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Aim: It can be challenging to distinguish COVID-19 in children from other common infections. We set out to determine the rate at which children consulting a primary care paediatrician with an acute infection are infected with SARS-CoV-2 and to compare distinct findings. Method: In seven out-patient clinics, children aged 0–13 years with any new respiratory or gastrointestinal symptoms and presumed infection were invited to be tested for SARS-CoV-2. Factors that were correlated with testing positive were determined. Samples were collected from 25 January 2021 to 01 April 2021. Results: Seven hundred and eighty-three children participated in the study (median age 3 years and 0 months, range 1 month to 12 years and 11 months). Three hundred and fifty-eight were female (45.7%). SARS-CoV-2 RNA was detected in 19 (2.4%). The most common symptoms in children with as well as without detectable SARS-CoV-2 RNA were rhinitis, fever and cough. Known recent exposure to a case of COVID-19 was significantly correlated with testing positive, but symptoms or clinical findings were not. Conclusion: COVID-19 among the children with symptoms of an acute infection was uncommon, and the clinical presentation did not differ significantly between children with and without evidence of an infection with SARS-CoV-2.
The majority of excitatory synapses terminating on cortical neurons are found on dendritic spines. The geometry of spines, in particular the size of the spine head, tightly correlates with the strength of the excitatory synapse formed with the spine. Under conditions of synaptic plasticity, spine geometry may change, reflecting functional adaptations. Since the cytokine tumor necrosis factor (TNF) has been shown to influence synaptic transmission as well as Hebbian and homeostatic forms of synaptic plasticity, we speculated that TNF-deficiency may cause concomitant structural changes at the level of dendritic spines. To address this question, we analyzed spine density and spine head area of Alexa568-filled granule cells in the dentate gyrus of adult C57BL/6J and TNF-deficient (TNF-KO) mice. Tissue sections were double-stained for the actin-modulating and plasticity-related protein synaptopodin (SP), a molecular marker for strong and stable spines. Dendritic segments of TNF-deficient granule cells exhibited ∼20% fewer spines in the outer molecular layer of the dentate gyrus compared to controls, indicating a reduced afferent innervation. Of note, these segments also had larger spines containing larger SP-clusters. This pattern of changes is strikingly similar to the one seen after denervation-associated spine loss following experimental entorhinal denervation of granule cells: Denervated granule cells increase the SP-content and strength of their remaining spines to homeostatically compensate for those that were lost. Our data suggest a similar compensatory mechanism in TNF-deficient granule cells in response to a reduction in their afferent innervation.
Grundlagen: Das Neuroblastom ist der häufigste extrakranielle solide Tumor im Kindesalter. Die Patienten in der Hochrisikogruppe haben trotz der Weiterentwicklung der Therapie immer noch eine sehr schlechte Prognose. Die Entwicklung von Resistenzen und die darauffolgende Progression der Erkrankung sind kennzeichnende Phänomene innerhalb dieser Patientengruppe.
Die hier vorgestellte Charakterisierung von MYCN amplifizierten, Cisplatin adaptierten chemoresistenten Neuroblastomsublinien UKF-NB-3rCDDP1000 I bis XII ist eine grundlegende Aufgabe, um den Phänotyp des multiresistenten/ Hochrisiko Neuroblastoms besser zu verstehen. Des Weiteren könnte diese Charakterisierung zu einem besseren Verständnis der Rolle von Krebsstammzellen beim Neuroblastom führen.
Methoden: Die Empfindlichkeit zu verschiedenen Zytostatika wurde im Viabilitätsassay untersucht. Die Expression mehrerer Stammzellmarker wurde durch Durchflusszytometrie überprüft. Im Western Blot wurde die Expression der Proteine p53, p21, XIAP und Survivin untersucht. Die Proliferation der verschiedenen Sublinien wurde durch den Kolonienbildungstest untersucht.
