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53. Laxens nedströmsvandring mot fiskavledare till Stornorrfors fisktrappa i Umeälvens nedre del

Author

Lundqvist, Hans, Leonardsson, Kjell, Lindberg, Dan-Erik, Westbergh, Stig, Forssén, Åke, and Hellström, J. Gunnar I.

Subjects
Fluid Mechanics and Acoustics, Ecology, Forest Science, Fish and Aquacultural Science, Strömningsmekanik och akustik
Abstract

Rapporten sammanfattar våra arbeten med målsättning att skapa en fungerande fiskavledning för nedströmsvandrande fisk i vid Stornorrfors kraftverkskomplex i Umeälven. Rapporten visar även på verksamheter som nyttjats vid planering och utvärdering av gjorda åtgärder. Åtgärder i fisktrappan, fiskavledare och utrustning för registrering av PIT-tags har möjliggjorts genom finansiering av Europeiska Fiskefonden, Havs- och Vattenmyndigheten, Umeå kommun, Vattenfall och SLU. Arbetena har genomförts som två pilotprojekt (3b Nedströmsvandring Stornorrfors 2009-2010 och 3b2 Nedströmsvandring Stornorrfors 2011-2013). Vilda lax- och öring bestånd i våra älvar är viktiga naturresurser för människan och ekosystemet. Vindelälvens naturliga fiskproduktion av lax- och havsöring ungar är betydande för Östersjöns laxbestånd. De senaste åren har mer än 10 000 lax årligen vandrat uppströms för lek i älven. Många föräldrafiskar (Kelt, vraklax, besa, mm) överlever leken och vill vandra tillbaka till havet. Laxens naturliga avkomma, smolten, strävar också att ta sig till födoområdena i Östersjön. I flödesreglerade vattendrag som Umeälven med sitt unika laxbestånd i biflödet Vindelälven finns problem med dödlighet då kelt och smolt på sin nedströmsvandring ska passera Stornorrfors kraftverk. I Umeälvens nedre del färdigställdes en ny fisktrappa i Norrfors 2010 som utrustats med en ”fiskavledare”. Projektets mål var att bygga och ansluta fiskavledaren till nya fisktrappan och utvärdera dess funktion/effektivitet. Det mätbara målet för den planerade anläggningen vid Stornorrfors utskovsdamm sattes till att 75 % av den utvandrande vilda smolten och minst 50 % av den övervintrande kelten skulle avledas till nya fisktrappan för vidare vandring till havet. Detta mål kunde inte uppnås. Den nya fisktrappan skulle alltså fungera som ett klassiskt "omlöp" förbi kraftverket. Vild smolt har märkts med Passiva Integrerade Transpondrar (PIT) eller aktiva Radiomärken (RT) och senare skannats vid passage i fisktrappsområdet (PIT + RT-märkt fisk) eller vid intaget till Stornorrfors kraftverk (RT-märkt fisk). SLU’s utvärdering av ledarmens funktion och fiskens vandring nedströms har visat att fiskavledarens funktion varit mycket svår att kontrollera då ledarmen inte fungerat som tänkt i den tuffa strömmiljön ovan fisktrappans område mellan 2010-2012. Avledningseffektiviteten kunde med visst förtroende endast värderas vid 2013 års försök med PIT-märkt fisk (n=1749 fiskar) som släpptes dagligen efter fångst i Vindelälven (INDEX Spöland) när flödet var < 800 m3/s i älven. Den totala avledningseffektiviteten visade sig vara 4,5 %. Begränsande för utvärderingen har varit att stora grupper smolt periodvis inte kunnat fångas och märkas på grund av höga flöden i Vindelälven. Effektiviteten i ledarmen har varierat mellan 0 och 100 % under säsongen. Väldigt få Kelt av lax kunde avledas. Höga turbinflöden tycks haft en positiv inverkan på ledarmens funktion. Smoltens passage nedströms i och genom fisktrappan verkar fungera utan större problem. Via PIT-märkt fisk och videofilmning i flera delförsök kunde vi visa på en lyckad genomfart där laxsmolten passerar fisktrappan inom några timmar till 2-3 dagar. Flödesmätning och modellering av strömningen runt fiskavledarens område mot ingången till nya fisktrappan visar att ledarmen borde ökas till ca 150 meters längd istället för dagens 110 meter. Flödesmodelleringar visar då att en större del av ytströmmen kan styras in mot fisktrappans ingång. Försöken med fångst, märkning, utsättning och återfångst har fungerat bra och PIT-märkningstekniken bedöms överlägsen andra märktekniker för detektering av fisk om detekteringsutrustning installerats. Detta kan utvecklas vidare inom ramen för indexälvsverksamheten (ICES-DCF) som nu bedrivs i Vindelälven. Sverige bör fortsätta att ta ansvar för den här typen av utveckling då det finns samordningsvinster mellan indexvattendrag, fiskavledning och utvärdering av fisktrappan för lekvandrande fisk. Lyckas man avleda den naturligt producerade avkomman av lax och öring i reglerade vattendrag med unika bestånd finns mycket att vinna för att etablera långsiktigt hållbara bestånd av vandringsfisk. Den typ av fiskavledare som nu prövats har tidigare inte prövats i Europa varför detta pilotprojekt är unikt. Arbetet som nu avslutats har varit ett samverkansprojekt mellan Europeiska Fiskerifonden, Havs- och Vattenmyndigheten, vattenkraftsägare, lokala och nationella fiskeriadministratörer samt forskare i fiskbiologi och hydraulik.

Published
2014

54. Uppströmsvandring i den restaurerade gamla älvfåran samt funktionskontroll av ny fisktrappa i Norrfors (Umeälven) under laxens vandringssäsong 2012-2013

Author

Leonardsson, Kjell, Karlsson, Robert, Nilsson, Jan, and Lundqvist, Hans

Subjects
Ecology, Fish and Aquacultural Science
Abstract

Rapporten sammanfattar 2012 och 2013 års funktionskontroll av fisktrappan samt uppföljning av restureringsåtgärder i Umeälvens nedre del. Lax fångades, märktes och släpptes nedströms utskovet vid dammen i Norrfors 2012 och i älvens mynningsområde vid Långhalsudden (Obbola) 2013. Under 2012 märktes 104 vilda laxar med aktiva radio- och passiva PIT-märken, samt 278 laxar som enbart märktes med PIT-märken. Under 2013 märktes 148 vilda laxar med både aktiva radio- och passiva PIT-märken, samt 216 vilda och 33 odlade laxar som enbart märktes med PIT-märken. Återvändande vuxenlax som tidigare PIT-märkts som smolt i Spöland eller i fiskodlingen inkluderades också i analyserna. Ett fenprov för DNA-analys togs från alla radiomärkta fiskar innan frisläppning för bestämning av laxens stamtillhörighet. 2012 hade ca 85 % av den märkta laxen Ume/Vindelälvsursprung, medan resterande lax hade en genetisk uppsättning som påminde om Luleälvslax trots intakt fettfena. 2013 befanns alla märkta laxar vara av Ume/Vindelälvsursprung. Radiomärkt fisk registrerades när de kom i närheten av fasta automatiska undervattens- eller luftantenner som placerats i sammanflödet, i den gamla älvfåran som restaurerats med vilpooler samt vid fisktrappan och uppströms i Vindelälven. PIT-märkt fisk detekterades när de passerade antenner som monterats i fisktrappans mellanväggar samt när de kom i närheten av den plattdetektor som installerades i Baggböleforsens nedre poolvägg 2013. All fisk som passerade fisktrappans övre del räknades via en sk VAKI utrustning.

