and female survival

Animal Behaviour ◽

10.1016/j.anbehav.2017.03.032 ◽

2017 ◽

Vol 128 ◽

pp. 165-173 ◽

Cited By ~ 1

Author(s):

Ann L. Rypstra ◽

Chad D. Hoefler ◽

Matthew H. Persons

Keyword(s):

Access To Information ◽

Wolf Spiders ◽

Male And Female ◽

Differential Effects ◽

Female Survival

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Progression of the smoking epidemic in high-income regions and its effects on male-female survival differences: a cohort-by-age analysis of 17 countries

BMC Public Health ◽

10.1186/s12889-020-8148-4 ◽

2020 ◽

Vol 20 (1) ◽

Cited By ~ 2

Author(s):

Maarten Wensink ◽

Jesús-Adrián Alvarez ◽

Silvia Rizzi ◽

Fanny Janssen ◽

Rune Lindahl-Jacobsen

Keyword(s):

Sex Differences ◽

North America ◽

Life Expectancy ◽

Time Lag ◽

High Income ◽

Attributable Mortality ◽

Birth Cohorts ◽

Male And Female ◽

Female Survival ◽

Survival Differences

Abstract Background Of all lifestyle behaviours, smoking caused the most deaths in the last century. Because of the time lag between the act of smoking and dying from smoking, and because males generally take up smoking before females do, male and female smoking epidemiology often follows a typical double wave pattern dubbed the ‘smoking epidemic’. How are male and female deaths from this epidemic differentially progressing in high-income regions on a cohort-by-age basis? How have they affected male-female survival differences? Methods We used data for the period 1950–2015 from the WHO Mortality Database and the Human Mortality Database on three geographic regions that have progressed most into the smoking epidemic: high-income North America, high-income Europe and high-income Oceania. We examined changes in smoking-attributable mortality fractions as estimated by the Preston-Glei-Wilmoth method by age (ages 50–85) across birth cohorts 1870–1965. We used these to trace sex differences with and without smoking-attributable mortality in period life expectancy between ages 50 and 85. Results In all three high-income regions, smoking explained up to 50% of sex differences in period life expectancy between ages 50 and 85 over the study period. These sex differences have declined since at least 1980, driven by smoking-attributable mortality, which tended to decline in males and increase in females overall. Thus, there was a convergence between sexes across recent cohorts. While smoking-attributable mortality was still increasing for older female cohorts, it was declining for females in the more recent cohorts in the US and Europe, as well as for males in all three regions. Conclusions The smoking epidemic contributed substantially to the male-female survival gap and to the recent narrowing of that gap in high-income North America, high-income Europe and high-income Oceania. The precipitous decline in smoking-attributable mortality in recent cohorts bodes somewhat hopeful. Yet, smoking-attributable mortality remains high, and therefore cause for concern.

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Antagonistic effect of helpers on breeding male and female survival in a cooperatively breeding bird

Journal of Animal Ecology ◽

10.1111/1365-2656.12377 ◽

2015 ◽

Vol 84 (5) ◽

pp. 1354-1362 ◽

Cited By ~ 20

Author(s):

Matthieu Paquet ◽

Claire Doutrelant ◽

Ben J. Hatchwell ◽

Claire N. Spottiswoode ◽

Rita Covas

Keyword(s):

Antagonistic Effect ◽

Breeding Bird ◽

Male And Female ◽

Cooperatively Breeding ◽

Female Survival

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The Clinical, Roentgenological and Morphological Effects of an Acute Exposure of Phosgene on the Lungs of Dogs

Proceedings, annual meeting, Electron Microscopy Society of America ◽

10.1017/s0424820100065237 ◽

1971 ◽

Vol 29 ◽

pp. 236-237

Author(s):

R. F. Bils ◽

W. F. Diller ◽

F. Huth

Keyword(s):

