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Background: The potential anti-cancer effects of mammalian target of rapamycin (mTOR) inhibitors are being intensively studied. To date, however, few randomised clinical trials (RCT) have been performed to demonstrate anti-neoplastic effects in the pure oncology setting, and at present, no oncology endpoint-directed RCT has been reported in the high-malignancy risk population of immunosuppressed transplant recipients. Interestingly, since mTOR inhibitors have both immunosuppressive and anti-cancer effects, they have the potential to simultaneously protect against immunologic graft loss and tumour development. Therefore, we designed a prospective RCT to determine if the mTOR inhibitor sirolimus can improve hepatocellular carcinoma (HCC)-free patient survival in liver transplant (LT) recipients with a pre-transplant diagnosis of HCC. Methods: The study is an open-labelled, randomised, RCT comparing sirolimus-containing versus mTOR-inhibitor-free immunosuppression in patients undergoing LT for HCC. Patients with a histologically confirmed HCC diagnosis are randomised into 2 groups within 4-6 weeks after LT; one arm is maintained on a centre-specific mTOR-inhibitor-free immunosuppressive protocol and the second arm is maintained on a centre-specific mTOR-inhibitor-free immunosuppressive protocol for the first 4-6 weeks, at which time sirolimus is initiated. A 3-year recruitment phase is planned with a 5-year follow-up, testing HCC-free survival as the primary endpoint. Our hypothesis is that sirolimus use in the second arm of the study will improve HCC-free survival. The study is a non-commercial investigator-initiated trial (IIT) sponsored by the University Hospital Regensburg and is endorsed by the European Liver and Intestine Transplant Association; 13 countries within Europe, Canada and Australia are participating. Discussion: If our hypothesis is correct that mTOR inhibition can reduce HCC tumour growth while simultaneously providing immunosuppression to protect the liver allograft from rejection, patients should experience less post-transplant problems with HCC recurrence, and therefore could expect a longer and better quality of life. A positive outcome will likely change the standard of posttransplant immunosuppressive care for LT patients with HCC. (trial registered at www.clinicaltrials.gov: NCT00355862) (EudraCT Number: 2005-005362-36)
Einleitung: Schwer verletzte Patienten nach Trauma (ISS > 16) sind häufig in Folge der Verletzungen über mehrere Tage beatmet. 40% dieser Patienten weisen eine Lungenkontusion auf. Mit zunehmender Beatmungsdauer steigt das Risiko einer Ventilator-assoziierten Pneumonie (VAP). Zeitgleich findet eine Reparation des Lungengewebes statt. Eine zeitnahe antiinfektive Therapie bei Verdacht auf eine VAP zu initiieren ist schwierig. Derzeit existiert kein validierter Parameter oder Score, der eine sichere Diskriminierung zwischen Infektion und Inflammation zulässt. Triggering receptor on myeloid cells (TREM-1) ist ein Rezeptor des angeborenen Immunsystems und wurde im Jahr 2000 erstmalig beschrieben. Sein löslicher Anteil, sTREM-1, ist in der bronchoalveolären Lavage (BAL) bei Patienten mit Pneumonie signifikant erhöht (> 200pg/ml). Es liegen keine Daten zu sTREM-1 bei Patienten nach Lungenkontusion vor. Unklar ist, ob sTREM-1 als Pneumonie-Marker nach Lungenkontusion geeignet ist. Material & Methoden: Nach Zustimmung der Ethikkommission und Einwilligung durch einen Angehörigen wurden prospektiv 42 Patienten mit Thoraxtrauma rekrutiert. Am ersten (im Median 15h nach dem Trauma) und an den Behandlungstagen zwei, drei, fünf, sechs und sieben wurden bei allen Patienten über den Tubus mit einem Aero-Jet Katheter BAL (20ml Spülung) gewonnen und zeitgleich Serumproben entnommen. Die Messung der sTREM-1-Konzentration erfolgte mittels Sandwich-ELISA in Doppelbestimmung (Quantikine sTREM-1 Immunoassay; Firma R&D Systems). Die Serum-Konzentrationen der Interleukine (IL) 6 und 10 sowie des Lipopolysaccharid bindenden Proteins (LBP) wurden mittels Immulite® bestimmt. Die Diagnose Pneumonie wurde retrospektiv mittels Clinical Pulmonary Infection Score (CPIS) gestellt: CPIS > 6 Pneumonie, ≤ 6 keine Pneumonie. Ergebnisse & Diskussion: 15 Stunden nach Trauma wurde der sTREM-1 Spiegel in der BAL, bei im Verlauf pulmonal klinisch unauffälligen Patienten, im Median mit 219pg/ml bestimmt. Im Weiteren stieg sTREM-1 im Median nach 