Published
2013

58. Prospective observational study of 177Lu-DOTA-octreotate therapy in 200 patients with advanced metastasized neuroendocrine tumours (NETs): feasibility and impact of a dosimetry-guided study protocol on outcome and toxicity.

Author

Garske-Román, Ulrike, Sandström, Mattias, Fröss Baron, Katarzyna, Lundin, Lars, Hellman, Per, Welin, Staffan, Johansson, Silvia, Khan, Tanweera, Lundqvist, Hans, Eriksson, Barbro, Sundin, Anders, and Granberg, Dan

Subjects
NEUROENDOCRINE tumors, RADIATION dosimetry, PEPTIDE receptors, RADIOISOTOPES, DISEASE progression, ACUTE leukemia
Abstract

Purpose: Peptide receptor radionuclide therapy in patients with neuroendocrine tumours has yielded promising results. This prospective study investigated the feasibility of dosimetry of the kidneys and bone marrow during therapy and its impact on efficacy and outcome.Methods: The study group comprised 200 consecutive patients with metastasized somatostatin receptor-positive neuroendocrine tumours progressing on standard therapy or not suitable for other therapeutic options. A treatment cycle consisted of 7.4 GBq 177Lu-DOTA-octreotate with co-infusion of a mixed amino acid solution, and cycles were repeated until the absorbed dose to the kidneys reached 23 Gy or there were other reasons for stopping therapy. The Ki-67 index was ≤2% in 47 patients (23.5%), 3-20% in 121 (60.5%) and >20% in 16 (8%).Results: In 123 patients (61.5%) the absorbed dose to the kidneys reached 23 Gy with three to nine cycles during first-line therapy; in no patient was a dose to the bone marrow of 2 Gy reached. The best responses (according to RECIST 1.1) were a complete response (CR) in 1 patient (0.5%), a partial response (PR) in 47 (23.5%), stable disease (SD) in 135 (67.5%) and progressive disease (PD) in 7 (3.5%). Median progression-free survival was 27 months (95% CI 22-30 months) in all patients, 33 months in those in whom the absorbed dose to the kidneys reached 23 Gy and 15 months in those in whom it did not. Median overall survival (OS) was 43 months (95% CI 39-53 months) in all patients, 54 months in those in whom the absorbed dose to the kidneys reached 23 Gy and 25 months in those in whom it did not. Median OS was 60 months in patients with a best response of PR or CR, 42 months in those with SD and 16 months in those with PD. Three patients (1.5%) developed acute leukaemia, 1 patient (0.5%) chronic leukaemia (unconfirmed) and 30 patients (15%) grade 3 or 4 bone marrow toxicity. Eight patients (4%) developed grade 2 kidney toxicity and one patient (0.5%) grade 4 kidney toxicity.Conclusions: Dosimetry-based therapy with 177Lu-DOTA-octreotate is feasible. Patients in whom the absorbed dose to the kidneys reached 23 Gy had a longer OS than those in whom it did not. Patients with CR/PR had a longer OS than those with SD. Bone marrow dosimetry did not predict toxicity. [ABSTRACT FROM AUTHOR]

Published
2018
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60. A numerical study of the location and function of the entrance of a fishway in a regulated river

Author

Andersson, Anders G., Lindberg, Dan-Erik, Lindmark, Elianne, Leonardsson, Kjell, Andreasson, Patrik, Lundqvist, Hans, and Lundström, Staffan

Subjects
Fluid Mechanics and Acoustics, Strömningsmekanik och akustik
Abstract

Simulation driven design with Computational Fluid Dynamics has been used to evaluate the flow downstream a hydropower plant with regards to upstream migrating fish. Field measurements with an Acoustic Doppler Current Profiler were performed and the measurements were used to validate the simulations. The measurements indicate a more unstable flow than the simulations and the tailrace jet from the turbines is stronger in the simulations. The simulations are however considered to capture the important features of the flow in a way that makes them viable for attraction water simulations. A fishway entrance was included in the simulations and the subsequent attraction water was evaluated for two positions and two angles of the entrance at different turbine discharges. Results show that both positions are viable and that a position where the flow from the fishway does not have to compete with the flow from the power plant will generate superior attraction water. Simulations were also performed further downstream where the flow from the turbines meets the old river bed which is the current fish passage for upstream migrating fish. A modification of the old river bed was made in the model as one scenario to generate better attraction water. This considerably increases the attraction water although it cannot compete with the flow from the tailrace tunnel. Godkänd; 2010; 20101119 (aneane)

Published
2010

62. Quantitative and Qualitative Intrapatient Comparison of 68Ga-DOTATOC and 68Ga-DOTATATE : Net Uptake Rate for Accurate Quantification.

Author

Velikyan, Irina, Sundin, Anders, Sörensen, Jens, Lubberink, Mark, Sandström, Mattias, Garske-Román, Ulrike, Lundqvist, Hans, Granberg, Dan, Eriksson, Barbro, Velikyan, Irina, Sundin, Anders, Sörensen, Jens, Lubberink, Mark, Sandström, Mattias, Garske-Román, Ulrike, Lundqvist, Hans, Granberg, Dan, and Eriksson, Barbro

Abstract

UNLABELLED: Quantitative imaging and dosimetry are crucial for individualized treatment during peptide receptor radionuclide therapy (PRRT). (177)Lu-DOTATATE and (68)Ga-DOTATOC/(68)Ga-DOTATATE are used, respectively, for PRRT and PET examinations targeting somatostatin receptors (SSTRs) in patients affected by neuroendocrine tumors. The aim of the study was to quantitatively and qualitatively compare the performance of (68)Ga-DOTATOC and (68)Ga-DOTATATE in the context of subsequent PRRT with (177)Lu-DOTATATE under standardized conditions in the same patient as well as to investigate the sufficiency of standardized uptake value (SUV) for estimation of SSTR expression. METHODS: Ten patients with metastatic neuroendocrine tumors underwent one 45-min dynamic and 3 whole-body PET/CT examinations at 1, 2, and 3 h after injection with both tracers. The number of detected lesions, SUVs in lesions and normal tissue, total functional tumor volume, and SSTR volume (functional tumor volume multiplied by mean SUV) were investigated for each time point. Net uptake rate (Ki) was calculated according to the Patlak method for 3 tumors per patient. RESULTS: There were no significant differences in lesion count, lesion SUV, Ki, functional tumor volume, or SSTR volume between (68)Ga-DOTATOC and (68)Ga-DOTATATE at any time point. The detection rate was similar, although with differences for single lesions in occasional patients. For healthy organs, marginally higher uptake of (68)Ga-DOTATATE was observed in kidneys, bone marrow, and liver at 1 h. (68)Ga-DOTATOC uptake was higher in mediastinal blood pool at the 1-h time point (P = 0.018). The tumor-to-liver ratio was marginally higher for (68)Ga-DOTATOC at the 3-h time point (P = 0.037). Blood clearance was fast and similar for both tracers. SUV did not correlate with Ki linearly and achieved saturation for a Ki of greater than 0.2 mL/cm(3)/min, corresponding to an SUV of more than 25. CONCLUSION: (68)Ga-DOTATOC and (68)Ga-DOTATATE are

Published
2014
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63. Basin-scale phenology and effects of climate variability on global timing of initial seaward migration of Atlantic salmon (Salmo salar)