Ergebnise: In dieser Arbeit wurde nachgewiesen, dass die Cisplatin adaptierten Sublinien zusätzliche Resistenzen gegenüber weiteren klassischen Zytostatika zeigen. Abgesehen von der erworbenen Cisplatin-Resistenz zeigen die
Cisplatinsublinien erhöhte IC50-Werte für die Wirkstoffe YM-155, Doxorubicin, Melphalan, Vincristin, Docetaxel, Etoposid, Carboplatin und Vinblastin (jeweils im Vergleich zu UKF-NB-3). Von den getesteten klassischen Zytostatika hat nur Gemcitabin bei den Cisplatin adaptierten Sublinien eine gute Wirksamkeit. In dieser Arbeit konnte die Expression von mehreren Stammzellmarkern, sowohl bei den Cisplatin resistenten Sublinien als auch bei der parentalen Zelle UKFNB-3, nachgewiesen werden. Durch die Cisplatinadaptierung ergaben sich Unterschiede in der Expression von CD-133, Nanog, Nestin, Sox-2 und GD2. Im Kolonienbildungstest konnten keine großen Unterschiede festgestellt werden, die
Cisplatin-adaptierten Sublinien zeigen tendenziell eine geringere Kolonienbildung als UKF-NB-3.
Konklusion: Der Nachweis von unterschiedlichen Stammzellmarkern bei den Neuroblastomsublinien UKF-NB-3rCDDP1000 I bis XII ist ein wichtiger Hinweis für die Existenz von Zellen mit Stammzellfähigkeiten innerhalb der Sublinien.
Durch ein besseres Verständnis der biologischen Merkmale in resistenten Neuroblastomzellen könnten neuartige gezielte Therapiestrategien entdeckt werden. Viele der bei dieser Arbeit untersuchten Moleküle vermögen einen Effekt bei der Entstehung von Resistenzen und bei Aufrechterhaltung der Proliferation und Überleben von Neuroblastomzellen sowie Neuroblastomkrebsstammzellen zu haben. Folglich könnten diese Zielmoleküle (CD-133, Nanog, Nestin, Sox-2 und GD2) in der Zukunft benutzt werden, um neue therapeutische Strategien zu entwickeln, die sowohl die multiresistenten Neuroblastomzellen als auch die Neuroblastom-krebsstammzellen besser abtöten können. Zusätzlich ist Gemcitabin als Medikament nach Cisplatintherapie klinisch interessant.
In der Akuten Lymphatischen Leukämie (ALL) im Erwachsenenalter beträgt die 5–Jahres-Überlebensrate trotz verbesserter Therapien unter 40%. Die Prognose wird durch das Auftreten von Rezidiven signifikant verschlechtert. ALL entsteht durch genetische Veränderungen lymphatischer Vorläuferzellen im Knochenmark, welche zu einem Differenzierungsblock und zu starker Zunahme der Vorläufer-zellen führen. Eine mögliche Erklärung für das bestehende hohe Rezidiv-Risiko wird in der unvollständigen Elimination von Leukämie-induzierenden Zellen (LIZ) durch die Primärtherapie gesehen. Die Identifizierung und Charakterisierung von LIZ in der ALL anhand spezifischer Oberflächenmarker war bisher nicht möglich, daher ist die molekulare und funktionelle Charakterisierung von LIZ für die Entwicklung moderner Therapieansätze unabdingbar. Metabolische Analysen primärer ALL-Langzeitkulturen (LZK) in Vorarbeiten zeigten eine deutliche Abweichung des Kohlenhydratstoffwechsels vom physiologischen metabolischen Profil einer Knochenmarkszelle hin zur Nutzung der Glykolyse mit zunehmendem leukämogenen Potential der etablierten LZK. Folglich ist in dieser Dissertation der Zusammenhang zwischen höherer Glukoseaffinität, schnellerer Glukoseaufnahme und dem Vorliegen eines höheren leukämogenen Potentials der Zellen und damit einer Definition der LIZ anhand ihres Energiestoffwechsels untersucht worden.
Hierfür wurden Tests im Mausmodell in vivo und in vitro mit drei ALL-LZK CR, PH und BV durchgeführt. Wir etablierten unter Verwendung des fluoreszenzmarkierten Glukoseanalogons 2–NBDG sowie eines gegen den GLUT–1 gerichteten Antikör-pers jeweils ein durchflusszytometrisches Verfahren zur quantitativen Messung der Glukoseaufnahme. Anhand dieser Parameter erfolgte die FACS-Anreicherung unterschiedlicher Zellpopulationen der LZK und die Xenotransplantation zur Evaluation potentieller Unterschiede des leukämogenen Potentials.
