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  • 1
    Online Resource
    Online Resource
    Propuesta de un sistema de estadiaje de tumores de mediastino
    Colegio de Medicos y Cirujanos de Costa Rica ; 2010
    In:  Acta Médica Costarricense Vol. 52, No. 3 ( 2010-06-11)
    Details
    In: Acta Médica Costarricense, Colegio de Medicos y Cirujanos de Costa Rica, Vol. 52, No. 3 ( 2010-06-11)
    Abstract: El mediastino es un compartimento que aloja tumores de variado origen histológico, dada la diversidad de órganos y estructuras que lo ocupan o lo transitan. Debido a la gran capacidad de la cavidad torácica, los pacientes se presentan frecuentemente con tumores de gran tamaño, a veces ya invadiendo órganos vitales, complicando el estado clínico, el eventual manejo anestésico y los procedimientos quirúrgicos necesarios. Actualmente no existe un método común para categorizar pacientes con tumores mediastinales. Lo que hoy se hace es estudiar las imágenes y describir la masa, indicando sus dimensiones y relaciones, y de ahí se deduce la gravedad o no de la situación. De existir un sistema, los médicos tratantes podrían comunicarse, describir, y entender bien cada lesión, el grado de respuesta al tratamiento y el pronóstico de cada paciente. Siguiendo el TNM, se propone un método de estadiaje para pacientes con tumores mediastinales, utilizando algunas modificaciones importantes, utilizando las letras: T/ I / N / M. La T no representa las medidas lineales de la masa como en ese sistema, sino que más bien expresa la relación del volumen del tumor con el de la cavidad torácica del mismo individuo (T= R: Vol Tum / Vol Tórax). Estos datos se obtienen directamente del tomógrafo, o bien, calcularse según el software de cada equipo de tomografía. Usualmente el estudio tomográfico de un tumor mediastinal comprende una gran cantidad de cortes realizados a milímetros de distancia entre sí. Primero se determina el rango del coeficiente de atenuación en unidades Hounsfield del tumor, y en cada corte se dibuja el perímetro de éste. Se pide a la computadora que sume todos los volúmenes con el rango de unidades que cubran el tumor, y se obtiene así el volumen de la masa. De igual manera, se determina el coeficiente del aire que rodea el tumor (representa los pulmones) y se obtiene el volumen de la cavidad ocupado por éste. El volumen total de la cavidad torácica será la suma del volumen del aire más el del tumor. La relación se obtiene al dividir el volumen tumoral por el torácico total. El corazón, la tráquea y los grandes vasos, comunes a todos, no se toman en cuenta. La I indica invasión de cualquier estructura, sea vena cava, tráquea, aorta, etc. La disminución o compromiso de la luz en 50%. La N se refiere a la presencia o no de ganglioslinfáticos, particularmente en tumores no linfomatosos, y la M a la existencia o no de metástasis. El estadio del tumor de cada paciente puede determinarse según sea su combinación letras, como se indica en el texto.
    Type of Medium: Online Resource
    ISSN: 2215-5856 , 0001-6012
    URL: Issue
    URL: Article
    DOI: 10.51481/amc.v52i3
    DOI: 10.51481/amc.v52i3.663
    Language: Unknown
    Publisher: Colegio de Medicos y Cirujanos de Costa Rica
    Publication Date: 2010
    detail.hit.zdb_id: 2145413-9
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  • 2
    Online Resource
    Online Resource
    What happens to the traditional taxonomy when a well-known tropical saturniid moth fauna is DNA barcoded?