Author

Norwegian Research Council, Otero, Jaime, L'Abée-Lund, J. H., Castro-Santos, Ted, Leonardsson, Kjell, Storvik, Geir O., Jönsson, Bror F., Dempson, Brian, Russell, Ian C., Jensen, Arne J., Baglinière, Jean-Luc, Dionne, Mélanie, Armstrong, John D., Romakkaniemi, Atso, Letcher, Benjamin H., Kocik, John F., Erkinaro, Jaakko, Poole, Russell, Rogan, Ger, Lundqvist, Hans, MacLean, Julian C., Jokikokko, Erkki, Arnekleiv, Jo Vegar, Kennedy, Richard J., Niemelä, Eero, Caballero, Pablo, Music, Paul A., Antonsson, Thorolfur, Gudjonsson, Sigurdur, Veselov, Alexey E., Lamberg, Anders, Groom, Steve, Taylor, Benjamin H., Taberner, Malcolm, Dillane, Mary, Arnason, Fridthjofur, Horton, Gregg, Hvidsten, Nils A., Jonsson, Ingi R., Jonsson, Nina, McKelvey, Simon, Næsje, Tor F., Skaala, Øystein, Smith, Gordon W., Sægrov, Harald, Stenseth, Nils Christian, Vøllestad, Leif Asbjørn, Norwegian Research Council, Otero, Jaime, L'Abée-Lund, J. H., Castro-Santos, Ted, Leonardsson, Kjell, Storvik, Geir O., Jönsson, Bror F., Dempson, Brian, Russell, Ian C., Jensen, Arne J., Baglinière, Jean-Luc, Dionne, Mélanie, Armstrong, John D., Romakkaniemi, Atso, Letcher, Benjamin H., Kocik, John F., Erkinaro, Jaakko, Poole, Russell, Rogan, Ger, Lundqvist, Hans, MacLean, Julian C., Jokikokko, Erkki, Arnekleiv, Jo Vegar, Kennedy, Richard J., Niemelä, Eero, Caballero, Pablo, Music, Paul A., Antonsson, Thorolfur, Gudjonsson, Sigurdur, Veselov, Alexey E., Lamberg, Anders, Groom, Steve, Taylor, Benjamin H., Taberner, Malcolm, Dillane, Mary, Arnason, Fridthjofur, Horton, Gregg, Hvidsten, Nils A., Jonsson, Ingi R., Jonsson, Nina, McKelvey, Simon, Næsje, Tor F., Skaala, Øystein, Smith, Gordon W., Sægrov, Harald, Stenseth, Nils Christian, and Vøllestad, Leif Asbjørn

Abstract

Migrations between different habitats are key events in the lives of many organisms. Such movements involve annually recurring travel over long distances usually triggered by seasonal changes in the environment. Often, the migration is associated with travel to or from reproduction areas to regions of growth. Young anadromous Atlantic salmon (Salmo salar) emigrate from freshwater nursery areas during spring and early summer to feed and grow in the North Atlantic Ocean. The transition from the freshwater ('parr') stage to the migratory stage where they descend streams and enter salt water ('smolt') is characterized by morphological, physiological and behavioural changes where the timing of this parr-smolt transition is cued by photoperiod and water temperature. Environmental conditions in the freshwater habitat control the downstream migration and contribute to within- and among-river variation in migratory timing. Moreover, the timing of the freshwater emigration has likely evolved to meet environmental conditions in the ocean as these affect growth and survival of the post-smolts. Using generalized additive mixed-effects modelling, we analysed spatio-temporal variations in the dates of downstream smolt migration in 67 rivers throughout the North Atlantic during the last five decades and found that migrations were earlier in populations in the east than the west. After accounting for this spatial effect, the initiation of the downstream migration among rivers was positively associated with freshwater temperatures, up to about 10 °C and levelling off at higher values, and with sea-surface temperatures. Earlier migration occurred when river discharge levels were low but increasing. On average, the initiation of the smolt seaward migration has occurred 2.5 days earlier per decade throughout the basin of the North Atlantic. This shift in phenology matches changes in air, river, and ocean temperatures, suggesting that Atlantic salmon emigration is responding to the curre

Published
2014

64. Basin-scale phenology and effects of climate variability on global timing of initial seaward migration of Atlantic salmon (Salmo salar)

Author

Otero, Jaime, L'Abee-Lund, Jan Henning, Castro-Santos, Ted, Leonardsson, Kjell, Storvik, Geir O., Jonsson, Bror, Dempson, Brian, Russell, Ian C., Jensen, Arne J., Bagliniere, Jean-Luc, Dionne, Melanie, Armstrong, John D., Romakkaniemi, Atso, Letcher, Benjamin H., Kocik, John F., Erkinaro, Jaakko, Poole, Russell, Rogan, Ger, Lundqvist, Hans, MacLean, Julian C., Jokikokko, Erkki, Arnekleiv, Jo Vegar, Kennedy, Richard J., Niemela, Eero, Caballero, Pablo, Music, Paul A., Antonsson, Thorolfur, Gudjonsson, Sigurdur, Veselov, Alexey E., Lamberg, Anders, Groom, Steve, Taylor, Benjamin H., Taberner, Malcolm, Dillane, Mary, Arnason, Fridthjofur, Horton, Gregg, Hvidsten, Nils A., Jonsson, Ingi R., Jonsson, Nina, McKelvey, Simon, Naesje, Tor F., Skaala, Oystein, Smith, Gordon W., Saegrov, Harald, Stenseth, Nils C., Vollestad, Leif Asbjorn, Otero, Jaime, L'Abee-Lund, Jan Henning, Castro-Santos, Ted, Leonardsson, Kjell, Storvik, Geir O., Jonsson, Bror, Dempson, Brian, Russell, Ian C., Jensen, Arne J., Bagliniere, Jean-Luc, Dionne, Melanie, Armstrong, John D., Romakkaniemi, Atso, Letcher, Benjamin H., Kocik, John F., Erkinaro, Jaakko, Poole, Russell, Rogan, Ger, Lundqvist, Hans, MacLean, Julian C., Jokikokko, Erkki, Arnekleiv, Jo Vegar, Kennedy, Richard J., Niemela, Eero, Caballero, Pablo, Music, Paul A., Antonsson, Thorolfur, Gudjonsson, Sigurdur, Veselov, Alexey E., Lamberg, Anders, Groom, Steve, Taylor, Benjamin H., Taberner, Malcolm, Dillane, Mary, Arnason, Fridthjofur, Horton, Gregg, Hvidsten, Nils A., Jonsson, Ingi R., Jonsson, Nina, McKelvey, Simon, Naesje, Tor F., Skaala, Oystein, Smith, Gordon W., Saegrov, Harald, Stenseth, Nils C., and Vollestad, Leif Asbjorn