Durch durchflusszytometrische Messungen konnten in den drei LZK jeweils drei Subpopulationen von Zellen anhand ihrer Glukoseaffinität unterschieden werden (2–NBDG negativ, 2–NBDG positiv und 2–NBDG hochaffin). Auch zeigten sich Unterschiede in der Kinetik der Glukoseaufnahme der drei getesteten LZK, wobei CR Zellen mit Abstand am schnellsten 2–NBDG aufnahmen, gefolgt von PH. Die schnellere Glukoseaufnahme der LZK CR und PH wurde durch eine vermehrte Expression des GLUT-1 Rezeptors und einen höheren Anteil an GLUT–1 positiver Zellen hervorgerufen. Interessanterweise bestand auch eine Korrelation zwischen höherem leukämogenem Potential mit schnellerer Glukoseaufnahme und stärkerer GLUT–1 Expression. Hierbei zeigte sich, dass die HIF-1α Stabilisierung unter Normoxie in einer vermehrten GLUT–1 Expression und daraufhin vermehrter Glukoseaufnahme resultierte. Die prospektive Anreicherung von distinkten Zellsubpopulationen der LZK CR und PH aufgrund ihrer Glukoseaufnahme (gemessen durch 2–NBDG) und Transplantation der sortierten Zellpopulationen in NSG Empfängermäuse zeigte keine kohärente Beziehung zwischen der Glukoseaffinität der Zellen und der Entwicklung der Leukämie. Während es bei CR Zellen initial zu einer beschleunigten Expansion der 2–NBDG-positiv sortierten Leukämiezellen kommt, was sich aber nicht signifikant auf das Gesamtüberleben der Empfängermäuse auswirkt, zeigte die serielle Transplantation von 2–NBDG negativen Zellen ein schnelleres Ableben der Tiere. Bei der LZK PH expandierten 2–NBDG-negative Zellen schneller in primären Empfängermäusen als positive Zellen. Dabei konnten zelltoxische Effekte durch die Verwendung von 2–NBDG ausgeschlossen werden. Auch die Transplantation von GLUT-1 positiven bzw. negativen CR Zellen zeigte, dass GLUT-1 negative Zellen schneller in den Mäusen expandierten, eine aggressivere Leukämie verursachten und zu einem früheren Ableben der Mäuse führte.
Diese Ergebnisse zeigen keine unmittelbare Korrelation von Glukoseaufnahme oder GLUT-1 Expression und der Leukämogenität der untersuchten ALL Zellen. Daher können diese Eigenschaften nicht dazu verwendet werden LIZ in ALL prospektiv anzureichern. Im Rahmen dieser Dissertation zeigte sich aber auch, dass sich die LZK in ihrer jeweiligen Gesamtpopulation bezüglich ihres Glukoseaufnahmeverhaltens und ihrem Anteil GLUT-1-positiver Zellen unterschieden. Weiterführende Untersuchungen sind nötig, um den Grund der differentiellen Expression von GLUT-1 und der damit zusammenhängenden gesteigerten Glukoseaufnahme einzelner Zellen in der ALL zu ermitteln.
Stereotaktische Biospien gehören seit vielen Jahren zu den Standardoperationen zahlreicher neurochirurgischer Kliniken. Hierbei werden Proben von Hirnläsionen entnommen, um diese histopathologisch zu untersuchen.
Die histopathologische Diagnose unklarer Hirnläsionen ist zwingend erforderlich, um eine adäquate Therapie durchzuführen. Eine weitere Therapie kann aus Bestrahlung, Chemotherapie, Kombination beider oder Resektion bestehen. In wenigen Fällen wird eine zweite oder dritte Biopsie benötigt, um eine endgültige Diagnose zu erhalten. Das Ziel dieser Studie war es, jene Patienten genauer zu untersuchen, bei denen die erste Biopsie kein definitives Ergebnis erbracht hatte. Die meisten dieser Patienten mussten sich einer zweiten Biopsie unterziehen. Wir haben eine umfassende Recherche der letzten 10 Jahre durchgeführt und eine Datenbank mit den Patienten erstellt, bei denen die erste Biopsie kein Ergebnis erbracht hatte.
Hierbei wurden klinische Parameter, welche einen Einfluss auf die nicht zielführenden Biopsie haben können, erhoben, beschrieben und diskutiert. Die Parameter umfassten die entnommene Probenanzahl, Kontrastmittelaufnahme der Läsion, Lokalisation der Läsion, Erfahrung des Operateurs, neuroradiologische Verdachtsdiagnose und Vorbehandlung.
Wir haben in dieser retrospektiven Arbeit unser Augenmerk auf die klinischen Aspekte der einzelnen Patienten, bei denen die erste Biopsie kein definitives Ergebnis erbrachte, gelegt.