24h auf 575pg/ml an und zeigte ähnliche Konzentrationen im Beobachtungszeitraum. Der Schweregrad der Lungenkontusion korreliert mit der Höhe des sTREM-1-Spiegels in der BAL 40h nach Trauma. Patienten mit schwerer Lungenkontusion (im Median 2240pg/ml) haben signifikant höhere Werte gegenüber Patienten ohne Kontusion (Median 217pg/ml), oder geringer Kontusion (Median 339pg/ml). Am Tag der Diagnosestellung Pneumonie (CPIS > 6, n= 9) zeigten die betroffenen Patienten einen signifikant erhöhten sTREM-1-Spiegel in der BAL (Median 2145pg/ml, p < 0,05) im Vergleich zum Tag vor der Pneumonie (Median 588pg/ml). Wird der cut off für sTREM-1 bei 800pg/ml festgelegt ergibt sich eine Sensitivität von 87% und eine Spezifität von 38%. Eine positive BAL weist im Vergleich zu einer negativen BAL signifikant höhere sTREM-1-Konzentrationen (Median 1492pg/ml vs. 971pg/ml, p < 0,05) auf. Die Sensitivität (85%) ist hoch, die Spezifität (51%) gering. Somit ist sTREM-1 nicht nur durch eine Infektion, sondern auch durch eine Gewebeschädigung mit Einblutung und Inflammation stimulierbar. sTREM-1 ist durch die kontusionsbedingte Stimulation in der ersten Woche nach Trauma ungeeignet, um sicher zwischen einer Pneumonie und einer kontusionsbedingten Inflammation zu unterscheiden. Zytokine und akute Phase Proteine (IL-6, LBP, Procalcitonin) sind bekanntermaßen ebenfalls nicht zur sicheren Diskriminierung einer Infektion geeignet. In Kombination mit sTREM-1 lassen sich jedoch zur Diagnosestellung einer Pneumonie vergleichbare Werte für Sensitivität und Spezifität erreichen wie mittels CPIS Score, wobei der CPIS nur retrospektiv ermittelt werden kann. Die Laborparameter liegen bereits am Tag des Verdachts auf eine Infektion vor. Die klinische Entscheidung zur Initiierung einer Antiinfekitvatherapie korrelierte weder mit dem CPIS noch mit den Inflammationsparametern. Drei von neun Patienten erhielten trotz steigenden Entzündungszeichen und einem CPIS > 6 keine Antiinfektiva. In der Konsequenz könnte eine Kombination aus IL-6 und LBP im Serum, sTREM-1 in der BAL und klinischen Parameter des CPIS eine sensitive und spezifische Entscheidungshilfe für eine antiinfektive Therapie bei Polytrauma und Verdacht auf eine VAP werden.
Introduction: It has been proposed that individual genetic variation contributes to the course of severe infections and sepsis. Recent studies of single nucleotide polymorphisms (SNPs) within the endotoxin receptor and its signaling system showed an association with the risk of disease development. This study aims to examine the response associated with genetic variations of TLR4, the receptor for bacterial LPS, and a central intracellular signal transducer (TIRAP/Mal) on cytokine release and for susceptibility and course of severe hospital acquired infections in distinct patient populations. Methods: Three intensive care units in tertiary care university hospitals in Greece and Germany participated. 375 and 415 postoperative patients and 159 patients with ventilator associated pneumonia (VAP) were included. TLR4 and TIRAP/Mal polymorphisms in 375 general surgical patients were associated with risk of infection, clinical course and outcome. In two prospective studies, 415 patients following cardiac surgery and 159 patients with newly diagnosed VAP predominantly caused by Gram-negative bacteria were studied for cytokine levels in-vivo and after ex-vivo monocyte stimulation and clinical course. Results: Patients simultaneously carrying polymorphisms in TIRAP/Mal and TLR4 and patients homozygous for the TIRAP/Mal SNP had a significantly higher risk of severe infections after surgery (odds ratio (OR) 5.5; confidence interval (CI): 1.34 - 22.64; P = 0.02 and OR: 7.3; CI: 1.89 - 28.50; P < 0.01 respectively). Additionally we found significantly lower circulating cytokine levels in double-mutant individuals with ventilator associated pneumonia and reduced cytokine production in an ex-vivo monocyte stimulation assay, but this difference was not apparent in TIRAP/Mal-homozygous patients. In cardiac surgery patients without infection, the cytokine release profiles were not changed when comparing different genotypes. Conclusions: Carriers of mutations in sequential components of the TLR signaling system may have an increased risk for severe infections. Patients with this genotype showed a decrease in cytokine release when infected which was not apparent in patients with sterile inflammation following cardiac surgery.