Abstract

Migrations between different habitats are key events in the lives of many organisms. Such movements involve annually recurring travel over long distances usually triggered by seasonal changes in the environment. Often, the migration is associated with travel to or from reproduction areas to regions of growth. Young anadromous Atlantic salmon (Salmo salar) emigrate from freshwater nursery areas during spring and early summer to feed and grow in the North Atlantic Ocean. The transition from the freshwater ('parr') stage to the migratory stage where they descend streams and enter salt water ('smolt') is characterized by morphological, physiological and behavioural changes where the timing of this parr-smolt transition is cued by photoperiod and water temperature. Environmental conditions in the freshwater habitat control the downstream migration and contribute to within- and among-river variation in migratory timing. Moreover, the timing of the freshwater emigration has likely evolved to meet environmental conditions in the ocean as these affect growth and survival of the post-smolts. Using generalized additive mixed-effects modelling, we analysed spatio-temporal variations in the dates of downstream smolt migration in 67 rivers throughout the North Atlantic during the last five decades and found that migrations were earlier in populations in the east than the west. After accounting for this spatial effect, the initiation of the downstream migration among rivers was positively associated with freshwater temperatures, up to about 10 °C and levelling off at higher values, and with sea-surface temperatures. Earlier migration occurred when river discharge levels were low but increasing. On average, the initiation of the smolt seaward migration has occurred 2.5 days earlier per decade throughout the basin of the North Atlantic. This shift in phenology matches changes in air, river, and ocean temperatures, suggesting that Atlantic salmon emigration is responding to the curre

Published
2014
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65. Site-Specific Radiometal Labeling and Improved Biodistribution Using ABY-027, A Novel HER2-Targeting Affibody Molecule-Albumin-Binding Domain Fusion Protein

Author

Orlova, Anna, Jonsson, Andreas, Rosik, Daniel, Lundqvist, Hans, Lindborg, Malin, Abrahmsen, Lars, Ekblad, Caroline, Frejd, Fredrik Y, Tolmachev, Vladimir, Orlova, Anna, Jonsson, Andreas, Rosik, Daniel, Lundqvist, Hans, Lindborg, Malin, Abrahmsen, Lars, Ekblad, Caroline, Frejd, Fredrik Y, and Tolmachev, Vladimir

Abstract

Because of their better penetration, smaller targeting proteins may be superior to antibodies for radioimmunotherapy of solid tumors. Therefore, Affibody molecules (6.5 kDa) have a potential for being suitable as targeted moiety for radiolabeled therapeutic proteins. Previous studies have demonstrated that a fusion of an Affibody molecule with an albumin-binding domain (ABD) provides a strong noncovalent binding to albumin in vivo. This strong noncovalent binding can be used for reduction of the renal uptake of the Affibody molecule while maintaining a size smaller than that of an antibody, which is important when using residualizing radionuclide labels conjugated to Affibody molecules. The goal of this study was to design and evaluate a new targeting Affibody–ABD fusion protein with improved biodistribution properties for radionuclide therapy. Methods: A novel Affibody-based construct, ZHER2:2891-ABD035-DOTA (ABY-027), was created by fusion of the reengineered HER2-binding Affibody molecule ZHER2:2891 to the N terminus of the high-affinity ABD035, and a maleimido-derivative of DOTA was conjugated at the C terminus of the construct. Binding and processing of 177Lu-ABY-027 by HER2-expressing cells were evaluated in vitro. Targeting of HER2-expressing SKOV-3 xenografts was evaluated in BALB/C nu/nu mice and compared with targeting of previously reported ABD-(ZHER2:342)2. Results: The binding affinity (dissociation constant) of ABY-027 to HER2 (74 pM) was the same as for the parental ZHER2:2891 (76 pM). ABY-027 was stably labeled with 177Lu and 111In with preserved specific binding to HER2-expressing cells in vitro. In vivo receptor saturation experiments demonstrated that targeting of SKOV-3 xenografts in BALB/C nu/nu mice was HER2-specific. 177Lu-ABY-027 demonstrated substantially (2- to 3-fold) lower renal and hepatic uptake than previously assessed HER2-specific Affibody-based albumin-binding agents. Tumor uptake of radiolabeled ABY-027 at 48 h after injection was

Published
2013
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66. Individualized dosimetry of kidney and bone marrow in patients undergoing 177Lu-DOTA-octreotate treatment

Author

Sandström, Mattias, Garske-Román, Ulrike, Granberg, Dan, Johansson, Silvia, Widström, Charles, Eriksson, Barbro, Sundin, Anders, Lundqvist, Hans, Lubberink, Mark, Sandström, Mattias, Garske-Román, Ulrike, Granberg, Dan, Johansson, Silvia, Widström, Charles, Eriksson, Barbro, Sundin, Anders, Lundqvist, Hans, and Lubberink, Mark

Abstract

The organs at risk in radionuclide therapy with 177Lu-octreotate are the bone marrow and the kidneys. The primary aim of this study was to develop an individualized dosimetry protocol for the bone marrow. The secondary aim was to identify those patients, undergoing fractionated therapy with 7.4 GBq/cycle, who first reached an accumulated dose of either 2 Gy to the bone marrow or 23 Gy to the kidneys. Methods: Two hundred patients with metastatic neuroendocrine tumors with high somatostatin receptor expression were included. After the administration of 7.4 GBq of 177Lu-octreotate, blood samples were drawn 6 times within the first 24 h. In 50 patients, additional blood samples were obtained at 96 and 168 h. Moreover, urine was collected from 30 patients during the first 24 h. Planar whole-body and SPECT/CT images over the abdomen were acquired at 24, 96, and 168 h after the infusion. Calculation of the absorbed radiation dose to the bone marrow was based on blood and urinary activity curves combined with organ-based analysis of the whole-body images. The absorbed dose to the kidney was calculated from the pharmacokinetic data obtained from SPECT/CT. Results: For a single cycle of 7.4 GBq, the absorbed dose to the bone marrow and the kidney ranged from 0.05 to 0.4 Gy and from 2 to 10 Gy, respectively. In 197 of 200 patients, the kidneys accumulated an absorbed dose of 23 Gy before the bone marrow reached 2 Gy. Between 2 and 10 cycles of 177Lu-octreotate could be administered before the upper dose limit for the individual patient was reached. Conclusion: A method based on repeated whole-body imaging in combination with blood and urinary activity data over time was developed to determine the absorbed dose to the bone marrow. The dose-limiting organ was the kidney in 197 of 200 patients. In 50% of the patients, more than 4 cycles of 7.4 GBq of 177Lu-octreotate could be administered, whereas 20% of the subjects were treated with fewer than 4 cycles. Individualized absorbed

Published
2013
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68. Comparative Biodistribution and Radiation Dosimetry of Ga-68-DOTATOC and Ga-68-DOTATATE in Patients with Neuroendocrine Tumors

Author

Sandström, Mattias, Velikyan, Irina, Garske-Roman, Ulrike, Sörensen, Jens, Eriksson, Barbro, Granberg, Dan, Lundqvist, Hans, Sundin, Anders, Lubberink, Mark, Sandström, Mattias, Velikyan, Irina, Garske-Roman, Ulrike, Sörensen, Jens, Eriksson, Barbro, Granberg, Dan, Lundqvist, Hans, Sundin, Anders, and Lubberink, Mark

Abstract

Ga-68-DOTATOC and Ga-68-DOTATATE are 2 radiolabeled somatostatin analogs for in vivo diagnosis of neuroendocrine tumors with PET. The aim of the present work was to measure their comparative biodistribution and radiation dosimetry. Methods: Ten patients diagnosed with neuroendocrine tumors were included. Each patient underwent a 45-min dynamic and 3 whole-body PET/CT scans at 1, 2, and 3 h after injection of each tracer on consecutive days. Absorbed doses were calculated using OLINDA/EXM 1.1. Results: Data from 9 patients could be included in the analysis. Of the major organs, the highest uptake at 1, 2, and 3 h after injection was observed in the spleen, followed by kidneys and liver. For both tracers, the highest absorbed organ doses were seen in the spleen and urinary bladder wall, followed by kidney, adrenals, and liver. The absorbed doses to the liver and gallbladder wall were slightly but significantly higher for Ga-68-DOTATATE. The total effective dose was 0.021 +/- 0.003 mSv/MBq for both tracers. Conclusion: The effective dose for a typical 100-MBq administration of Ga-68-DOTATATE and Ga-68-DOTATOC is 2.1 mSv for both tracers. Therefore, from a radiation dosimetry point of view, there is no preference for either tracer for PET/CT evaluation of somatostatin receptor-expressing tumors.