    CSIRO Publishing ; 2012
    In:  Invertebrate Systematics Vol. 26, No. 6 ( 2012), p. 478-
    Details
    In: Invertebrate Systematics, CSIRO Publishing, Vol. 26, No. 6 ( 2012), p. 478-
    Abstract: Biodiversity of tropical Saturniidae, as measured through traditionally described and catalogued species, strongly risks pooling cryptic species under one name. We examined the DNA barcodes, morphology, habitus and ecology of 32 ‘well known’ species of dry forest saturniid moths from Area de Conservacion Guanacaste (ACG) in north-western Costa Rica and found that they contain as many as 49 biological entities that are probably separate species. The most prominent splitting of traditional species – Eacles imperialis, Automeris zugana, Automeris tridens, Othorene verana, Hylesia dalina, Dirphia avia, Syssphinx molina, Syssphinx colla, and Syssphinx quadrilineata – is where one species was believed to breed in dry forest and rain forest, but is found to be two biological entities variously distinguishable by DNA barcodes and morphology, habitus, and/or microecological distribution. This implies that ‘standard’ biological information about each traditional species may be an unconscious mix of interspecific information, and begs renewed DNA barcoding, closer attention to so-called intraspecific variation, and increased museum collection and curation of specimens from more individual and ecologically characterised sites – as well as eventually more species descriptions. Simultaneously, this inclusion of sibling species as individual entities in biodiversity studies, rather than pooled under one traditional name, reduces the degree of ecological and evolutionary generalisation perceived by the observer.
    Type of Medium: Online Resource
    ISSN: 1445-5226
    URL: Article
    DOI: 10.1071/IS12038
    Language: English
    Publisher: CSIRO Publishing
    Publication Date: 2012
    SSG: 12
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  • 3
    Online Resource
    Online Resource
    Manejo de Bosques con Ganadería Integrada en Patagonia argentina: ajuste metodológico para la determinación de la línea de base en ecosistemas complejos y paisajes heterogéneos
    SciELO Agencia Nacional de Investigacion y Desarrollo (ANID) ; 2023
    In:  Bosque (Valdivia) Vol. 44, No. 1 ( 2023-04), p. 255-259
    Details
    In: Bosque (Valdivia), SciELO Agencia Nacional de Investigacion y Desarrollo (ANID), Vol. 44, No. 1 ( 2023-04), p. 255-259
    Type of Medium: Online Resource
    ISSN: 0717-9200
    URL: Article
    DOI: 10.4067/s0717-92002023000100255
    Language: English
    Publisher: SciELO Agencia Nacional de Investigacion y Desarrollo (ANID)
    Publication Date: 2023
    detail.hit.zdb_id: 2138018-1
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  • 4
    Online Resource
    Online Resource
    2640 Meters Closer to the Stars: Does High Altitude Affect Fontan Results?
    Elsevier BV ; 2022
    In:  The Annals of Thoracic Surgery Vol. 114, No. 6 ( 2022-12), p. 2330-2336
    Details
    In: The Annals of Thoracic Surgery, Elsevier BV, Vol. 114, No. 6 ( 2022-12), p. 2330-2336
    Type of Medium: Online Resource
    ISSN: 0003-4975
    URL: Article
    DOI: 10.1016/j.athoracsur.2022.03.053
    RVK:
    XA 23980
    Language: English
    Publisher: Elsevier BV
    Publication Date: 2022
    detail.hit.zdb_id: 1499869-5
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  • 5
    Online Resource
    Online Resource
    Susceptibilidad genética a hantavirus Andes: Asociación entre la expresión clínica de la infección y alelos del sistema HLA en pacientes chilenos
    SciELO Agencia Nacional de Investigacion y Desarrollo (ANID) ; 2007
    In:  Revista chilena de infectología Vol. 24, No. 5 ( 2007-10)
    Details
    In: Revista chilena de infectología, SciELO Agencia Nacional de Investigacion y Desarrollo (ANID), Vol. 24, No. 5 ( 2007-10)
    Type of Medium: Online Resource
    ISSN: 0716-1018
    URL: Article
    DOI: 10.4067/S0716-10182007000500001
    Language: English
    Publisher: SciELO Agencia Nacional de Investigacion y Desarrollo (ANID)
    Publication Date: 2007
    detail.hit.zdb_id: 2048815-4
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  • 6
    Online Resource
    Online Resource
    CD40 Stimulation Sensitizes CLL Cells to CD20-Triggered Cell Death by Rituximab and GA101 Via a Different Mechanism
    American Society of Hematology ; 2010
    In:  Blood Vol. 116, No. 21 ( 2010-11-19), p. 3979-3979
    Details
    In: Blood, American Society of Hematology, Vol. 116, No. 21 ( 2010-11-19), p. 3979-3979
    Abstract: Abstract 3979 Although treatment results for Chronic Lymphocytic Leukemia (CLL) have improved considerably over the last decade, unfortunately a curative treatment is still not available. In part this might be due to the interaction of CLL cells with their micro-environment in lymph nodes, spleen and bone marrow. Micro-environment derived signals are not only capable of driving proliferation of CLL cells, but can also induce resistance of CLL to cytotoxic drugs. Previously we have shown that in vitro CD40 stimulation of peripheral blood derived CLL cells can to a certain extent mimic the lymph node microenvironment and result in resistance to cytotoxic drugs (Kater AP et al. Br J Haematol 2004;127:404; Smit LA et al. Blood 2007;109:1660.; Hallaert DY et al. Blood 2008;112:5141). At present it is not known whether sensitivity of CLL cells to CD20 monoclonal antibodies (mAbs) is modulated by micro environmental stimuli. Therefore in the present study we investigated anti-CD20 mediated cell death of CD40-stimulated CLL cells from 17 CLL patients. We observed that in sharp contrast with the response towards cytotoxic drugs, CD40 stimulation sensitizes CLL cells to cell death mediated by anti-CD20 mAbs. In CD40-stimulated CLL cells, cell death induced by both Rituximab (a type I anti-CD20 mAb) and GA101 (a novel type II anti-CD20 mAb) (Moessner E et al. Blood, 2010;127:404, 115(22):4393-402) is increased. Both anti-CD20 mAbs induce a non-apoptotic, caspase- and p53-independent rapid cell death, but interestingly the mechanism of Rituximab and GA101-induced cell death appears to be different. Rituximab-induced cell death is dependent on extracellular Ca2+ and ROS production and CD40 stimulation sensitizes CLL cells by increasing basal ROS production. In contrast, GA101 induces cell death via a lysosome-dependent mechanism and CD40 stimulation sensitizes CLL cells by increasing the lysosomal volume of the cell. Moreover, in contrast to Rituximab, GA101 induces cell death in the absence of a secondary crosslinking mAb. Combination of GA101 with fludarabine, chlorambucil, bortezomib or bendamustine shows additive effects and results in strong cell death of CD40-stimulated CLL cells, even in p53 dysfunctional CLL cells. Our findings not only provide a rationale for combining cytotoxic drugs and anti-CD20 monoclonal antibodies, but also show that GA101 is a potent promising new anti-CD20 mAb for the treatment of CLL. Disclosures: Klein: Roche: Employment, Equity Ownership, Patents & Royalties.
    Type of Medium: Online Resource
    ISSN: 0006-4971 , 1528-0020
    URL: Article
    DOI: 10.1182/blood.V116.21.3979.3979
    RVK:
    XA 33000
    RVK:
    XA 10000
    Language: English
    Publisher: American Society of Hematology
    Publication Date: 2010
    detail.hit.zdb_id: 1468538-3
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  • 7
    Online Resource
    Online Resource
    Crystal Structure Analysis Reveals That the Novel Type II Anti-CD20 Antibody GA101 Interacts with a Similar Epitope as Rituximab and Ocrelizumab but in a Fundamentally Different Way.
    American Society of Hematology ; 2009
    In:  Blood Vol. 114, No. 22 ( 2009-11-20), p. 3726-3726
    Details
    In: Blood, American Society of Hematology, Vol. 114, No. 22 ( 2009-11-20), p. 3726-3726
    Abstract: Abstract 3726 Poster Board III-662 CD20 is a specific cell surface marker found on normal as well as malignant B cells. Rituximab, a monoclonal antibody directed against CD20, has a major impact on treatment of malignant lymphomas. Although all therapeutic CD20 antibodies are directed against the two relatively small extracellular loops of CD20, such antibodies can be classified into Type I CD20 antibodies like Rituximab, Ofatumumab or Ocrelizumab or Type II CD20 antibodies like the novel glycoengineered humanized CD20 antibody GA101 or the murine antibody Tositumumab. Type I and Type II antibodies differ significantly in their mode of action and mechanisms of killing malignant B-cells. The molecular basis of this is not understood. We use data from epitope mapping, X-ray crystallography, isothermal titration calorimetry, and point mutagenesis i) to accurately map the epitopes of different anti-CD20 antibodies, in particular GA101, and ii) to compare the molecular interactions involved in their binding. Although the epitope regions of these antibodies largely overlap, the crystal structure shows that GA101 binds CD20 in a completely different orientation from Rituximab, Ocrelizumab and Ofatumumab and that its binding also involves a larger surface area. In agreement with predictions based on the crystallographic data, point mutagenesis of single amino acid residues confirmed that exchanges at certain positions in CD20 affect binding of Rituximab and GA101 differently. Our data suggest that engagement of CD20 by these antibodies favors different conformations of CD20, which could form the molecular basis for the observed differences in cellular signals triggered by the respective antibodies. Disclosures: Niederfellner: Roche: Employment. Schwaiger:Roche: Employment. Georges:Roche: Employment. Wiechmann:Roche: Research Funding. Franke:Roche: Research Funding. Schaefer:Roche: Employment. Jenewein:Roche: Employment. Slootstra:Pepscan: Employment, Patents & Royalties. Moessner:Glycart: Employment, Equity Ownership, Patents & Royalties. Umana:Glycart: Employment, Equity Ownership, Patents & Royalties. Hopfner:Roche: Research Funding. Klein:Roche: Employment, Equity Ownership, Patents & Royalties.
    Type of Medium: Online Resource
    ISSN: 0006-4971 , 1528-0020
    URL: Article
    DOI: 10.1182/blood.V114.22.3726.3726
    RVK:
    XA 33000
    RVK:
    XA 10000
    Language: English
    Publisher: American Society of Hematology
    Publication Date: 2009
    detail.hit.zdb_id: 1468538-3
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  • 8
    Online Resource
    Online Resource
    The Triple Combination of the CD20 Antibody Obinutuzumab with the Bcl-2 Inhibitor Venetoclax (GDC-199) and the MDM2 Inhibitor Idasanutlin Results in Superior Efficacy and Long Term Response in Wildtype p53 NHL Tumor Models
    American Society of Hematology ; 2016
    In:  Blood Vol. 128, No. 22 ( 2016-12-02), p. 4178-4178
    Details
    In: Blood, American Society of Hematology, Vol. 128, No. 22 ( 2016-12-02), p. 4178-4178
    Abstract: Introduction: Previous preclinical studies have shown that the CD20 antibody obinutuzumab achieved greater anti-tumor efficacy together with the Bcl-2 inhibitor venetoclax (GDC-199) (Sampath et al, Blood 122 (21), 4412), and the MDM2 inhibitor idasanutlin (RG7388) (Herting et al., Blood 124 (21), 1780). Clinical combination studies combining obinutuzumab with venetoclax (NCT01685892) or idasanutlin (NCT02624986) are currently ongoing. Based on the data we investigated whether the triple combination of obinutuzumab with venetoclax and idasanutlin can further improve outcome in two preclinical human wildtype p53 NHLtumor xenograft models. Experimental Methods: The in vivo antitumor efficacy of the triple combination and the respective double combinations and monotherapies was evaluated in two different CD20 positive p53 wildtype xenograft models in female SCID beige mice bearing established s.c. human DoHH-2 diffuse large B cell lymphoma (DLBCL) or human Z-138 mantle cell lymphoma (MCL) tumors. In the DoHH-2 model, mice were treated when tumors reached 200 mm3 with vehicle control, obinutuzumab (ip, 10 mg/kg, q7d, days 13, 21, 27), idasanutlin (po, 30 mg/kg, days 13-17, 20-24, 27-29) or venetoclax (po, 100 mg/kg, days 13-29). One study group received the triple combination at the indicated days. In the Z-138 model, mice were treated when the tumors reached 500 mm3 with vehicle control, a sub-optimal dose of obinutuzumab (ip, 0.5 mg/kg, q7d, days 18, 25, 32), idasanutlin (po, 100 mg/kg, days 18-22, 80 mg/kg days 25-36) or venetoclax (po, 100 mg/kg, daily, days 18-36). In the combination groups, obinutuzumab, idasanutlin and venetoclax were administered at the same dosages and on the same days. Results: In the DoHH-2 model all monotherapies resulted in significant anti-tumor efficacy with 56% tumor growth inhibition (TGI) for idasanutlin (npTCR 0.48, CI 0.33-0.68), 60% TGI for venetoclax (npTCR 0.43, CI 0.27-0.67) and a TGI of 90% for obinutuzumab (npTCR 0.17, CI 0.08-2.24). Superior efficacy compared to the respective monotherapies was observed for the triple combination group which induced tumor regression in 90% of the animals with 30% reaching complete tumor remission (npTCR 0.009, CI 0.00-0.02). In the Z-138 model monotherapy treatment using obinutuzumab, venetoclax or idasanutlin resulted in TGI of 47 % (npTCR 0.56, CI 0.42 - 0.76), 53% (npTCR 0.50, CI 0.40 - 0.64) or 67% (npTCR 0.43, CI 0.32 - 0.55), respectively. Combination of obinutuzumab with venetoclax or idasanutlin yielded