Introduction: It has been proposed that individual genetic variation contributes to the course of severe infections and sepsis. Recent studies of single nucleotide polymorphisms (SNPs) within the endotoxin receptor and its signaling system showed an association with the risk of disease development. This study aims to examine the response associated with genetic variations of TLR4, the receptor for bacterial LPS, and a central intracellular signal transducer (TIRAP/Mal) on cytokine release and for susceptibility and course of severe hospital acquired infections in distinct patient populations. Methods: Three intensive care units in tertiary care university hospitals in Greece and Germany participated. 375 and 415 postoperative patients and 159 patients with ventilator associated pneumonia (VAP) were included. TLR4 and TIRAP/Mal polymorphisms in 375 general surgical patients were associated with risk of infection, clinical course and outcome. In two prospective studies, 415 patients following cardiac surgery and 159 patients with newly diagnosed VAP predominantly caused by Gram-negative bacteria were studied for cytokine levels in-vivo and after ex-vivo monocyte stimulation and clinical course. Results: Patients simultaneously carrying polymorphisms in TIRAP/Mal and TLR4 and patients homozygous for the TIRAP/Mal SNP had a significantly higher risk of severe infections after surgery (odds ratio (OR) 5.5; confidence interval (CI): 1.34 - 22.64; P = 0.02 and OR: 7.3; CI: 1.89 - 28.50; P < 0.01 respectively). Additionally we found significantly lower circulating cytokine levels in double-mutant individuals with ventilator associated pneumonia and reduced cytokine production in an ex-vivo monocyte stimulation assay, but this difference was not apparent in TIRAP/Mal-homozygous patients. In cardiac surgery patients without infection, the cytokine release profiles were not changed when comparing different genotypes. Conclusions: Carriers of mutations in sequential components of the TLR signaling system may have an increased risk for severe infections. Patients with this genotype showed a decrease in cytokine release when infected which was not apparent in patients with sterile inflammation following cardiac surgery.
Nanocarbon structures, such as fullerenes and nanotubes, have generated considerable interest and research, due to their unique properties and potential applications. In this thesis, we present a study of the phase transition properties of nanocarbon clusters,in particular, we pay special consideration to fullerenes. The work presented in this thesis is largely theoretical and computational in nature, employing as a tool, molecular dynamics simulations to probe the dynamic stability of fullerenes and associated nanocarbon structures such as graphenes and nanotubes.
Blood vessels form de novo through the tightly regulated programs of vasculogenesis and angiogenesis. Both processes are distinct but one of the steps they share is the formation of a central lumen, when groups of cells organized as vascular cords undergo complex changes to achieve a tube-like morphology. Recently, a protein termed epidermal growth factor-like domain 7 (EGFL7) was described as a novel endothelial cell-derived factor involved in the regulation of the spatial arrangement of cells during vascular tube assembly. With its impact on tubulogenesis and vessel shape EGFL7 joined the large family of molecules governing blood vessel formation. Only recently, the molecular mechanisms underlying EGFL7's effects have been started to be elucidated and shaping of the extracellular matrix (ECM) as well as Notch signaling might very well play a role in mediating its biological effects. Further, findings in knock-out animal models suggest miR-126, a miRNA located within the egfl7 gene, has a major role in vessel development by promoting VEGF signaling, angiogenesis and vascular integrity. This review summarizes our current knowledge on EGFL7 and miR-126 and we will discuss the implications of both bioactive molecules for the formation of blood vessels.