Published
2013
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69. Ny lag behövs för att skydda åar och älvar

Author

Nilsson, Christer, Greenberg, Larry, Humborg, Christoph, Lundqvist, Hans, Nilsson, Christer, Greenberg, Larry, Humborg, Christoph, and Lundqvist, Hans

Abstract

Vi vet idag mycket mer om de skadliga effekterna av dammar och flödesreglering, än vad som var känt då vattenkraften byggdes ut i Sverige. I en ny utredning föreslås också flera viktiga åtgärder där miljö och fiskvägar skyddas. Vi hoppas nu att Sveriges regering är beredd att ta steget och lagstifta för att genomföra de förslag som finns för att bättre skydda åar och älvar, skriver fyra professorer.

Published
2013

70. Experimental radionuclide therapy of HER2-expressing xenografts using two-step targeting Nuclisome-particles

Author

Gedda, Lars, Fondell, Amelie, Lundqvist, Hans, Park, John, Edwards, Katarina, Gedda, Lars, Fondell, Amelie, Lundqvist, Hans, Park, John, and Edwards, Katarina

Abstract

The therapeutic potential of Auger-electron emitting radionuclides is strongly dependent on their close vicinity to DNA, since the energy deposition is mainly localized within a few cubic nanometers around the site of decay. Thus, apart from specificity, successful tumor therapy relies on a nuclear delivery strategy. We recently presented a two-step targeting strategy to transport Auger-electron-emitting radionuclides into the cell nucleus by means of nuclide-filled liposomes (Nuclisome particles), that is, polyethylene glycol-stabilized, tumor-cell-targeting liposomes loaded with (125)I-labeled anthracyclines. In the present study, the survival of mice intraperitoneally inoculated with human HER2-expressing SKOV-3 tumor cells and treated with HER2-targeting Nuclisome particles was studied. METHODS: BALB/c nu/nu mice were inoculated with 10(7) SKOV-3 cells intraperitoneally and thereafter directly injected with Nuclisome particles with increasing specific radioactivity. Groups of 10-12 mice were treated with 0.01 MBq/mouse up to 2 MBq/mouse, and survival was monitored and compared with that in control groups (n = 33). Organs were analyzed for HER2 expression and radiotoxic effects histologically. Absorbed doses were estimated using dose factors from the online Radiation Dose Assessment Resource model. RESULTS: The results showed a clear correlation between administered radioactive dose and survival. No such dose-dependent survival was observed for mice treated with Nuclisome particles lacking HER2-targeting ability. With HER2-targeting Nuclisome particles, a significant increase in survival, compared with that of untreated control mice, could already be seen at an administered activity of 0.1 MBq/mouse (P = 0.0301). At the highest activity administered, 2 MBq/mouse (P < 0.0001), 70% of the mice survived the study and most were tumor-free. Neither macroscopic nor microscopic radiotoxic side effects were observed. Dosimetric calculations, assuming nonreceptor targe

Published
2012
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71. Exploring Co-57 as a new isotope for brachytherapy applications

Author

Enger, Shirin A., Lundqvist, Hans, D'Amours, Michel, Beaulieu, Luc, Enger, Shirin A., Lundqvist, Hans, D'Amours, Michel, and Beaulieu, Luc

Abstract

Purpose: The characteristics of the radionuclide Co-57 make it interesting for use as a brachytherapy source. Co-57 combines a possible high specific activity with the emission of relatively low-energy photons and a half-life (272 days) suitable for regular source exchanges in an afterloader. Co-57 decays by electron capture to the stable Fe-57 with emission of 136 and 122 keV photons. Methods: A hypothetical Co-57 source based on the Flexisource brachytherapy encapsulation with the active core set as a pure cobalt cylinder (length 3.5 mm and diameter 0.6 mm) covered with a cylindrical stainless-steel capsule (length 5 mm and thickness 0.125 mm) was simulated using Geant4 Monte Carlo (MC) code version 9.4. The radial dose function, g(r), and anisotropy function F(r,theta), for the line source approximation were calculated following the TG-43U1 formalism. The results were compared to well-known Ir-192 and 1(25)I radionuclides, representing the higher and the lower energy end of brachytherapy, respectively. Results: The mean energy of photons in water, after passing through the core and the encapsulation material was 123 keV. This hypothetical Co-57 source has an increasing g(r) due to multiple scatter of low-energy photons, which results in a more uniform dose distribution than Ir-192. Conclusions: Co-57 has many advantages compared to Ir-192 due to its low-energy gamma emissions without any electron contamination. Co-57 has an increasing g(r) that results in a more uniform dose distribution than Ir-192 due to its multiple scattered photons. The anisotropy of the Co-57 source is comparable to that of Ir-192. Furthermore, Co-57 has lower shielding requirements than Ir-192.

Published
2012
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73. Lessons on Tumour Response : Imaging during Therapy with Lu-177-DOTA-octreotate. A Case Report on a Patient with a Large Volume of Poorly Differentiated Neuroendocrine Carcinoma

Author

Garske, Ulrike, Sandström, Mattias, Johansson, Silvia, Granberg, Dan, Lundqvist, Hans, Lubberink, Mark, Sundin, Anders, Eriksson, Barbro, Garske, Ulrike, Sandström, Mattias, Johansson, Silvia, Granberg, Dan, Lundqvist, Hans, Lubberink, Mark, Sundin, Anders, and Eriksson, Barbro

Abstract

Favourable outcomes of peptide receptor radiotherapy (PRRT) of neuroendocrine tumours have been reported during the last years. Still, there are uncertainties on the radionuclides to be used, the treatment planning, and the indication in patients with a high proliferation rate. This case report describes a patient with a high tumour burden of poorly differentiated neuroendocrine carcinoma of unknown primary with a proliferation rate in liver metastases up to 50%, undergoing fractionated treatment with 7 cycles of Lu-177-DOTA-octreotate (7.4 GBq each) after disease progression on two different chemotherapy regiments. Based on initial staging scintigraphy, somatostatin receptor expression was very high. Longitudinal dosimetry studies during therapy indicated ongoing increases in tumour-to-organ ratios that coincided with an objective response. We conclude that fractionated therapy with Lu-177-DOTA-octreotate should be considered a treatment option also for those patients with large tumours, high proliferation, and high receptor expression.