Hier zeigten sich keinerlei Auffälligkeiten, welche positiv mit einer nichtzielführenden Biopsie einhergehen könnten.
Wir folgern, dass in den meisten Fällen eine definitive Diagnose zu erwarten ist. Unklar bleibt, bei welchen Patienten keine zielführende Biopsie erfolgen wird, so dass sie einer erneuten Biopsie unterzogen werden müssen.
Beim Auffinden menschlicher Überreste stellt sich neben der Beurteilung des postmortalen Intervalls auch konsequent die Frage nach der Möglichkeit des Vorliegens eines Tötungsdelikts. Da Weichgewebe nur in begrenztem Ausmaß Verwesung, Fäulnis oder Umwelteinflüssen standhält, ist dieses nur bedingt geeignet, auch langfristig Spuren von Gewalteinwirkung zu konservieren. Knochengewebe hingegen kann Läsionen noch nach langen Zeiträumen nahezu unverändert abbilden und stellt somit einen forensisch bedeutenden Spurenträger dar.
Im Rahmen dieser retrospektiven Studie sollte geklärt werden, inwieweit und in welchem Ausmaß bei Tötungsdelikten knöcherne Verletzungen entstehen. Ob bei definierten Formen letaler Gewalteinwirkung unterschiedliche Häufigkeiten des Auftretens knöcherner Verletzungen zu beobachten und zudem bevorzugte Körperregionen zu identifizieren sind, stellte eine weitere wesentliche Fragestellung der Arbeit dar.
Nach Auswertung der Sektionsprotokolle von insgesamt 897 im Institut für Rechtsmedizin in Frankfurt am Main obduzierten, im In- und Ausland begangenen Tötungsdelikten im Zeitraum 01.01.1994 bis 31.12.2014 zeigte sich, dass unabhängig von der Art der tödlichen Gewalteinwirkung 70,9% der Opfer mindestens eine knöcherne Verletzung aufwiesen und darüber hinaus bei insgesamt 45,5% der Opfer mehrfache knöcherne Verletzungen nachgewiesen werden konnten.
Zudem zeigte sich, dass unterschiedliche, definierte letale Gewalteinwirkungen entsprechend charakteristische Häufigkeiten und Verteilungen knöcherner Verletzungen zur Folge haben. So sind mit 92,6 % die häufigsten knöchernen Läsionen bei Schussopfern festzustellen. Nach stumpfer und scharfer Gewalt mit je 80 % und 66,3 % ließ sich auch nach tödlicher Gewalteinwirkung gegen den Hals in 53,3 % der Fälle mindestens eine knöcherne Läsion nachweisen.
Das Fehlen knöcherner Verletzungen in insgesamt 29% der im Auswertungszeitraum untersuchten 897 Tötungsdelikte zeigt auch, dass selbst bei knöchern unversehrten, vollständigen Skelettfunden ein Homizid keineswegs ausgeschlossen werden kann. Neben der gerichtlichen Leichenöffnung sind stets ergänzende forensische Aufarbeitungen der menschlichen Überreste zu fordern. Hierbei sind einerseits physikalische und chemische Methoden in Betracht zu ziehen, vor allem jedoch auch radiologische Untersuchungen. Weitere Untersuchungen der gewonnenen Ergebnisse im Rahmen einer weiteren Studie sollen klären, welcher Stellenwert der postmortalen Computertomographie zugesprochen werden kann.
Correction to: Infection (2020) 48:723–733 https://doi.org/10.1007/s15010-020-01469-6. The original version of this article unfortunately contained a mistake. In this article the authors Dirk Schürmann at affiliation Charité, University Medicine, Berlin, Olaf Degen at affiliation University Clinic Hamburg Eppendorf, Hamburg and Heinz-August Horst at affiliation University Hospital Schleswig–Holstein, Kiel, Germany were missing from the author list. The original article has been corrected.
Objective: Prisoners constitute a high-risk group for suicide, with suicide rates about 5 to 8 times higher than in the general population. The first weeks of imprisonment are a particularly vulnerable time, but there is limited knowledge about the risk factors for either early or late suicide events. Methods: Based on a national total sample of prison suicides in Germany between 2005 and 2017, suicides within the first 2 (4 and 8) weeks after reception into prison were matched by age and penalty length with cases that occurred later. Factors that potentially influence the timing of suicide were investigated. Results: The study has shown that 16.7% (31.5%) of all 390 suicides in German prisons occurred within the first two weeks (two months) of imprisonment. Factors that facilitate adaptation to the prison environment (e.g. prior prison experience) were negatively associated with early suicide events. Factors that hindered the adaptation process (e.g. withdrawal from illicit drugs) were observed more frequently in early suicide events than in late ones. These factors are active at different times of imprisonment. Conclusion: At reception, particular attention should be paid to the following factors associated with early suicide events: widowed marital status, lack of prison experience, and drug dependency.