Background: Up to the 1950s, there was an ongoing debate about the diversity of hereditary optic neuropathies, in particular as to whether all inherited optic atrophies can be ascribed to Leber's hereditary optic neuropathy (LHON) or represent different disease entities. In 1954 W. Jaeger published a detailed clinical and genealogical investigation of a large family with explicit autosomal dominant segregation of optic atrophy thus proving the existence of a discrete disease different from LHON, which is nowadays known as autosomal dominant optic atrophy (ADOA). Since the year 2000 ADOA is associated with genomic mutations in the OPA1 gene, which codes for a protein that is imported into mitochondria where it is required for mitochondrial fusion. Interestingly enough, the underlying mutation in this family has not been identified since then. Results: We have reinvestigated this family with the aim to identify the mutation and to further clarify the underlying pathomechanism. Patients showed a classical non-syndromic ADOA. The long term deterioration in vision in the two teenagers examined 50 years later is of particular note 5/20 to 6/120. Multiplex ligation probe amplification revealed a duplication of the OPA1 exons 7-9 which was confirmed by long distance PCR and cDNA analysis, resulting in an in-frame duplication of 102 amino acids. Segregation was verified in 53 available members of the updated pedigree and a penetrance of 88% was calculated. Fibroblast cultures from skin biopsies were established to assess the mitochondrial network integrity and to qualitatively and quantitatively study the consequences of the mutation on transcript and protein level. Fibroblast cultures demonstrated a fragmented mitochondrial network. Processing of the OPA1 protein was altered. There was no correlation of the OPA1 transcript levels and the OPA1 protein levels in the fibroblasts. Intriguingly an overall decrease of mitochondrial proteins was observed in patients' fibroblasts, while the OPA1 transcript levels were elevated. Conclusions: The thorough study of this family provides a detailed clinical picture accompanied by a molecular investigation of patients' fibroblasts. Our data show a classic OPA1-associated non-syndromic ADOA segregating in this family. Cell biological findings suggest that OPA1 is regulated by post-translational mechanisms and we would like to hypothesize that loss of OPA1 function might lead to impaired mitochondrial quality control. With the clinical, genetic and cell biological characterisation of a family described already more than 50 years ago, we span more than half a century of research in optic neuropathies.
Background: Vaccinia virus strain Lister Elstree (VACV) is a test virus in the DVV/RKI guidelines as representative of the stable enveloped viruses. Since the potential risk of laboratory-acquired infections with VACV persists and since the adverse effects of vaccination with VACV are described, the replacement of VACV by the modified vaccinia Ankara strain (MVA) was studied by testing the activity of different chemical biocides in three German laboratories. Methods: The inactivating properties of different chemical biocides (peracetic acid, aldehydes and alcohols) were tested in a quantitative suspension test according to the DVV/RKI guideline. All tests were performed with a protein load of 10% fetal calf serum with both viruses in parallel using different concentrations and contact times. Residual virus was determined by endpoint dilution method. Results: The chemical biocides exhibited similar virucidal activity against VACV and MVA. In three cases intra-laboratory differences were determined between VACV and MVA - 40% (v/v) ethanol and 30% (v/v) isopropanol are more active against MVA, whereas MVA seems more stable than VACV when testing with 0.05% glutardialdehyde. Test accuracy across the three participating laboratories was high. Remarkably inter-laboratory differences in the reduction factor were only observed in two cases. Conclusions: Our data provide valuable information for the replacement of VACV by MVA for testing chemical biocides and disinfectants. Because MVA does not replicate in humans this would eliminate the potential risk of inadvertent inoculation with vaccinia virus and disease in non-vaccinated laboratory workers.
Introduction: Amniotic fluid harbors cells indicative of all three germ layers, and pluripotent fetal amniotic fluid stem cells (AFSs) are considered potentially valuable for applications in cellular therapy and tissue engineering. We investigated whether it is possible to direct the cell fate of AFSs in vivo by transplantation experiments into a particular microenvironment, the mammary fat pad. This microenvironment provides the prerequisites to study stem cell function and the communication between mesenchymal and epithelial cells. On clearance of the endogenous epithelium, the ductal tree can be reconstituted by the transfer of exogenously provided mammary stem cells. Analogously, exogenously provided stem cells from other tissues can be investigated for their potential to contribute to mammary gland regeneration. Methods: We derived pluripotent murine AFSs, measured the expression of stem cell markers, and confirmed their in vitro differentiation potential. AFSs were transplanted into cleared and non cleared fat pads of immunocompromised mice to evaluate their ability to assume particular cell fates under the instructive conditions of the fat-pad microenvironment and the hormonal stimulation during pregnancy. Results: Transplantation of AFSs into cleared fat pads alone or in the presence of exogenous mammary epithelial cells caused their differentiation into stroma and adipocytes and replaced endogenous mesenchymal components surrounding the ducts in co-transplantation experiments. Similarly, transplantation of AFSs into fat pads that had not been previously cleared led to AFS-derived stromal cells surrounding the elongating endogenous ducts. AFSs expressed the marker protein α-SMA, but did not integrate into the myoepithelial cell layer of the ducts in virgin mice. With pregnancy, a small number of AFS-derived cells were present in acinar structures. Conclusions: Our data demonstrate that the microenvironmental cues of the mammary fat pad cause AFSs to participate in mammary gland regeneration by providing mesenchymal components to emerging glandular structures, but do not incorporate or differentiate into ductal epithelial cells.
