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Differentialdiagnostik der frühen primären Myelofibrose (präPMF) gemäß der neuen WHO-Klassifikation
(2020)
Die vorliegende Arbeit stützt sich auf die retrospektive Begutachtung von 348 Knochenmarkbiopsien, welche anhand der WHO-Klassifikation von 2016 erneut reevaluiert wurden. Insbesondere widmeten wir uns der Differentialdiagnostik der „echten ET“ und der thrombozythämisch verlaufenden Form der PMF (präPMF). Die Einteilung erfolgte anhand morphologischer Kriterien, wie sie in der WHO-Klassifikation von 2016 aufgeführt sind.
Zusammengefasst ist eine richtungsweisende diagnostische Entscheidung der Patienten mit ET und präPMF nur möglich, wenn man sowohl die molekulargenetischen und klinischen Parameter in Kombination mit histologischen Kriterien und deren charakteristischen Mustern betrachtet. Eine repräsentative Knochenmarkbiopsie und deren standardisierte Befundung ist daher von absoluter diagnostischer Wichtigkeit für die Subtypisierung der MPN. Augenmerk sollte auf das typisch dargebotene morphologische Muster gelegt werden und nicht auf einzelne Merkmale. Die vorliegende Knochenmarkbiopsie muss nicht, wie früher praktiziert, anhand vieler einzelner Merkmale detailliert betrachtet und bewertet werden. Durch eine kombinierte Betrachtung von nur wenigen morphologischen Schlüsselparametern ist bereits eine Diagnose mit hoher Reproduzierbarkeit möglich. Mit dieser Arbeit wird der Stellenwert der WHO-Klassifikation unterstrichten, da die hier vorgegebenen Kriterien absolut essentiell und trotzdem in ihrem Umfang ausreichend sind, um die Differentialdiagnostik der MPN in Zukunft zu verbessern.
The aim of the study was to obtain volumetric data of the components of the inner ear using three-dimensional reconstruction of high-resolution cone-beam computed tomography (CBCT) images. Two hundred three CBCT image series of the temporal bone from 118 anatomically normal patients (55 women and 63 men; mean age: 49.4 ± 20.4 years) with different suspected disorders were included in this study. Normative volumetric measurements of the inner ear, the cochlea, the semicircular canals (SSC), and the vestibule were determined using a semi-automated reconstruction method of the Workstation. Volumetric measurements were successfully completed in all 118 patients. Mean inner ear, cochlear, and vestibule volumes were statistically significantly larger in males than in females on both sides (p < 0.001). Regarding the semicircular canals, no statistically significant (p = 0.053) volume difference was found. The difference between the volumes on both sides was not significant. No correlation between the patient’s age and the volume of the compartments was seen (p > 0.05). There was no significant difference between mean bony inner ear volumes when the clinical diagnoses were compared (p > 0.05 for all clinical diagnoses and volumes). Our study concluded that three-dimensional reconstruction and assessment of the volumetric measurements of the inner ear can be obtained using high-resolution CBCT imaging.
Locomotor activity patterns of laboratory mice are widely used to analyze circadian mechanisms, but most investigations have been performed under standardized laboratory conditions. Outdoors, animals are exposed to daily changes in photoperiod and other abiotic cues that might influence their circadian system. To investigate how the locomotor activity patterns under outdoor conditions compare to controlled laboratory conditions, we placed 2 laboratory mouse strains (melatonin-deficient C57Bl and melatonin-proficient C3H) in the garden of the Dr. Senckenbergische Anatomie in Frankfurt am Main. The mice were kept singly in cages equipped with an infrared locomotion detector, a hiding box, nesting material, and with food and water ad libitum. The locomotor activity of each mouse was recorded for 1 year, together with data on ambient
temperature, light, and humidity. Chronotype, chronotype stability, total daily activity, duration of the activity period, and daily diurnality indices were determined from the actograms. C3H mice showed clear seasonal differences in the chronotype, its stability, the total daily activity, and the duration of the activity period. These pronounced seasonal differences were not observed in the C57Bl. In both strains, the onset of the main activity period was mainly determinedby the evening dusk, whereas the offset was influenced by the ambient temperature. The actograms did not reveal infra-, ultradian, or lunar rhythms or a weekday/weekend pattern. Under outdoor conditions, the 2 strains retained their nocturnal locomotor identity as observed in the laboratory. Our results indicate that the chronotype displays a seasonal plasticity that may depend on the melatoninergic system. Photoperiod and ambient temperature are the most potent abiotic entraining cues. The timing of the evening dusk mainly affects the onset of the activity period; the ambient temperature during this period influences the latter’s duration. Humidity, overall light intensities, and human activities do not affect the locomotor behavior.
