209 research outputs found
Immune-Neuroendocrine Interactions and Autoimmune Diseases
The relationship between immune-neuroendocrine system is firmly established. The messengers of this connection are hormones, neuropeptides, neurotransmitters and cytokines. The immune-neuroendocrine system have the capacity to synthesize and release these molecules, which, in turn, can stimulate or suppress the activity of immune or neuroendocrine cells by binding to receptors. In fact, hormones, neuropeptides and neurotransmitters participate in innate and adaptive immune response
A mosaic of phytoplankton responses across Patagonia, the SE Pacific and SW Atlantic Ocean to ash deposition and trace metal release from the Calbuco 2015 volcanic eruption
Following the April 2015 eruption of the Calbuco volcano, an extensive ash plume spread across northern Patagonia and into the SE Pacific and SW Atlantic Ocean. Here we report the results of field surveys conducted in the marine region receiving the highest ash load following the eruption (Reloncaví Fjord). The fortuitous location of a long-term monitoring station in Reloncaví Fjord provided data to evaluate inshore phytoplankton bloom dynamics and carbonate chemistry during April–May 2015. Satellite derived chlorophyll-a measurements over the ocean regions affected by the ash plume in May 2015 were obtained to determine the spatial-temporal gradient in offshore phytoplankton response to ash. Additionally, leaching experiments were performed to quantify the release of total alkalinity, trace elements (Fe, Mn, Pb, Co, Cu, Ni and Cd) and major ions (Fl, Cl, SO4, NO3, Li, Na, NH4, K, Mg, Ca) from ash into solution. Within Reloncaví Fjord, integrated peak diatom abundances during the May 2015 austral bloom were higher than usual (up to 1.4 × 1011 cells m−2, integrated to 15 m depth), with the bloom intensity perhaps moderated due to high ash loadings in the two weeks following the eruption. In the offshore SE Pacific, a short duration phytoplankton bloom corresponded closely in space and time to the maximum observed ash plume, potentially in response to Fe-fertilization of a region where phytoplankton growth is typically Fe-limited at this time of year. Conversely, no clear fertilization was found in the area subject to an ash plume over the SW Atlantic where the availability of fixed nitrogen is thought to limit phytoplankton growth which was consistent with no significant release of fixed nitrogen from ash.
In addition to release of nanomolar concentrations of dissolved Fe from ash suspended in seawater, it was observed that low loadings (< 5 mg L−1) of freshly deposited ash were an unusually prolific source of Fe(II) into solution (up to 1.0 µmol Fe g−1), suggesting that the release of bioaccessible Fe from ash sources may generally be under-estimated when quantified from aged ash. This release of Fe(II) may make freshly deposited ash an unusually efficient dissolved Fe source with the 18–38 % fraction of dissolved Fe released as Fe(II) from Calbuco ash roughly comparable to literature values for Fe released into seawater from aerosols collected over the Pacific Ocean
Data preprocessing workflow for exhaled breath analysis by GC/MS using open sources
© 2020 The Authors. This document is made available under the CC-BY 4.0 license. http://creativecommons.org/licenses/by /4.0/
This document is the Accepted version of a Published Work that appeared in final form in Scientifc Reports. To access the final edited and published work see https://doi.org/10.1038/s41598-020-79014-
Case-Control Analysis of the Impact of Anemia on Quality of Life in Patients with Cancer: A Qca Study Analysis
Anemia is a common condition in cancer patients and is associated with a wide variety
of symptoms that impair quality of life (QoL). However, exactly how anemia affects QoL in cancer
patients is unclear because of the inconsistencies in its definition in previous reports. We aimed to
examine the clinical impact of anemia on the QoL of cancer patients using specific questionnaires.
We performed a post-hoc analysis of a multicenter, prospective, case-control study. We included
patients with cancer with (cases) or without (controls) anemia. Participants completed the European
Organization for Research and Treatment of Cancer Quality of Life questionnaire version 3.0 (EORTC
QLQ-C30) and Euro QoL 5-dimension 3-level (EQ–5D–3L) questionnaire. Statistically significant
and clinically relevant differences in the global health status were examined. From 2015 to 2018,
365 patients were included (90 cases and 275 controls). We found minimally important differences in
global health status according to the EORTC QLQ-C30 questionnaire (case vs. controls: 45.6 vs. 58%,
respectively; mean difference: −12.4, p < 0.001). Regarding symptoms, cancer patients with anemia
had more pronounced symptoms in six out of nine scales in comparison with those without anemia.