This work reports on the study of the projectile x-ray emission in relativistic ion-atom collisions. Excitation of K-shell in He-like uranium ions, electron capture into H-like uranium ions and Simultaneous ionization and excitation of initially He-like uranium ions have been studied using the experimental storage ring at GSI. Information about the population of the excited states for the H- and He-like uranium ions, can be obtained by measuring the angular distribution of the decay radiation. Since the Ly_alpha2 transition is isotropic, the intensities of the Ly_alpha1 and K_alpha transitions were normalized to the Ly_alpha2 line. For the K_alpha1 and K_alpha2 transitions originating from the excitation of the He-like uranium ions, no alignment was observed. In contrast, the Ly_alpha1 radiation from the simultaneous ionization-excitation process of the He-like uranium ions shows a clear alignment. It is shown that the alignment of Ly_alpha1 was obtained by the Alignment parameter A_20. The experimental value leads to the inclusion of a magnetic term in the interaction potential. It is interesting to note that in the case of the Ly_alpha1 emission the small M2 contribution added coherently to the E1 transition amplitudes enhances the anisotropy. The capture process of target electrons into the highly-charged heavy ions was studied using H-like uranium ions at an incident energy of 220 MeV/u, impinging on N2 gas-target. It was shown that, the strongly aligned electrons captured in 2p3/2 level will couple with the available 1s1/2 electron which shows no initial directional preference. The magnetic sub-state population of the 2p3/2 electron will be redistributed according to the coupling rules to the magnetic sub-states of the relevant two-electron states. Consequently, the 1^P1 and 3^P2 states are corresponding to the the strongly aligned 2p3/2 state. This leads to the large anisotropy in the corresponding individual ground state transitions contributing to the K_alpha1 emission. Due to the fact that the 1^P1 --> 1^S0 and 3^P2 --> 1^S0 transitions are experimentally not resolved, a more detailed analysis of the angular dependence of the K_alpha1 radiation is required. From the K_alpha1/K_alpha2 ratio, the current results show that the incoherent addition of the E1 and M2 transition components yield to an almost isotropic emission of the total K_alpha1. In contrast to the radiative electron capture, the experimental results for the K-shell single excitation of He-like uranium ions indicate that only the 1^P1 level contributes to the K_alpha1 transition. For this case, the anisotropy parameter beta_20 was found to be -0.20 + 0.03 which is similar to that one calculated for pure E1 transition. This work also reports on the study of a two-electron process: the simultaneous ionization and excitation occurring in relativistic collisions of heavy highly-charged ions with gaseous targets. The investigation was performed on He-like uranium ions impinging upon xenon gas-target at an incident energy of 220 MeV/u. The measurements have been performed at the ESR gas-target using atomic xenon with a typical area density of 10^12 particles/cm^2. In contrast to the solid state target, the use of gas target offers the advantage of clear separation of the one step two-electron process due to the fact that the probability of two consecutive collision in such thin targets is negligible and the double step processes can be excluded. During the process of simultaneous ionization and excitation in He-like uranium ions, one of the ground-state electrons is promoted into the continuum and the other into the L-subshell states of the projectile. To select this process, the Lyman-series radiation has been measured at various observation angles in coincidence with up-charged projectiles (U^91+). From the yields of the Ly_alpha1 and Ly_alpha2 projectile radiation, the relative cross section for the process of simultaneous ionization and excitation was directly determined. The angle dependent measurement of the radiation yields provide information about the angular distributions of the emitted radiation and permits the determination of the alignment parameter A_{20}. This parameter gives information on the level population and the collision impact parameter. The present results (b^exp = 810 fm) show that the simultaneous ionization and excitation is a process which occurs at small impact parameter.