Introduction: Prophylaxis with factor VIII (FVIII) concentrates in children with haemophilia A (HA) is current standard of care. The benefit of prophylactic treatment for adult HA patients is not commonly accepted.
Aim: To investigate the benefit of prophylaxis over on‐demand treatment in adult and elderly patients with severe or non‐severe HA in a real‐life setting.
Methods: Data from 163 patients comprising 1202 patient‐years were evaluated for 7.5 (±5.3) years. The effects on the annual bleeding rate (ABR, including spontaneous and traumatic bleeds) of treatment with a plasma‐derived FVIII concentrate, the patient's age and disease severity were investigated. The effect of changing the treatment from on demand to continuous prophylaxis on the patients’ ABRs was further analysed.
Results: Prophylaxis had the greatest effect on the ABRs of patients of any age with severe or non‐severe HA. The difference in ABR of all patients treated on demand (median 31.4; interquartile range (IQR) 27.6; N = 83) compared with those treated prophylactically (median 1.3; IQR 3.6; N = 122) was statistically significant (P < .05), even for patients with non‐severe HA (median 8.4; IQR 15.5; N = 11) vs median 1.5; IQR 4.2 (N = 17), P < .05). Patients, aged up to 88 years, switching from on demand to continuous prophylaxis showed the lowest median ABR (1.1; N = 51) after their regimen change.
Conclusion: Any (even low‐frequency) prophylaxis results in lower ABR than on‐demand treatment. Patients switching to prophylaxis benefitted the most, irrespective of age or HA severity. Prophylactic treatment—even tertiary—is the regimen of choice for patients of any age, including elderly patients, with severe or non‐severe HA.
Purpose: Surgery of KOOS IV vestibular schwannoma remains challenging regarding the balance of extent of tumor resection (EoR) and functional outcome. Our aim was to evaluate the outcome of surgical resection and define a cut-off value for safe resection with low risk for tumor regrowth of KOOS IV vestibular schwannoma.
Methods: All patients presenting at the authors’ institution between 2000 and 2019 with surgically treated KOOS IV vestibular schwannoma were included. Outcome measures included EoR, facial/hearing nerve function, surgical complications and progression of residual tumor during the median follow-up period of 28 months.
Results: In 58 patients, mean tumor volume was 17.1 ± 9.2 cm3, and mean EoR of 81.6 ± 16.8% could be achieved. Fifty-one patients were available for the follow-up analysis. Growth of residual tumor was observed in 11 patients (21.6%) followed by adjuvant treatment with stereotactic radiosurgery or repeat surgery in 15 patients (29.4%). Overall serviceable hearing preservation was achieved in 38 patients (74.5%) and good facial outcome at discharge was observed in 66.7% of patients, significantly increasing to 82.4% at follow-up. Independent predictors for residual tumor growth was EoR ≤ 87% (OR11.1) with a higher EoR being associated with a very low number of residual tumor progression amounting to 7.1% at follow-up (p=0.008).
Conclusions: Subtotal tumor resection is a good therapeutic concept in patients with KOOS IV vestibular schwannoma resulting in a high rate of good hearing and facial nerve function and a very low rate of subsequent tumor progression. The goal of surgery should be to achieve more than 87% of tumor resection to keep residual tumor progression low.