Latent Period ◽

Chemical Industry ◽

Toxic Substance ◽

Lung Edema ◽

X Rays ◽

Beagle Dogs ◽

Male And Female ◽

Morphological Alterations ◽

Before And After ◽

Electron Microscopes

Phosgene still plays an important role as a toxic substance in the chemical industry. Thiess (1968) recently reported observations on numerous cases of phosgene poisoning. A serious difficulty in the clinical handling of phosgene poisoning cases is a relatively long latent period, up to 12 hours, with no obvious signs of severity. At about 12 hours heavy lung edema appears suddenly, however changes can be seen in routine X-rays taken after only a few hours' exposure (Diller et al., 1969). This study was undertaken to correlate these early changes seen by the roengenologist with morphological alterations in the lungs seen in the'light and electron microscopes.Forty-two adult male and female Beagle dogs were selected for these exposure experiments. Treated animals were exposed to 94.5-107-5 ppm phosgene for 10 min. in a 15 m3 chamber. Roentgenograms were made of the thorax of each animal before and after exposure, up to 24 hrs.

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Ultrastructural investigation of spontaneous pituitary gonadotroph cell adenomas in aging Sprague-Dawley rats

Proceedings, annual meeting, Electron Microscopy Society of America ◽

10.1017/s0424820100077086 ◽

1983 ◽

Vol 41 ◽

pp. 702-703

Author(s):

D. J. McComb ◽

J. Beri ◽

F. Zak ◽

K. Kovacs

Keyword(s):

Electron Microscopy ◽

Animal Model ◽

Epoxy Resin ◽

Immunoelectron Microscopy ◽

Tumor Type ◽

Gonadal Function ◽

Sprague Dawley ◽

Male And Female ◽

Reticulin Fibers ◽

Sprague Dawley Rats

Gonadotroph cell adenomas of the pituitary are infrequent in human patients and are not invariably associated with altered gonadal function. To date, no animal model of this tumor type exists. Herein, we describe spontaneous gonadotroph cell adenomas in old male and female Sprague-Dawley rats by histology, immunocytology and electron microscopy.The material consisted of the pituitaries of 27 male and 38 female Sprague Dawley rats, all 26 months of age or older, removed at routine autopsy. Sections of formal in-fixed, paraffin-embedded tissue were stained with hematoxylin-phloxine-saffron (HPS), the PAS method and the Gordon-Sweet technique for the demonstration of reticulin fibers. For immunostaining, sections were exposed to anti-rat β-LH, anti-ratβ-TSH, anti-rat PRL, anti-rat GH and anti-rat ACTH 1-39. For electron microscopy, tissue was fixed in 2.5% glutaraldehyde, postfixed in 1% OsO4 and embedded in epoxy-resin. Tissue fixed in 10% formalin, embedded in epoxy resin without osmification, was used for immunoelectron microscopy.

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Quantitative ultrastructural reconstruction of small regions within large volumes by correlative light and high voltage electron microscopy of serial 0.25-0.50 μm sections

Proceedings, annual meeting, Electron Microscopy Society of America ◽

10.1017/s0424820100127396 ◽

1987 ◽

Vol 45 ◽

pp. 578-581

Author(s):

Conly L. Rieder ◽

Frederick J. Miller ◽

Edwin Davison ◽

Samuel S. Bowser ◽

Kirsten Lewis ◽

...

Keyword(s):

Electron Microscopy ◽

High Voltage ◽

Mitotic Spindle ◽

Meiotic Spindle ◽

High Voltage Electron Microscopy ◽

Male And Female ◽

Voltage Electron ◽

High Voltage Electron ◽

Differential Stability ◽

Sperm Aster

In this abstract we Illustrate how same-section correlative light and high voltage electron microscopy (HVEM) of serial 0.25-0.50-μm sections can answer questions which are difficult to approach by EM of 60-100 nm sections.Starfish (Pisaster and Asterlas) eggs are fertilized at meiosis I when the oocyte contains two maternal centrosomes (e.g., asters) which form the poles of the first meiotic spindle. Immediately after fertilization a sperm aster is assembled in the vicinity of the male pronucleus and persists throughout meiosis. At syngamy the sperm aster splits to form the poles of the first mitotic spindle. During this time the functional and replicative properties of the maternal centrosome, inherited from the last meiotic division, are lost. The basis for this differential stability, of male and female centrosomes in the same cytoplasm, is a mystery.

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