In conclusion, cancer patients with anemia had a worse QoL both clinically and statistically
Serum tryptase monitoring in indolent systemic mastocytosis: association with disease features and patient outcome
This is an open-access article distributed under the terms of the Creative Commons Attribution License.-- et al.[Background]: Serum baseline tryptase (sBT) is a minor diagnostic criterion for systemic mastocytosis (SM) of undetermined prognostic impact. We monitored sBT levels in indolent SM (ISM) patients and investigated its utility for predicting disease behaviour and outcome. [Methods]: In total 74 adult ISM patients who were followed for ≥48 months and received no cytoreductive therapy were retrospectively studied. Patients were classified according to the pattern of evolution of sBT observed. [Results]: Overall 16/74 (22%) cases had decreasing sBT levels, 48 (65%) patients showed increasing sBT levels and 10 (13%) patients showed a fluctuating pattern. Patients with significantly increasing sBT (sBT slope ≥0.15) after 48 months of follow-up showed a slightly greater rate of development of diffuse bone sclerosis (13% vs. 2%) and hepatomegaly plus splenomegaly (16% vs. 5%), as well as a significantly greater frequency of multilineage vs. mast cells (MC)-restricted KIT mutation (p = 0.01) together with a greater frequency of cases with progression of ISM to smouldering and aggressive SM (p = 0.03), and a shorter progression-free survival (p = 0.03). [Conclusions]: Monitoring of sBT in ISM patients is closely associated with poor prognosis disease features as well as with disease progression, pointing out the need for a closer follow-up in ISM patients with progressively increasing sBT values.This work was supported by grants from the Fondo de Investigaciones Sanitarias (FIS) of the Ministerio de Ciencia e Innovación of Spain (RETICS RD06/0020/0035-FEDER and PS09/00032); Fundación Sociosanitaria de Castilla-La Mancha (FISCAM 2007/36, FISCAM 2010/008 and G-2010/C-002); Instituto de Salud Carlos III of the Ministerio de Economía y Competitividad of Spain (PI11/02399); Junta de Castilla y León (SAN/103/2011); Fundación Ramón Areces; Fundación Española de Mastocitosis (FEM 2010); Hospital Virgen de la Salud Biobank (BioB-HVS) supported by grant of RETICS RD09/0076/00074, (Toledo, Spain).Peer Reviewe
Mast cell-related disorders presenting with Kounis syndrome
Letter to the Editor.-- et al.Peer Reviewe
CD30 expression by bone marrow mast cells from different diagnostic variants of systemic mastocytosis
[Aims]: CD30 expression by bone marrow (BM) mast cells (MC) has been reported recently in systemic mastocytosis (SM) patients. The aim of this study was to investigate the potential diagnostic and prognostic value of CD30 expression in SM as assessed by multiparameter flow cytometry. [Methods and results]: A total of 163 consecutive BM samples corresponding to 142 SM patients and 21 non-mastocytosis cases were studied. CD30 was positive in most SM patients (80%), but in only one non-mastocytosis case (4.8%). When combined with CD25, CD30 contributed to an improved accuracy over that of CD25 alone (98% versus 93%) mainly because most (eight of nine) of the well-differentiated SM (WDSM), who lacked CD25, were CD30+. Similar levels of expression of CD30 were observed among all different subgroups of SM except mast cell leukaemia; among indolent SM (ISM) patients, no significant association was observed between the levels of CD30 expression and other clinical and biological features of the disease. [Conclusions]: The increased expression of CD30 associated with absence of CD25 contributes to the diagnosis of WDSM and its distinction from other subtypes of SM. By contrast, CD30 expression did not contribute either to prognostic stratification of ISM or to the differential diagnosis between ISM and aggressive SM cases.This work was supported by grants from the Fondo de Investigaciones Sanitarias (FIS) PI11/02399, PS09/00032 and RETICs RD09/0076/00133, RD09/0076/00074 and RD12/0036/0048 (FEDER) from the Instituto de Salud Carlos III, Ministerio de Economía
y Competitividad, Spain; Fundacion Sociosanitaria de Castilla-La Mancha (2010/008 y G-2010/C-002); Fundación Espanola de Mastocitosis (FEM 2010); and by a grant from Fundaçao para a Ciência e Tecnologia (FCT) of Portugal (SFRH/BD/22972/2005).Peer Reviewe
Detection of the KIT D816V mutation in peripheral blood of systemic mastocytosis: diagnostic implications