Published
2012
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74. A study of the location of the entrance of a fishway in a regulated river with CFD and ADCP

Author

Andersson, Anders G., Lindberg, Dan-Erik, Lindmark, Elianne, Leonardsson, Kjell, Andreasson, Patrik, Lundqvist, Hans, Lundström, T. Staffan, Andersson, Anders G., Lindberg, Dan-Erik, Lindmark, Elianne, Leonardsson, Kjell, Andreasson, Patrik, Lundqvist, Hans, and Lundström, T. Staffan

Abstract

Simulation-driven design with computational fluid dynamics has been used to evaluate the flow downstream of a hydropower plant with regards to upstream migrating fish. Field measurements with an Acoustic Doppler Current Profiler were performed, and the measurements were used to validate the simulations. The measurements indicate a more unstable flow than the simulations, and the tailrace jet from the turbines is stronger in the simulations. A fishway entrance was included in the simulations, and the subsequent attraction water was evaluated for two positions and two angles of the entrance at different turbine discharges. Results show that both positions are viable and that a position where the flow from the fishway does not have to compete with the flow from the power plant will generate superior attraction water. Simulations were also performed for further downstream where the flow from the turbines meets the old river bed which is the current fish passage for upstream migrating fish. A modification of the old river bed was made in the model as one scenario to generate better attraction water. This considerably increases the attraction water although it cannot compete with the flow from the tailrace tunnel., Validerad; 2012; Bibliografisk uppgift: Article ID 327929; 20120229 (stlu)

Published
2012
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75. Improved Tumor-to-Organ Ratios of a Novel 67Ga-Human Epidermal Growth Factor Radionuclide Conjugate with Preadministered Antiepidermal Growth Factor Receptor Affibody Molecules

Author

Sandström, Karl, Haylock, Anna-Karin, Velikyan, Irina, Spiegelberg, Diana, Kareem, Heewa, Tolmachev, Vladimir, Lundqvist, Hans, Nestor, Marika, Sandström, Karl, Haylock, Anna-Karin, Velikyan, Irina, Spiegelberg, Diana, Kareem, Heewa, Tolmachev, Vladimir, Lundqvist, Hans, and Nestor, Marika

Abstract

The over-expression of the epidermal growth factor receptor (EGFR) in head and neck squamous cell carcinoma (HNSCC) is associated with poor prognosis. Targeted nuclear imaging of the EGFR expression could improve the diagnostics in patients with HNSCC. However, the high expression of EGFR in normal organs may conceal the tumor uptake and therefore limit the use. In this study, we have assessed the biodistribution of a novel hEGF radionuclide conjugate after pre-injection with anti-EGFR Affibody molecules. hEGF was conjugated with p-SCN-Bn-NOTA and labeled with 67Ga. The biodistribution of [67Ga]Ga-NOTA-Bn-NCS-hEGF in nude mice with EGFR-expressing xenografts was evaluated either alone or 45 minutes after pre-injection with one of the anti-EGFR Affibody molecules ZEGFR:1907, (ZEGFR:1907)2 or (ZEGFR:955)2. The novel radioimmunoconjugate, [67Ga]Ga-NOTA-Bn-NCS-hEGF demonstrated high stability in vitro and specific binding to hEGF in vitro and in vivo. Pre-injection with anti-EGFR Affibody molecules improved the tumor-to-organ ratio in the liver, salivary glands and colon. Overall, the dimeric high affinity Affibody molecule (ZEGFR:1907)2 exhibited the best results. These findings show that pre-blocking with an anti-EGFR Affibody molecule is a promising tool that could improve the outcome of radionuclide-based imaging of EGFR-expressing tumors.

Published
2011
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76. Minor changes in effective half-life during fractionated 177Lu-Octreotate therapy

Author

Garske, Ulrike, Sandström, Mattias, Johansson, Silvia, Sundin, Anders, Granberg, Dan, Eriksson, Barbro, Lundqvist, Hans, Garske, Ulrike, Sandström, Mattias, Johansson, Silvia, Sundin, Anders, Granberg, Dan, Eriksson, Barbro, and Lundqvist, Hans

Abstract

Fractionated (177)Lu-DOTA-octreotate therapy has been reported to be an effective treatment option for patients with generalized neuroendocrine tumors. In our clinic, full individual dosimetry is performed during the first therapy cycle, while dosimetry at later cycles is based on the 24 h uptake measurement assuming an unchanged effective half-life. Our aim was to evaluate this assumption and the variation in the 24 h uptake during therapy. Patients. Thirty patients, 13 women and 17 men, were included in the study. Methods. During the first therapy cycle the (177)Lu-concentration was measured with SPECT/CT over the abdomen at 24 h, 96 h and 168 h after infusion. The effective half-life was determined for the kidneys, liver and spleen. The procedure was repeated at cycle 4 or 5. Results. The median ratio between the effective half-lives of the latter and the first cycle was 0.97 and 1.01 for the right and left kidney, with a range of 0.89-1.01 (1st-3rd quartile) and 0.93-1.05, respectively. Discussion. The mean value of the ratios was slightly lower than one, indicating a tendency towards increased activity elimination during therapy. In individual patients, significant changes were found for all organs, often when a large tumor burden reduction occurred during treatment. Possible contributing factors appeared to be larger amounts of non-tumor bound tracer, improved organ function (kidneys), decrease of vessel obstruction (spleen), less scatter from large tumors and reduction of small metastases (liver and spleen). Conclusion. With most patients it is safe to estimate absorbed doses to kidneys, liver and spleen from 24 h activity concentration assuming an unchanged effective half-life during therapy. Patients with risk factors for kidney dysfunction need to be monitored in more detail. Simplified dosimetry based on the assumption of unchanged effective half-life can function as guidance to the number of therapy cycles an individual patient can tolerate.

Published
2011
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77. Individualized dosimetry in patients undergoing therapy with Lu-177-DOTA-D-Phe(1)-Tyr(3)-octreotate

Author

Sandström, Mattias, Garske, Ulrike, Granberg, Dan, Sundin, Anders, Lundqvist, Hans, Sandström, Mattias, Garske, Ulrike, Granberg, Dan, Sundin, Anders, and Lundqvist, Hans

Abstract

In recent years, targeted radionuclide therapy with [Lu-177-DOTA(0), Tyr(3)]octreotate for neuroendocrine tumours has yielded promising results. This therapy may be further improved by using individualized dosimetry allowing optimization of the absorbed dose to the tumours and the normal organs. The aim of this study was to investigate the feasibility and reliability of individualized dosimetry based on SPECT in comparison to conventional planar imaging. Attenuation-corrected SPECT data were analysed both by using organ-based volumes of interest (VOIs) to obtain the total radioactivity in the organ, and by using small VOIs to measure the tissue radioactivity concentration. During the first treatment session in 24 patients, imaging was performed 1, 24, 96 and 168 h after [Lu-177-DOTA(0), Tyr(3)]octreotate infusion. Absorbed doses in non tumour-affected kidney, liver and spleen were calculated and compared for all three methods (planar imaging, SPECT organ VOIs, SPECT small VOIs). Planar and SPECT dosimetry were comparable in areas free of tumours, but due to overlap the planar dosimetry highly overestimated the absorbed dose in organs with tumours. Furthermore, SPECT dosimetry based on small VOIs proved to be more reliable than whole-organ dosimetry. We conclude that SPECT dosimetry based on small VOIs is feasible and more accurate than conventional planar dosimetry, and thus may contribute towards optimising targeted radionuclide therapy.