a TGI of 85% (npTCR 0.26, CI 0.20 - 0.34) or 86% (npTCR 0.26, CI 0.19 - 0.35), respectively. Combination of idasanutlin with venetoclax and the triple combination showed tumor regression (TGI 〉 100%) on day 32. To elucidate the long term effects a time-to-event (TTE) analysis was performed until study termination on day 125. Whereas, monotherapy with obinutuzumab at the suboptimal dose of 0.5 mg/kg resulted in 2/10 and the combination of idasanutlin and venetoclax in 5/10 tumor-free animals, the triple combination resulted in a complete tumor remission in 10/10 animals until study termination on day 125. Conclusions: These preclinical data demonstrate a strong anti-tumoral efficacy of combining the CD20 antibody obinutuzumab with the Bcl-2 inhibitor venetoclax and the MDM2 inhibitor idasanutlin, in particular regarding complete tumor remissions and long term response, and support the clinical investigation of this triple combination for the treatment of B cell malignancies. Disclosures Herting: Roche: Employment, Equity Ownership, Patents & Royalties: Roche. Friess:Roche: Employment, Equity Ownership, Patents & Royalties: Roche. Umaña:Roche: Employment, Equity Ownership, Patents & Royalties. Steven:Roche: Employment, Equity Ownership. Klein:Roche: Employment, Equity Ownership, Patents & Royalties.
    Type of Medium: Online Resource
    ISSN: 0006-4971 , 1528-0020
    URL: Article
    DOI: 10.1182/blood.V128.22.4178.4178
    RVK:
    XA 33000
    RVK:
    XA 10000
    Language: English
    Publisher: American Society of Hematology
    Publication Date: 2016
    detail.hit.zdb_id: 1468538-3
    detail.hit.zdb_id: 80069-7
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  • 9
    Online Resource
    Online Resource
    Enhanced Activity of GA101, a Novel Type II, Glycoengineered CD20 Antibody, In Combination with Bendamustine or Fludarabine, and with the Bcl-2 Family Inhibitors ABT-737 or ABT-263
    American Society of Hematology ; 2010
    In:  Blood Vol. 116, No. 21 ( 2010-11-19), p. 3915-3915
    Details
    In: Blood, American Society of Hematology, Vol. 116, No. 21 ( 2010-11-19), p. 3915-3915
    Abstract: Abstract 3915 GA101 is type II, glycoengineered CD20 antibody currently in PhII/III clinical trials. GA101 mediates enhanced direct cell death with a concomitant reduction of CDC; and high ADCC induction due to increased affinity for FcgRIIIa. We have shown that GA101 compared to rituximab mediates superior efficacy in NHL xenograft models including the induction of complete tumor remission. In clinical practice the combination of rituximab with chemotherapy e.g. CHOP, CVP, bendamustine, fludarabine or FC results in a substantial clinical benefit. To assess the potential of GA101 for combination with bendamustine or fludarabine, in vivo combination studies in s.c. Z138 (MCL) xenografts in Scid beige mice were devised. GA101 and rituximab at sub-optimal doses of 1 mg/kg (once weekly) were combined with 3 mg/kg bendamustine (days 19, 20, 21, 22); or with 40 mg/kg fludarabine (days 22, 23, 24) and compared to the corresponding monotherapy arms. GA101 in combination with bendamustine mediated statistically superior efficacy in terms of tumor growth inhibition (TGI) compared to the combination of rituximab and bendamustine: TGI values on day 33 were 29% for rituximab, 42% for rituximab + bendamustine, 47% for GA101 and 72% for GA101 + bendamustine. Treatment with bendamustine did not show significant antitumor activity. Statistical evaluation based on sAUC showed a more than additive and significant effect on tumor growth for the combination of GA101 with bendamustine compared to the corresponding monotherapy arms. GA101 in combination with fludarabine demonstrated statistically superior efficacy in terms of TGI and yielded a significant difference compared to the combination of rituximab and fludarabine or GA101 as monotherpy. TGI values on day 36 were 50% for fludarabine, 60% for rituximab, 85% for rituximab + fludarabine, 86% for GA101 and 〉 100% for GA101 + fludarabine. Furthermore, the superiority of the GA101-fludarabine combination was demonstrated by the observation of 3 tumor-free animals at the end of the study. ABT-263 (navitoclax) is a Bcl-2 family inhibitor that is currently in Phase I/II clinical trials for lymphoid malignancies. To provide evidence that GA101 can be combined with ABT-263 and the experimental Bcl-2 family inhibitor ABT-737, in vivo combination studies in s.c. SU-DHL4 (DLBCL) xenografts in Scid beige mice were devised. 10 mg/kg GA101 and rituximab (once weekly) were combined with 50 mg/kg ABT-737 (i.p., days 19, 22, 24, 26, 29, 31, 33). In a second study, 3 mg/kg GA101 or 10 mg/kg rituximab (once weekly) were combined with 100 mg/kg ABT-263 (orally, once daily). GA101 at a sub-optimal dose of 10 mg/kg demonstrated statistically superior efficacy in combination with ABT-737 in terms of tumor growth inhibition compared to GA101 alone or the combination of 10 mg/kg rituximab and ABT-737. Both combination treatments were statistically significant compared to the corresponding monotherapy arms. TGI values based on means on day 36 were 20% for ABT-737, 45% for rituximab, 92% for rituximab + ABT-737, 96% for GA101 and 〉 100% for GA101 + ABT-737. The superiority of the combination of GA101 and ABT-737 was supported by complete tumor regression in all animals whereas none was observed with the combination of rituximab and ABT-737. GA101 at a sub-optimal dose of 3 mg/kg or rituximab at a dose of 10 mg/kg mediated statistically superior efficacy in terms of tumor growth inhibition in combination with ABT-263 compared to the respective monotherapy arms. TGI values based on means on day 43 were 15% for ABT-263, 89% for rituximab, 〉 100% for rituximab + ABT-263, 80% for GA101 (at the sub-optimal dose) and 〉 100% for GA101 (sub-optimal dose) + ABT-263. Taken together i) GA101 as single agent was at least as efficacious as the combination of rituximab with bendamustine, fludarabine or ABT-737; ii) the combination of GA101 with bendamustine or fludarabine was superior to the respective monotherapy arms and resulted in an enhanced, at least additive effect of the combination; iii) the combination of GA101 with Bcl-2 family inhibitors ABT-737 and ABT-263 was superior to the respective monotherapy arms and resulted in an enhanced effect of the combination including the induction of tumor remission. These data strongly support the further clinical investigation of GA101 in combination with Fludarabine, Bendamustine or Bcl-2 family inhibitors. Disclosures: Herting: Roche: Employment. Bader:Roche: Employment. Umana:Roche: Employment, Equity Ownership. Klein:Roche: Employment, Equity Ownership.