Traumatische Verletzungen fordern jährlich über fünf Millionen Todesopfer. Sie sind bei unter 45-Jährigen die häufigste Ursache für Tod und körperliche Behinderung dar. Ein Polytrauma verursacht eine schwere Belastung für das Immunsystem und ist häufig von schweren Störungen der Immunregulation gekennzeichnet. Die Immunreaktion übersteigt bei schweren Traumata das für lokale Reparaturmechanismen notwendige Maß, und so kommt es je nach Ausmaß der Verletzungen innerhalb der ersten Minuten bis Stunden zu einer systemischen Hyperinflammation, dem sogenannten Systemischen Inflammatorischen Response- Syndrom (SIRS). Auch in nicht verletzten Organen verursacht SIRS Störungen in der Endothel-Funktion, wodurch die Mikrozirkulation in diesen Organgen beeinträchtigt ist. In der Folge kommt es zu interstitieller Ödembildung, zur Gewebsinfiltration durch Leukozyten und zu Zelluntergang. Diese Prozesse können zur Fehlfunktion von Organen bis hin zum Organversagen, und, da sie häufig in mehreren Organen gleichzeitig ablaufen, auch zum klinisch dann oft schwer beherrschbaren Multiorganversagen (MOV) führen. Auf der anderen Seite stoßen schwere Verletzungen antiinflammatorische Prozesse an, die zu einer ausgeprägten Immunsuppression führen können, dem Kompensatorischen Antiinflammatorischen Response-Syndrom (CARS), mit der Folge, dass polytraumatisierte Patienten erhöht anfällig für infektiöse Komplikationen sind. Die beschriebenen Funktionsstörungen des Immunsystems sind ein wichtiger Mortalitätsfaktor von polytraumatisierten Patienten. Während wir SIRS und seine Folgen über die letzten Jahre immer besser verstehen, mit signifikanten Fortschritten auch für die klinische Handhabung dieser Komplikationen des Polytraumas, ist CARS weit schlechter untersucht.
Während der post-traumatschen Immunantwort spielen nicht nur Zellen der angeborenen, sondern auch solche der erworbenen Immunabwehr eine wichtige Rolle. So sind regulatorische T-Zellen (Treg) entscheidend an der posttraumatischen Immunsuppression beteiligt. Treg beeinflussen die immunologische Homöostase Treg mit einem Arsenal immunsuppressiver Werkzeuge. Sie töten oder beeinflussen beispielsweise antigenpräsentierende Zellen oder T-Effektorzellen und verändern das Zytokinmilieu und metabolische Signalwege. Nach einem Trauma kann eine überschießende Aktivität von Treg die immunologische Balance so beeinträchtigen, dass eine posttraumatische Immunsuppression entsteht oder intensiviert wird. Die hier vorgestellte Studie Ziel dient daher dem besseren Verständnis der Dynamik von Treg nach einer stattgehabten traumatischen Verletzung. Dafür untersuchten wir die Verläufe verschiedener Subpopulationen von Treg im Blut schwer verletzter Patienten. Da der Forschung am Menschen in vivo enge ethische und methodologische Grenzen gesetzt sind, nehmen Tiermodelle in der Traumaforschung einen hohen Stellenwert ein. Daher verglichen wir die an Patienten erhobenen Daten über die posttraumatische Dynamik von Treg mit den Verläufen in einem adäquaten Tiermodell.
Aufgrund der guten anatomischen, physiologischen und genetischen Ähnlichkeit zum Menschen werden Tiermodelle am Schwein zunehmend beliebter. Ein Polytraumamodell am Schwein existiert erst seit wenigen Jahren. Über Treg wurde in diesem Rahmen bisher nicht geforscht. Die Charakterisierung ihres Immunphänotyps und ihrer Dynamik könnte die Anwendbarkeit des Schweine-Modells für Fragen der Trauma-Forschung verbessern und gleichzeitig unser Verständnis der Pathophysiologie posttraumatischer Komplikationen wir SIRS oder Sepsis erhöhen.
Bei 20 Traumapatienten (TP) mit einem Injury Severity Score (ISS) ≥ 16 wurde bei Ankunft in der Notaufnahme, nach einem und nach drei Tagen venöses Blut entnommen. Zehn gesunde Freiwillige (HV) fungierten in der Studie als Kontrollgruppe. Das Polytrauma im Großtiermodell am Schwein bestand aus einer Femurfraktur, einer Leberlazeration, einer Lungenkontusion und einem hämorrhagischen Schock, was einen ISS von 27 ergab. Auf die Traumainduktion folgte die Reanimationsphase und die chirurgische Versorgung der Femurfraktur nach dem damage-control-Prinzip. Die Blutentnahmen erfolgten bei den Versuchstieren vor und sofort nach Trauma, sowie nach 24 und 72 Stunden. Wir verglichen die Dynamik der Verläufe der Treg von TP mit denen von HV und mit Daten aus den Tierversuchen. Es herrscht noch kein wissenschaftlicher Konsens darüber, welche Kombination aus immunologischen Oberflächenmarkern die Identifikation von Treg zuverlässig gewährleisten kann. Dies liegt auch daran, dass Treg eine Gruppe verschiedener Unterpopulationen darstellen. Folglich analysierten wir verschiedene Kombinationen. Wir färbten Cluster of differentiation (CD) 4-positive und CD25-positive (CD4+CD25+), CD4+CD25+forkhead box P3 (FoxP3)+, CD4+CD25+CD127-negative (CD127−) und CD4+CD25+CD127−FoxP3+ Zellen mit Antikörpern und charakterisierten die jeweilige Gruppe mithilfe der Durchflusszytometrie. CD4+CD25+CD127− Treg sind beim Menschen bekannt. Beim Schwein werden sie in dieser Studie erstmalig beschrieben.
...
Simple Summary: Glioblastomas are very malignant and essentially incurable brain tumors. One problem is the extensive penetration of tumor cells into the adjacent normal brain tissue. Thus, the testing of novel drugs requires appropriate tumor models, preferentially avoiding animal studies. This paper describes so-called brain tissue slice tandem-culture systems. They consist of a slice of normal brain tissue and a second layer of tumor tissue. The microscopic analysis of these slice tandem-cultures allows for the simultaneous assessment of single cells invading into the normal brain tissue and the space occupying growth of the total tumor mass. It is shown that the direct application of test drugs onto the slices exerts inhibitory effects on both mechanisms. We thus describe a system mimicking the situation in glioblastoma patients. It reduces animal studies, allows for the direct application of test drugs and the precise quantitation of their inhibitory effects on tumor growth and invasion.
Abstract: Glioblastomas (GBMs) are the most malignant brain tumors and are essentially incurable even after extensive surgery, radiotherapy, and chemotherapy, mainly because of extensive infiltration of tumor cells into the adjacent normal tissue. Thus, the evaluation of novel drugs in malignant glioma treatment requires sophisticated ex vivo models that approach the authentic interplay between tumor and host environment while avoiding extensive in vivo studies in animals. This paper describes the standardized setup of an organotypic brain tissue slice tandem-culture system, comprising of normal brain tissue from adult mice and tumor tissue from human glioblastoma xenografts, and explore its utility for assessing inhibitory effects of test drugs. The microscopic analysis of vertical sections of the slice tandem-cultures allows for the simultaneous assessment of (i) the invasive potential of single cells or cell aggregates and (ii) the space occupying growth of the bulk tumor mass, both contributing to malignant tumor progression. The comparison of tissue slice co-cultures with spheroids vs. tissue slice tandem-cultures using tumor xenograft slices demonstrates advantages of the xenograft tandem approach. The direct and facile application of test drugs is shown to exert inhibitory effects on bulk tumor growth and/or tumor cell invasion, and allows their precise quantitation. In conclusion, we describe a straightforward ex vivo system mimicking the in vivo situation of the tumor mass and the normal brain in GBM patients. It reduces animal studies and allows for the direct and reproducible application of test drugs and the precise quantitation of their effects on the bulk tumor mass and on the tumor’s invasive properties
Background: The aim of this study was to collect standard reference values of the weight and the maximum pressure distribution in healthy adults aged 18–65 years and to investigate the influence of constitutional parameters on it.
Methods: A total of 416 healthy subjects (208 male / 208 female) aged between 18 and 65 years (Ø 38.3 ± 14.1 years) participated in this study, conducted 2015–2019 in Heidelberg. The age-specific evaluation is based on 4 age groups (G1, 18–30 years; G2, 31–40 years; G3, 41–50 years; G4, 51–65 years). A pressure measuring plate FDM-S (Zebris/Isny/Germany) was used to collect body weight distribution and maximum pressure distribution of the right and left foot and left and right forefoot/rearfoot, respectively.