Published
2010
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79. The influence of Bz-DOTA and CHX-AaEuro(3)-DTPA on the biodistribution of ABD-fused anti-HER2 Affibody molecules : implications for In-114m-mediated targeting therapy

Author

Tolmachev, Vladimir, Wallberg, Helena, Andersson, Karl, Wennborg, Anders, Lundqvist, Hans, Orlova, Anna, Tolmachev, Vladimir, Wallberg, Helena, Andersson, Karl, Wennborg, Anders, Lundqvist, Hans, and Orlova, Anna

Abstract

Affibody molecules represent a novel class of high-affinity agents for radionuclide tumour targeting. Fusion of the Affibody molecules with an albumin-binding domain (ABD) enables modification of the blood kinetics of the Affibody molecules and reduction of the renal dose. Lu-177-CHX-AaEuro(3)-DTPA-ABD-(Z(HER2:342))(2), an anti-HER2 Affibody molecule-ABD fusion protein has earlier demonstrated promising results in treatment of HER2-expressing micro-xenografts in mice. The use of the in vivo generator In-114m/In-114 as a label for ABD-fused Affibody molecules would create preconditions for efficient treatment of both micrometastases (due to conversion and Auger electrons of In-114m) and bulky tumours (due to high-energy beta particles from the daughter nuclide In-114). The goal of this study was to investigate if different chelators influence the biodistribution of ABD-(Z(HER2:342))(2) and to find an optimal chelator for attachment of In-114m to the Affibody molecule-ABD fusion protein. Isothiocyanate derivatives of Bz-DOTA and CHX-AaEuro(3)-DTPA were coupled to ABD-(Z(HER2:342))(2). The cellular processing of both conjugates was studied in vitro. The influence of chelators on the biodistribution was investigated in mice using double isotope (In-114m and In-111) labelling. The apparent affinity of CHX-AaEuro(3)-DTPA-ABD-(Z(HER2:342))(2) and Bz-DOTA-ABD-(Z(HER2:342))(2) to the extracellular domain of HER2 was similar, 13.5 and 15.0 pM, respectively. It was found that both conjugates were internalized by SKOV-3 cells. The use of CHX-AaEuro(3)-DTPA provided better cellular retention of the radioactivity, better tumour accumulation of radioactivity and better tumour to organ dose ratios than Bz-DOTA-ABD-(Z(HER2:342))(2). CHX-AaEuro(3)-DTPA is more suitable for In-114m labelling of Affibody molecule-ABD fusion proteins for radionuclide therapy.

Published
2009
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81. Cross-fire doses from β-emitting radionuclides in targeted radiotherapy : A theoretical study based on experimentally measured tumor characteristics

Author

Enger, Shirin Abbasinejad, Hartman, Torbjörn, Carlsson, Jörgen, Lundqvist, Hans, Enger, Shirin Abbasinejad, Hartman, Torbjörn, Carlsson, Jörgen, and Lundqvist, Hans

Abstract

A mathematical model based upon histological findings of cell cluster distributions in primary breast cancers and lymph node metastases was developed. The model is unique because it accounts for tumor cell cluster formations within both primary tumors and metastases. The importance of inter-cell cluster cross-fire radiation dose for beta-emitting radionuclides of different energies was studied. The cell clusters were simulated as spheres with 15, 25 and 50 microm radii having a homogeneous radioactivity distribution. The self-dose as well as the dose distribution around the spheres was calculated for seven radionuclides, (90)Y, (188)Re, (32)P, (186)Re, (159)Gd, (131)I and (177)Lu using the GEANT4 Monte Carlo code. Generally, the self-dose was decreasing with increasing energy of the emitted beta particles. An exception was (188)Re which, compared to (32)P, had higher beta energy as well as higher self-dose. This was due to the higher emission of conversion and Auger electrons in the (188)Re-decay. When the cell clusters had a mean distance that was shorter than the maximum range of beta-particles, then the inter-cluster cross-fire radiation contributed significantly to the absorbed dose. Thus, high-energy beta-particles may, in spite of a low self-dose to single clusters, still be favorable to use due to the contribution of inter-cluster cross-fire radiation.

Published
2008
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82. Targeting CD44v6 expressed in head and neck squamous cell carcinoma : preclinical characterization of an 111In-labeled monoclonal antibody

Author

Sandström, Karl, Nestor, Marika, Ekberg, Tomas, Engström, Mats, Anniko, Matti, Lundqvist, Hans, Sandström, Karl, Nestor, Marika, Ekberg, Tomas, Engström, Mats, Anniko, Matti, and Lundqvist, Hans

Abstract

In patients with head and neck squamous cell carcinoma (HNSCC) radioimmunodiagnosis could offer a more specific and sensitive tumor diagnostic method.Our aim was to evaluate the labeling and biodistribution of the novel radioimmunoconjugate (111)In-cMAb U36. In this study cMAb U36, targeting CD44v6, and huA33, as a negative control, were labeled with indium-111, using the chelator CHXA''-DTPA. Immunoreactivity assays and binding studies were performed in vitro. Biodistribution and tumor imaging were conducted after intravenous injection of the radioimmunoconjugate to nude mice bearing HNSCC xenografts expressing CD44v6. The immunoreactive fraction was very high and the binding was CD44v6-specific. In vivo results demonstrated a promising biodistribution, with tumors clearly accumulating radioactivity with time. At 168 h postinjection (p.i.) the tumor uptake was 54.7 +/- 16.6% injected dose/g. The cMAb U36 had significantly (p < 0.05) higher uptake in tumors 72 h p.i. compared to huA33. We produced a novel radioimmunoconjugate targeting CD44v6 for possible use in the detection of HNSCC. The conjugate demonstrates no adverse effects from labeling and a favorable biodistribution.

Published
2008
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83. Real-time viability assay based on 51Cr retention in adherent cells

Author

Vennström, Lina, Bysell, Camilla, Björkelund, Hanna, Lundqvist, Hans, Andersson, Karl, Vennström, Lina, Bysell, Camilla, Björkelund, Hanna, Lundqvist, Hans, and Andersson, Karl

Abstract

The chromium (51Cr) release assay has been widely used for viability measurements, even though it has major disadvantages such as high manual workload and poor time resolution. By the use of LigandTracer 51Cr release viability measurements on adherent cells can be significantly simplified and improved. LigandTracer enables a time-resolved detection of 5SCr in target cells, with the result that the effect of toxic material is updated continuously throughout the experiment. Here we explain the principle behind this novel real-time viability assay and show viability curves for known toxic compounds on A431 and U343MGaCl2:6 cell lines.

Published
2008
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84. Characterization of In-111 and Lu-177-labeled antibodies binding to CD44v6 using a novel automated radioimmunoassay

Author

Nestor, Marika, Andersson, Karl, Lundqvist, Hans, Nestor, Marika, Andersson, Karl, and Lundqvist, Hans

Abstract

Targeted cancer therapies rely on bifunctional molecules, typically a protein that specifically recognizes tumor cells and a toxic component which is linked to the protein. Therefore, development of such therapies includes detailed characterizations of protein-cell interactions in order to find a good targeting agent. Knowledge of factors such as antibody-antigen specificity, as well as cellular uptake, retention and affinity of the antibody are necessary in order to be successful. In this paper, we have used a novel instrument, LigandTracer (R) Yellow, to characterize the interactions of In-111 and Lu-177-labeled monoclonal antibodies (MAbs) with CD44v6. Uptake studies with varying specific radioactivity of the chimeric MAb U36 and with an irrelevant antibody for the CD44v6 receptor verified the reliability of the method, as well as the specificity of the antibody-receptor binding. Uptake, retention, and affinity were very similar for the In-111 and Lu-177-labeled conjugate, and were in line with earlier studies using manual methods. The fact that no adverse effects from labeling were seen, together with the high retention, could make these conjugates promising candidates for imaging and therapy of certain cancer types in the future. The novel LigandTracer technology reduced the workload and reagent spending while providing data with superior time resolution. The obtained results were in agreement with previously reported findings. In addition the real-time detection and higher time resolution made more detailed studies of the interactions possible.