    Type of Medium: Online Resource
    ISSN: 0006-4971 , 1528-0020
    URL: Article
    DOI: 10.1182/blood.V116.21.3915.3915
    RVK:
    XA 33000
    RVK:
    XA 10000
    Language: English
    Publisher: American Society of Hematology
    Publication Date: 2010
    detail.hit.zdb_id: 1468538-3
    detail.hit.zdb_id: 80069-7
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  • 10
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    Online Resource
    Obinutuzumab (GA101) Is Less Prone to Antagonism of Immune Effector Function By Ibrutinib Than Rituximab in Vitro and in Vivo
    American Society of Hematology ; 2014
    In:  Blood Vol. 124, No. 21 ( 2014-12-06), p. 1765-1765
    Details
    In: Blood, American Society of Hematology, Vol. 124, No. 21 ( 2014-12-06), p. 1765-1765
    Abstract: Introduction: Kohrt et al., Blood, 2014 demonstrated that ibrutinib antagonizes ADCC function of rituximab in vitro in ADCC assays and in vivo in the DHL-4 xenograft model through inhibition of FcgammaR signaling in immune effector cells, possibly mediated by inhibition of ITK. Obinutuzumab (GA101) is a glycoengineered type II CD20 antibody that mediates higher direct cell death induction than rituximab, and by being glycoengineered mediates enhanced induction of ADCC and ADCP. Here we aimed to investigate the impact of ibrutinib on the immune effector function of obinutuzumab as compared to rituximab. Experimental methods: The impact of ibrutinib (dose range 30, 100, 300 ng/ml to cover Cmax and Ctrough in patients) on NK cell mediated ADCC induction by obinutuzumab and rituximab was investigated using SU-DHL4 and Z138 cells as targets in LDH and chromium release assays or measuring CD16 downmodulation and the degranulation marker CD107a. IFNg release as a surrogate for NK cell activation was investigated using DHL-4 target cells or an autologous in vitro system using leukemic cells derived from CLL/NHL patients. Depletion of CD19 positive B-cells was determined in whole blood from healthy volunteers in flow cytometry-based whole blood assay. In vivo the combination of obinutuzumab or rituximab (10 mg/kg once weekly for 3 weeks) with ibrutinib (25mg/kg BID days 14-28) was investigated in the DHL-4 xenograft model. Results: In ADCC assays, ibrutinib (dose range 30, 100, 300 ng/ml) resulted in a reduction of the ADCC potency of obinutuzumab and rituximab. However, at saturating antibody concentrations of 10 ug/ml, ADCC mediated by obinutuzumab was retained while ADCC mediated by rituximab was strongly reduced as measured by chromium release (Figure 1A). Interestingly, in the whole blood B cell depletion assay only little impact of ibrutinib on obinutuzumab-mediated B cell depletion in terms of EC50 and maximal killing was observed at clinically meaningful concentrations of ibrutinib (30, 100, 300 ng/ml), while the activity of rituximab could be completely abolished with 300 ng/ml ibrutinib (Figure 1B). Notably, control experiments using an effector dead version of obinutuzmab that cannot any longer mediate ADCC or ADCP demonstrate that the retained B cell depletion by obinutuzumab in presence of ibrutinib is not due to direct cell death induction, but also due to immune effector cell mediated function (ADCC and ADCP). In the DHL-4 xenograft model where ibrutinib as a single agent has no anti-tumoral efficacy, the combination resulted in a reduced anti-tumoral efficacy of rituximab, whereas efficacy of obinutuzumab was not affected (Figure 1C). Conclusions: Surprisingly, we found that the inhibitory effect of ibrutinib on the immune effector mediated activity of obinutuzumab is not observed when compared to rituximab. Most notably, ADCC at saturating antibody doses, whole blood B cell depletion and in vivo efficacy of obinutuzumab were retained in presence of clinically relevant concentrations of ibrutinib covering Cmax and Ctrough levels, whereas the activity of rituximab was almost completely abolished under these conditions. We hypothesize that the differential behavior of obinutuzumab and rituximab may be related to the enhanced FcgRIII affinity and stronger FcgRIII signaling activation mediated by obinutuzumab as a consequence of glycoengineering that may subsequently overwrite inhibitory effects of ibrutinib. While the clinical relevance of the observed preclinical antagonism for the combination of rituximab with ibrutinib still needs further clinical investigation, these preclinical data strongly support the clinical investigation of ibrutinib in combination with the glycoengineered Type II CD20 antibody obinutuzumab for the treatment of chronic lymphocytic leukemia and other B-cell malignancies. Figure 1 Figure 1. Disclosures Herter: Roche: Employment. Bacac:Roche: Employment. Umana:Roche: Employment. Klein:Roche: Employment, Equity Ownership, Patents & Royalties.
    Type of Medium: Online Resource
    ISSN: 0006-4971 , 1528-0020
    URL: Article
    DOI: 10.1182/blood.V124.21.1765.1765
    RVK:
    XA 33000
    RVK:
    XA 10000
    Language: English
    Publisher: American Society of Hematology
    Publication Date: 2014
    detail.hit.zdb_id: 1468538-3
    detail.hit.zdb_id: 80069-7
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