Results: Body weight distribution of the left (50.07%) and right (50.12%) foot was balanced. There was higher load on the rearfoot (left 54.14%; right 55.09%) than on the forefoot (left 45.49%; right 44.26%). The pressure in the rearfoot was higher than in the forefoot (rearfoot left 9.60 N/cm2, rearfoot right 9.51 N/cm2/forefoot left 8.23 N/cm2, forefoot right 8.59 N/cm2). With increasing age, the load in the left foot shifted from the rearfoot to the forefoot as well as the maximum pressure (p ≤ 0.02 and 0.03; poor effect size). With increasing BMI, the body weight shifted to the left and right rearfoot (p ≤ 0.001, poor effect size). As BMI increased, so did the maximum pressure in all areas (p ≤ 0.001 and 0.03, weak to moderate effect size). There were significant differences in weight and maximum pressure distribution in the forefoot and rearfoot in the different age groups, especially between younger (18–40 years) and older (41–65 years) subjects.
Discussion: Healthy individuals aged from 18 to 65 years were found to have a balanced weight distribution in an aspect ratio, with a 20% greater load of the rearfoot. Age and BMI were found to be influencing factors of the weight and maximum pressure distribution, especially between younger and elder subjects. The collected standard reference values allow comparisons with other studies and can serve as a guideline in clinical practice and scientific studies.
Background: To detect deviations from a normal postural control, standard values can be helpful for comparison purposes. Since the postural control is influenced by gender and age, the aim of the present study was the collection of standard values for women between 31 and 40 years of age.
Methods: For the study, 106 female, subjectively healthy, German subjects aged between 31 and 40 years (35 ± 2.98 years) were measured using a pressure measuring platform.
Results: Their average BMI was 21.60 ± 4.65 kg/m2. The load distribution between left and right foot was almost evenly balanced with a median 51.46% load on the left [tolerance interval (TR) 37.02%/65.90%; confidence interval (CI) 50.06/52.85%] and 48.54% [TR 43.10/62.97%; CI 47.14/49.93%] on the right foot. The median forefoot load was 33.84% [TR 20.68/54.73%; CI 31.67/37.33%] and the rearfoot load was measured at 66.16% [TR 45.27/79.33%; CI 62.67/68.33%]. The median/mean body sway in the sagittal plane was measured 12 mm [TR 5.45/23.44 mm; CI 11.00/14.00 mm] and 8.17 mm in the frontal plane [TR 3.33/19.08 mm; CI 7.67/9.33 mm]. The median of the ellipse area is 0.72 cm2 [TR 0.15/3.69 cm2; CI 0.54/0.89°]. The ellipse width has a median of 0.66 cm [TR 0.30/1.77 cm; CI 0.61/0.78 cm] and the height of 0.33 cm [TR 0.13/0.71 cm; CI 0.30/0.37 cm]. The ellipse angle (sway, left forefoot to right rearfoot) has a mean of − 19.34° [TR − 59.21/− 0.44°; CI − 22.52/− 16.16°] and the ellipse angle sway from right forefoot to left rearfoot has a mean of 12.75° [TR 0.09/59.09°; CI 9.00/16.33°].
Conclusion: The right-to-left ratio is balanced. The forefoot-to-rearfoot ratio is approximately 1:2. Also, the body sway can be classified with 12 and 8 mm as normal. The direction of fluctuation is either approx. 19° from the left forefoot to the right rearfoot or approx. 13° the opposite. Body weight, height, and BMI were comparable to the German average of women in a similar age group, so that the measured standard values are representative and might serve as baseline for the normal function of the balance system in order to support the diagnosis of possible dysfunctions in postural control.
Bronchiolitis obliterans (BO) is a rare, chronic form of obstructive lung disease, often initiated with injury of the bronchiolar epithelium followed by an inflammatory response and progressive fibrosis of small airways resulting in nonuniform luminal obliteration or narrowing. The term BO comprises a group of diseases with different underlying etiologies, courses, and characteristics. Among the better recognized inciting stimuli leading to BO are airway pathogens such as adenovirus and mycoplasma, which, in a small percentage of infected children, will result in progressive fixed airflow obstruction, an entity referred to as postinfectious bronchiolitis obliterans (PIBO). The present knowledge on BO in general is reasonably well developed, in part because of the relatively high incidence in patients who have undergone lung transplantation or bone marrow transplant recipients who have had graft-versus-host disease in the posttransplant period. The cellular and molecular pathways involved in PIBO, while assumed to be similar, have not been adequately elucidated. Since 2016, an international consortium of experts with an interest in PIBO assembles on a regular basis in Geisenheim, Germany, to discuss key areas in PIBO which include diagnostic workup, treatment strategies, and research fields.