Recent studies have found the KIT D816V mutation in peripheral blood of virtually all adult systemic mastocytosis patients once highly sensitive PCR techniques were used; thus, detection of the KIT D816V mutation in peripheral blood has been proposed to be included in the diagnostic work-up of systemic mastocytosis algorithms. However, the precise frequency of the mutation, the biological significance of peripheral blood-mutated cells and their potential association with involvement of bone marrow hematopoietic cells other than mast cells still remain to be investigated. Here, we determined the frequency of peripheral blood involvement by the KIT D816V mutation, as assessed by two highly sensitive PCR methods, and investigated its relationship with multilineage involvement of bone marrow hematopoiesis. Overall, our results confirmed the presence of the KIT D816V mutation in peripheral blood of most systemic mastocytosis cases (161/190; 85%)-with an increasing frequency from indolent systemic mastocytosis without skin lesions (29/44; 66%) to indolent systemic mastocytosis with skin involvement (124/135; 92%), and more aggressive disease subtypes (11/11; 100%)-as assessed by the allele-specific oligonucleotide-qPCR method, which was more sensitive (P<.0001) than the peptide nucleic acid-mediated PCR approach (84/190; 44%). Although the presence of the KIT mutation in peripheral blood, as assessed by the allele-specific oligonucleotide-qPCR technique, did not accurately predict for multilineage bone marrow involvement of hematopoiesis, the allele-specific oligonucleotide-qPCR allele burden and the peptide nucleic acid-mediated-PCR approach did. These results suggest that both methods provide clinically useful and complementary information through the identification and/or quantification of the KIT D816V mutation in peripheral blood of patients suspected of systemic mastocytosis.This work was supported in part by grants from the Fondo de Investigaciones Sanitarias (FIS; grant number PI11/02399, FEDER) and Red Temática de
Investigación Cooperativa en Cancer (RTICC; grant number RD12/0036/0048, FEDER) of the Instituto deSalud Carlos III (Ministry of Economy and Competitivity, Madrid, Spain), from Fundacion Ramon Areces (Madrid, Spain; grant number CIVP16A1806) and from Ayudas a Proyectos de Investigación en
Salud de la Fundación Mutua Madrileña 2014 and Asociación Española de Enfermos de Mastocitosis (AEDM 2014). The National DNA Bank is supported
by grants from the Instituto de Salud Carlos III of the Ministerio de Economia y Competitividad of Spain (grand numbers PT13/0001/0037 and PT13/0010/
0067, FEDER). AM was supported by RTICC.Peer Reviewe
Clinical, immunophenotypic, and molecular characteristics of well-differentiated systemic mastocytosis
[Background]: Well-differentiated systemic mastocytosis (WDSM) is a rare variant of systemic mastocytosis (SM) characterized by bone marrow (BM) infiltration by mature-appearing mast cells (MCs) often lacking exon 17 KIT mutations. Because of its rarity, the clinical and biological features of WDSM remain poorly defined. [Objective]: We sought to determine the clinical, biological, and molecular features of a cohort of 33 patients with mastocytosis in the skin in association with BM infiltration by well-differentiated MCs and to establish potential diagnostic criteria for WDSM. Methods Thirty-three patients with mastocytosis in the skin plus BM aggregates of round, fully granulated MCs lacking strong CD25 and CD2 expression in association with clonal MC features were studied. [Results]: Our cohort of patients showed female predominance (female/male ratio, 4:1) and childhood onset of the disease (91%) with frequent familial aggregation (39%). Skin involvement was heterogeneous, including maculopapular (82%), nodular (6%), and diffuse cutaneous (12%) mastocytosis. KIT mutations were detected in only 10 (30%) of 33 patients, including the KIT D816V (n = 5), K509I (n = 3), N819Y (n = 1), and I817V (n = 1) mutations. BM MCs displayed a unique immunophenotypic pattern consisting of increased light scatter features, overexpression of cytoplasmic carboxypeptidase, and aberrant expression of CD30, together with absent (79%) or low (21%) positivity for CD25, CD2, or both. Despite only 9 (27%) of 33 patients fulfilling the World Health Organization criteria for SM, our findings allowed us to establish the systemic nature of the disease, which fit with the definition of WDSM. [Conclusions]: WDSM represents a rare clinically and molecularly heterogeneous variant of SM that requires unique diagnostic criteria to avoid a misdiagnosis of cutaneous mastocytosis per current World Health Organization criteria.Supported by grants from Asociación Española de Mastocitosis, Madrid, Spain (grant AEDM 2014); Instituto de Salud Carlos III, FEDER, Ministry of Economy and Competitivity, Madrid, Spain (grant PI11/02399); Fundación Ramón Areces, Madrid, Spain (grant CIVP16A1806); and Novartis Farmacéutica, S.A., Spain. I. Alvarez-Twose has received research support from Novartis Farmacéutica, S.A., Spain. A. García-Montero has received
research support from Fundacion Ramon Areces (grant no. CIVP16A1806) and ISCIII
Ministerio de Economia y Competitividad (grant no. PI11/02399). A. Orfao has
received research support from Fundacion Ramon Areces (grant no. CIVP16A1806).Peer Reviewe
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