Objective. We investigated the health-related quality of life (HRQoL) of patients with gastrointestinal stromal tumours (GIST). Methods: In the multicentre PROSa study, the HRQoL of adult GIST patients was assessed between 2017 and 2019 using the European Organisation for Research and Treatment of Cancer HRQoL questionnaire (EORTC QLQ-C30). We performed group comparisons and multivariate linear regressions. Results: Among 130 patients from 13 centres, the mean global HRQoL was 63.3 out of 100 points. Higher sores indicate better HRQoL. The highest restrictions were in emotional, social, role functioning, insomnia, fatigue, and pain. In multivariate linear regression, we found no significant differences between patients receiving tyrosine kinase inhibitor (TKI) treatment and those without TKI treatment as well as between patients treated with curative or with palliative intent. Patients who received multiple lines of TKI treatment had the most restrictions, notably in physical (unstandardized regression coefficient [B] = −15.7), role (B = −25.7), social (B = −18.4), and cognitive functioning (B = −19.7); fatigue (B = 15.93); general health (B = −14.23); and EORTC-sum score (B = −13.82) compared to all other patients. Conclusion: The highest HRQoL restrictions were in GIST patients receiving multiple lines of TKI therapy. Underlying causes need further investigation.
Objective: Using multimodal imaging, we tested the hypothesis that patients after hemispherotomy recruit non-primary motor areas and non-pyramidal descending motor fibers to restore motor function of the impaired limb. Methods: Functional and structural MRI data were acquired in a group of 25 patients who had undergone hemispherotomy and in a matched group of healthy controls. Patients’ motor impairment was measured using the Fugl-Meyer Motor Assessment. Cortical areas governing upper extremity motor-control were identified by task-based functional MRI. The resulting areas were used as nodes for functional and structural connectivity analyses. Results: In hemispherotomy patients, movement of the impaired upper extremity was associated to widespread activation of non-primary premotor areas, whereas movement of the unimpaired one and of the control group related to activations prevalently located in the primary motor cortex (all p ≤ 0.05, FWE-corrected). Non-pyramidal tracts originating in premotor/supplementary motor areas and descending through the pontine tegmentum showed relatively higher structural connectivity in patients (p < 0.001, FWE-corrected). Significant correlations between structural connectivity and motor impairment were found for non-pyramidal (p = 0.023, FWE-corrected), but not for pyramidal connections. Interpretation: A premotor/supplementary motor network and non-pyramidal fibers seem to mediate motor function in patients after hemispherotomy. In case of hemispheric lesion, the homologous regions in the contralesional hemisphere may not compensate the resulting motor deficit, but the functionally redundant premotor network.
Ependymomas encompass a heterogeneous group of central nervous system (CNS) neoplasms that occur along the entire neuroaxis. In recent years, extensive (epi-)genomic profiling efforts have identified several molecular groups of ependymoma that are characterized by distinct molecular alterations and/or patterns. Based on unsupervised visualization of a large cohort of genome-wide DNA methylation data, we identified a highly distinct group of pediatric-type tumors (n = 40) forming a cluster separate from all established CNS tumor types, of which a high proportion were histopathologically diagnosed as ependymoma. RNA sequencing revealed recurrent fusions involving the pleomorphic adenoma gene-like 1 (PLAGL1) gene in 19 of 20 of the samples analyzed, with the most common fusion being EWSR1:PLAGL1 (n = 13). Five tumors showed a PLAGL1:FOXO1 fusion and one a PLAGL1:EP300 fusion. High transcript levels of PLAGL1 were noted in these tumors, with concurrent overexpression of the imprinted genes H19 and IGF2, which are regulated by PLAGL1. Histopathological review of cases with sufficient material (n = 16) demonstrated a broad morphological spectrum of tumors with predominant ependymoma-like features. Immunohistochemically, tumors were GFAP positive and OLIG2- and SOX10 negative. In 3/16 of the cases, a dot-like positivity for EMA was detected. All tumors in our series were located in the supratentorial compartment. Median age of the patients at the time of diagnosis was 6.2 years. Median progression-free survival was 35 months (for 11 patients with data available). In summary, our findings suggest the existence of a novel group of supratentorial neuroepithelial tumors that are characterized by recurrent PLAGL1 fusions and enriched for pediatric patients.
Background: Compound flaps offer the advantage of one stage defect reconstruction respecting all relevant tissues and early functional recovery by optimal vascularity of all components. Due to its specific vascular anatomy and the three-dimensional donor site, compound flaps with bone components may result in higher complication rates compared to soft tissue compound flaps. The meta-analysis summarizes the available evidence and evaluates whether bone components are a risk factor for periprocedural complications in upper extremity multidimensional defect reconstruction. Method: PubMed and Embase were searched for all publications addressing compound free flaps for upper extremity defect reconstruction with bone or soft tissue components published between January 1988 and May 2018. The methodological quality was assessed with the American Society of Plastic Surgeons Evidence Rating Scale for Therapeutic Studies. Flap loss, thrombosis rate, early infection, hematoma, seroma, as well as donor site complications were extracted and analyzed. Results: Twelve out of 1157 potentially eligible studies (evidence-III) comprising 159 patients were finally included with publication bias for all summarized complication rates. Complication rates for flaps with/ without bone components were: total flap loss 5%, 95% CI = 3%–10% (6%/5%); partial flap loss 8%, 95% CI = 5%–15%, (9%/8%); arterial/venous thrombosis 7%, 95% CI = 4%–12%, (8%/5%)/14%, 95% CI = 9%–21% (16%/6%, P < .05) with higher risk for flaps with bone components; infection 6%, 95% CI = 3%–12% (6%/6%); hematoma 6%, 95% CI = 3%–11% (6%/5%); seroma 5%, 95% CI = 3%–10% (5%/5%); dehiscence 10%, 95% CI = 6%–17% (11%/9%). Conclusion: Compound flaps for upper extremity defect reconstruction including bone components have a higher venous thrombosis rate compared to compound soft-tissue flaps.
Scores to identify patients at high risk of progression of coronavirus disease (COVID-19), caused by the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), may become instrumental for clinical decision-making and patient management. We used patient data from the multicentre Lean European Open Survey on SARS-CoV-2-Infected Patients (LEOSS) and applied variable selection to develop a simplified scoring system to identify patients at increased risk of critical illness or death. A total of 1946 patients who tested positive for SARS-CoV-2 were included in the initial analysis and assigned to derivation and validation cohorts (n = 1297 and n = 649, respectively). Stability selection from over 100 baseline predictors for the combined endpoint of progression to the critical phase or COVID-19-related death enabled the development of a simplified score consisting of five predictors: C-reactive protein (CRP), age, clinical disease phase (uncomplicated vs. complicated), serum urea, and D-dimer (abbreviated as CAPS-D score). This score yielded an area under the curve (AUC) of 0.81 (95% confidence interval [CI]: 0.77–0.85) in the validation cohort for predicting the combined endpoint within 7 days of diagnosis and 0.81 (95% CI: 0.77–0.85) during full follow-up. We used an additional prospective cohort of 682 patients, diagnosed largely after the “first wave” of the pandemic to validate the predictive accuracy of the score and observed similar results (AUC for the event within 7 days: 0.83 [95% CI: 0.78–0.87]; for full follow-up: 0.82 [95% CI: 0.78–0.86]). An easily applicable score to calculate the risk of COVID-19 progression to critical illness or death was thus established and validated.
Background: Number of positive prostate biopsy cores represents a key determinant between high versus very high-risk prostate cancer (PCa). We performed a critical appraisal of the association between the number of positive prostate biopsy cores and CSM in high versus very high-risk PCa. Methods: Within Surveillance, Epidemiology, and End Results database (2010–2016), 13,836 high versus 20,359 very high-risk PCa patients were identified. Discrimination according to 11 different positive prostate biopsy core cut-offs (≥2–≥12) were tested in Kaplan–Meier, cumulative incidence, and multivariable Cox and competing risks regression models. Results: Among 11 tested positive prostate biopsy core cut-offs, more than or equal to 8 (high-risk vs. very high-risk: n = 18,986 vs. n = 15,209, median prostate-specific antigen [PSA]: 10.6 vs. 16.8 ng/ml, <.001) yielded optimal discrimination and was closely followed by the established more than or equal to 5 cut-off (high-risk vs. very high-risk: n = 13,836 vs. n = 20,359, median PSA: 16.5 vs. 11.1 ng/ml, p < .001). Stratification according to more than or equal to 8 positive prostate biopsy cores resulted in CSM rates of 4.1 versus 14.2% (delta: 10.1%, multivariable hazard ratio: 2.2, p < .001) and stratification according to more than or equal to 5 positive prostate biopsy cores with CSM rates of 3.7 versus 11.9% (delta: 8.2%, multivariable hazard ratio: 2.0, p < .001) in respectively high versus very high-risk PCa. Conclusions: The more than or equal to 8 positive prostate biopsy cores cutoff yielded optimal results. It was very closely followed by more than or equal to 5 positive prostate biopsy cores. In consequence, virtually the same endorsement may be made for either cutoff. However, more than or equal to 5 positive prostate biopsy cores cutoff, based on its existing wide implementation, might represent the optimal choice.
Ataxia-telangiectasia (A-T) is a hereditary immune system disorder with neurodegeneration. Its first neurologic symptoms include ataxic gait in early childhood, with slowly progressive cerebellar ataxia, oculomotor apraxia, oculocutaneous telangiectasia, and progressive muscle weakness. Neonatal screening for severe T-cell deficiency was recently found to diagnose A-T patients with a significantly reduced naïve T-cell pool. Our study includes 69 A-T patients between 8 January 2002 and 1 December 2019. Nineteen cases of cancer were diagnosed in 17 patients (25%), with a median overall survival [OS; 95% cumulative indcidence (CI)] of 26·9 years for the entire cohort. The 15-year OS of 82·5% (72–95%) was significantly decreased among A-T patients with malignancies, who had a median OS of 2·11 years, with a two-year-estimated OS of 50·7% (31–82%). Haematological malignancies were the major causes of death within the initial years of life with a 15 times increased risk for death [HR (95% CI): 6·9 (3·1–15.2), P < 0·001] upon malignancy diagnosis. Male patients with A-T are at a higher cancer risk than their female counterparts. This manuscript highlights the need for cancer surveillance and prevention, as well as optimal treatment in this cohort.
Background: Fabry disease (FD), the second most prevalent lysosomal storage disorder, is classified as a rare disease. It often leads to significant quality of life impairments and premature death. Many cases remain undiagnosed due to the rarity and heterogeneity. Further, costs related to treatment often constitute a substantial financial burden for patients and health systems. While its epidemiology is still unclear, newborn screenings suggest that its actual prevalence rate is significantly higher than previously suspected. Methods: Based on well-established methodologies, this study gives an overview about the background of the development of FD-related research and provides a critical view of future needs. Results: On the grounds of benchmarking findings, an increasing research activity on FD can be observed. Most publishing countries are the USA, some European countries, Japan, Taiwan, and South Korea. In general, high-income countries publish comparably more on FD than low- or middle-income economies. The countries' financial and infrastructural background are unveiled as crucial factors for the FD research activity. Conclusions: Overall, there is a need to foster FD research infrastructure in developing and emerging countries with focus on cost-intensive genetic research that is independent from economic interests of big pharmaceutical companies.
Objective: Deep brain stimulation (DBS) of the ventral intermediate nucleus (VIM) is a mainstay treatment for severe and drug-refractory essential tremor (ET). Although stimulation-induced dysarthria has been extensively described, possible impairment of swallowing has not been systematically investigated yet. Methods: Twelve patients with ET and bilateral VIM-DBS with self-reported dysphagia after VIM-DBS were included. Swallowing function was assessed clinically and using by flexible endoscopic evaluation of swallowing in the stim-ON and in the stim-OFF condition. Presence, severity, and improvement of dysphagia were recorded. Results: During stim-ON, the presence of dysphagia could be objectified in all patients, 42% showing mild, 42% moderate, and 16 % severe dysphagia. During stim-OFF, all patients experienced a statistically significant improvement of swallowing function. Interpretation: VIM-DBS may have an impact on swallowing physiology in ET-patients. Further studies to elucidate the prevalence and underlying pathophysiological mechanisms are warranted.
Background: Breast cancer is the leading cause of cancer-related deaths in women, demanding new treatment options. With the advent of immune checkpoint blockade, immunotherapy emerged as a treatment option. In addition to lymphocytes, tumor-associated macrophages exert a significant, albeit controversial, impact on tumor development. Pro-inflammatory macrophages are thought to hinder, whereas anti-inflammatory macrophages promote tumor growth. However, molecular markers to identify prognostic macrophage populations remain elusive. Methods: We isolated two macrophage subsets, from 48 primary human breast tumors, distinguished by the expression of CD206. Their transcriptomes were analyzed via RNA-Seq, and potential prognostic macrophage markers were validated by PhenOptics in tissue microarrays of patients with invasive breast cancer. Results: Normal human breast tissue contained mainly CD206+ macrophages, while increased relative amounts of CD206− macrophages were observed in tumors. The presence of CD206+ macrophages correlated with a pronounced lymphocyte infiltrate and subsets of CD206+ macrophages, expressing SERPINH1 and collagen 1, or MORC4, were unexpectedly associated with improved survival of breast cancer patients. In contrast, MHCIIhi CD206− macrophages were linked with a poor survival prognosis. Conclusion: Our data highlight the heterogeneity of tumor-infiltrating macrophages and suggest the use of multiple phenotypic markers to predict the impact of macrophage subpopulations on cancer prognosis. We identified novel macrophage markers that correlate with the survival of patients with invasive mammary carcinoma.
Aims: Systemic inflammatory response, identified by increased total leucocyte counts, was shown to be a strong predictor of mortality after transcatheter aortic valve implantation (TAVI). Yet the mechanisms of inflammation-associated poor outcome after TAVI are unclear. Therefore, the present study aimed at investigating individual inflammatory signatures and functional heterogeneity of circulating myeloid and T-lymphocyte subsets and their impact on 1 year survival in a single-centre cohort of patients with severe aortic stenosis undergoing TAVI. Methods and results: One hundred twenty-nine consecutive patients with severe symptomatic aortic stenosis admitted for transfemoral TAVI were included. Blood samples were obtained at baseline, immediately after, and 24 h and 3 days after TAVI, and these were analysed for inflammatory and cardiac biomarkers. Myeloid and T-lymphocyte subsets were measured using flow cytometry. The inflammatory parameters were first analysed as continuous variables; and in case of association with outcome and area under receiver operating characteristic (ROC) curve (AUC) ≥ 0.6, the values were dichotomized using optimal cut-off points. Several baseline inflammatory parameters, including high-sensitivity C-reactive protein (hsCRP; HR = 1.37, 95% CI: 1.15–1.63; P < 0.0001) and IL-6 (HR = 1.02, 95% CI: 1.01–1.03; P = 0.003), lower counts of Th2 (HR = 0.95, 95% CI: 0.91–0.99; P = 0.009), and increased percentages of Th17 cells (HR = 1.19, 95% CI: 1.02–1.38; P = 0.024) were associated with 12 month all-cause mortality. Among postprocedural parameters, only increased post-TAVI counts of non-classical monocytes immediately after TAVI were predictive of outcome (HR = 1.03, 95% CI: 1.01–1.05; P = 0.003). The occurrence of SIRS criteria within 48 h post-TAVI showed no significant association with 12 month mortality (HR = 0.57, 95% CI: 0.13–2.43, P = 0.45). In multivariate analysis of discrete or dichotomized clinical and inflammatory variables, the presence of diabetes mellitus (HR = 3.50; 95% CI: 1.42–8.62; P = 0.006), low left ventricular (LV) ejection fraction (HR = 3.16; 95% CI: 1.35–7.39; P = 0.008), increased baseline hsCRP (HR = 5.22; 95% CI: 2.09–13.01; P < 0.0001), and low baseline Th2 cell counts (HR = 8.83; 95% CI: 3.02–25.80) were significant predictors of death. The prognostic value of the linear prediction score calculated of these parameters was superior to the Society of Thoracic Surgeons score (AUC: 0.88; 95% CI: 0.78–0.99 vs. 0.75; 95% CI: 0.64–0.86, respectively; P = 0.036). Finally, when analysing LV remodelling outcomes, ROC curve analysis revealed that low numbers of Tregs (P = 0.017; AUC: 0.69) and increased Th17/Treg ratio (P = 0.012; AUC: 0.70) were predictive of adverse remodelling after TAVI. Conclusions: Our findings demonstrate an association of specific pre-existing inflammatory phenotypes with increased mortality and adverse LV remodelling after TAVI. Distinct monocyte and T-cell signatures might provide additive biomarkers to improve pre-procedural risk stratification in patients referred to TAVI for severe aortic stenosis.