Published
2008
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86. Basin-scale phenology and effects of climate variability on global timing of initial seaward migration of Atlantic salmon (Salmo salar)

Author

Otero, Jaime, primary, L'Abée-Lund, Jan Henning, additional, Castro-Santos, Ted, additional, Leonardsson, Kjell, additional, Storvik, Geir O., additional, Jonsson, Bror, additional, Dempson, Brian, additional, Russell, Ian C., additional, Jensen, Arne J., additional, Baglinière, Jean-Luc, additional, Dionne, Mélanie, additional, Armstrong, John D., additional, Romakkaniemi, Atso, additional, Letcher, Benjamin H., additional, Kocik, John F., additional, Erkinaro, Jaakko, additional, Poole, Russell, additional, Rogan, Ger, additional, Lundqvist, Hans, additional, MacLean, Julian C., additional, Jokikokko, Erkki, additional, Arnekleiv, Jo Vegar, additional, Kennedy, Richard J., additional, Niemelä, Eero, additional, Caballero, Pablo, additional, Music, Paul A., additional, Antonsson, Thorolfur, additional, Gudjonsson, Sigurdur, additional, Veselov, Alexey E., additional, Lamberg, Anders, additional, Groom, Steve, additional, Taylor, Benjamin H., additional, Taberner, Malcolm, additional, Dillane, Mary, additional, Arnason, Fridthjofur, additional, Horton, Gregg, additional, Hvidsten, Nils A., additional, Jonsson, Ingi R., additional, Jonsson, Nina, additional, McKelvey, Simon, additional, Naesje, Tor F., additional, Skaala, Øystein, additional, Smith, Gordon W., additional, Saegrov, Harald, additional, Stenseth, Nils C., additional, and Vøllestad, Leif Asbjørn, additional

Published
2013
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89. [Lu-177]pertuzumab : Experimental therapy of HER-2-expressing xenografts

Author

Persson, Mikael, Gedda, Lars, Lundqvist, Hans, Tolmachev, Vladimir, Nordgren, Hans, Malmström, Per-Uno, Carlsson, Jörgen, Persson, Mikael, Gedda, Lars, Lundqvist, Hans, Tolmachev, Vladimir, Nordgren, Hans, Malmström, Per-Uno, and Carlsson, Jörgen

Abstract

Pertuzumab (Omnitarg) is a novel antibody against HER-2, domain II. HER-2 is a tyrosine kinase receptor that is overexpressed in several carcinomas, especially breast cancer. Pertuzumab, labeled with the low-energy beta emitter Lu-177, might be a candidate for targeted radiotherapy of disseminated HER-2-positive micrometastases. The radiolabeled antibody [Lu-177]pertuzumab showed favorable targeting properties in BALB/c (nu/nu) mice with HER-2-overexpressing xenografts. The absorbed dose in tumors was more than five times higher than the absorbed dose in blood and more than seven times the absorbed dose in any other normal organ. Experimental therapy showed that [Lu-177]pertuzumab delayed tumor progression compared with controls (no treatment, P < 0.0001; nonlabeled pertuzumab antibody, P < 0.0001; and Lu-177-labeled irrelevant antibody, P < 0.01). No adverse side effects of the treatment could be detected. Thus, the experimental results support the planning of clinical studies applying [Lu-177]pertuzumab for therapy.

Published
2007
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90. Genotoxic hazard of radiopharmaceuticals in humans : chemical and radiation aspects coupled to microdosing

Author

Lundqvist, Hans, Antoni, Gunnar, Långström, Bengt, Lundqvist, Hans, Antoni, Gunnar, and Långström, Bengt

Abstract

Introduction To obtain the pharmacokinetic properties of drug candidates at an early stage of the development process, a microdosing (phase 0) concept to radiolabel drug candidates and administer them at subtoxic mass to a few volunteers has been suggested. Radiopharmaceuticals are special in the sense that the chemical carrier might be genotoxic, whereas it is well established that ionizing radiation coupled to the molecule is genotoxic, and that the mechanism that causes cancer is similar to certain genotoxic chemicals. Regulatory perspectives of the levels of toxicity An analysis shows that, e.g., positron emission tomography (PET) pharmaceuticals carry a mass less than what is regarded as an acceptable level of a genotoxic impurity. It has also been shown that the estimated genotoxicity hazard of the radioactivity is 10–100 times higher than that of the administered chemicals. Conclusion As radiation doses at this level are accepted in clinical trials, the conclusion is that the regulatory demands on radiopharmaceuticals produced at high specific radioactivity should be reconsidered in order to facilitate the use of the microdosing concept for drug development.

Published
2007
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91. Radionuclide therapy of HER2-positive microxenografts using a 177Lu-labeled HER2-specific Affibody molecule

Author

Tolmachev, Vladimir, Orlova, Anna, Pehrson, Rikard, Galli, Joakim, Baastrup, Barbro, Andersson, Karl, Sandström, Mattias, Rosik, Daniel, Carlsson, Jörgen, Lundqvist, Hans, Wennborg, Anders, Nilsson, Fredrik Y., Tolmachev, Vladimir, Orlova, Anna, Pehrson, Rikard, Galli, Joakim, Baastrup, Barbro, Andersson, Karl, Sandström, Mattias, Rosik, Daniel, Carlsson, Jörgen, Lundqvist, Hans, Wennborg, Anders, and Nilsson, Fredrik Y.

Abstract

A radiolabeled anti-HER2 Affibody molecule (Z(HER2:342)) targets HER2-expressing xenografts with high selectivity and gives good imaging contrast. However, the small size (approximately 7 kDa) results in rapid glomerular filtration and high renal accumulation of radiometals, thus excluding targeted therapy. Here, we report that reversible binding to albumin efficiently reduces the renal excretion and uptake, enabling radiometal-based nuclide therapy. The dimeric Affibody molecule (Z(HER2:342))(2) was fused with an albumin-binding domain (ABD) conjugated with the isothiocyanate derivative of CHX-A''-DTPA and labeled with the low-energy beta-emitter (177)Lu. The obtained conjugate [CHX-A''-DTPA-ABD-(Z(HER2:342))(2)] had a dissociation constant of 18 pmol/L to HER2 and 8.2 and 31 nmol/L for human and murine albumin, respectively. The radiolabeled conjugate displayed specific binding to HER2-expressing cells and good cellular retention in vitro. In vivo, fusion with ABD enabled a 25-fold reduction of renal uptake in comparison with the nonfused dimer molecule (Z(HER2:342))(2). Furthermore, the biodistribution showed high and specific uptake of the conjugate in HER2-expressing tumors. Treatment of SKOV-3 microxenografts (high HER2 expression) with 17 or 22 MBq (177)Lu-CHX-A''-DTPA-ABD-(Z(HER2:342))(2) completely prevented formation of tumors, in contrast to mice given PBS or 22 MBq of a radiolabeled non-HER2-binding Affibody molecule. In LS174T xenografts (low HER2 expression), this treatment resulted in a small but significant increase of the survival time. Thus, fusion with ABD improved the in vivo biodistribution, and the results highlight (177)Lu-CHX-A''-DTPA-ABD-(Z(HER2:342))(2) as a candidate for treatment of disseminated tumors with a high level of HER2 expression.

Published
2007
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92. Biodistribution of 211At labeled HER-2 binding affibody molecules in mice

Author

Steffen, Ann-Charlott, Almqvist, Ylva, Chyan, