62 research outputs found

    Vowel space area in later childhood and adolescence: Effects of age, sex and ease of communication

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    This study investigated vowel space area (VSA) development in childhood and adolescence and its impact on the ability to hyperarticulate vowels. In experiment 1, 96 participants aged 9-14 years carried out an interactive task when communication was easy (no barrier, 'NB') and difficult (the speech of one participant was filtered through a vocoder, 'VOC'). Previous recordings from 20 adults were used as reference. Measures of VSA (ERB2), F1 and F2 ranges (ERB) and articulation rate were obtained. Children's VSA were significantly larger than adults'. From the age of 11, vowel hyperarticulation was evident in VOC, but only because VSA were gradually reducing with age in NB. The results suggest that whilst large VSA do not prevent children from hyperarticulating vowels, the manner in which this is achieved may not be adult-like. Experiment 2 was conducted to verify that large VSA were not a by-product of children being unable to see each other. Thirteen participants carried out the same task face-to-face with their interlocutor. Comparisons to matched participants from experiment 1 showed no differences in VSA, indicating that the audio-only modality did not influence results. Possible reasons for larger VSA in the spontaneous speech of children and adolescents are discussed

    Novel immunohistochemistry-based signatures to predict metastatic site of triple-negative breast cancers

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    Background: Although distant metastasis (DM) in breast cancer (BC) is the most lethal form of recurrence and the most commonunderlying cause of cancer related deaths, the outcome following the development of DM is related to the site of metastasis.Triple negative BC (TNBC) is an aggressive form of BC characterised by early recurrences and high mortality. Athough multiplevariables can be used to predict the risk of metastasis, few markers can predict the specific site of metastasis. This study aimed atidentifying a biomarker signature to predict particular sites of DM in TNBC.Methods: A clinically annotated series of 322 TNBC were immunohistochemically stained with 133 biomarkers relevant to BC, todevelop multibiomarker models for predicting metastasis to the bone, liver, lung and brain. Patients who experienced metastasisto each site were compared with those who did not, by gradually filtering the biomarker set via a two-tailed t-test and Coxunivariate analyses. Biomarker combinations were finally ranked based on statistical significance, and evaluated in multivariableanalyses.Results: Our final models were able to stratify TNBC patients into high risk groups that showed over 5, 6, 7 and 8 times higher riskof developing metastasis to the bone, liver, lung and brain, respectively, than low-risk subgroups. These models for predictingsite-specific metastasis retained significance following adjustment for tumour size, patient age and chemotherapy status.Conclusions: Our novel IHC-based biomarkers signatures, when assessed in primary TNBC tumours, enable prediction of specificsites of metastasis, and potentially unravel biomarkers previously unknown in site tropism

    Endurance exercise diverts the balance between Th17 cells and regulatory T cells.

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    Endurance, marathon-type exertion is known to induce adverse changes in the immune system. Increased airway hyper-responsiveness and airway inflammation are well documented in endurance athletes and endurance exercise is considered a major risk factor for asthma in elite athletes. Yet, the mechanisms underlying this phenomenon are still to be deduced. We studied the effect of strenuous endurance exercise (marathon and half-ironman triathlon) on CD4+ lymphocyte sub-populations and on the balance between effector and regulatory CD4+ lymphocytes in the peripheral blood of trained athletes, Endurance exercise induced a significant increase in Th17 cells and a sustained decrease in peripheral blood regulatory T cells (Tregs). While interleukin (IL)-2 levels remained undetectable, post-race serum IL-6 and transforming growth factor (TGF) β levels were significantly elevated. Treg levels in sedentary controls' decreased in vitro after incubation with athletes' post-exercise serum, an effect that was attenuated by supplements of IL-2 or anti IL-6 neutralizing antibodies. Our data suggest that exercise-induced changes in serum cytokine levels promote alterations in Tregs and Th17 cell populations, which may divert the subtle balance in the immune system towards inflammation. This may explain allergic and autoimmune phenomena previously reported in endurance athletes and contribute to our understanding of exercise-related asthma
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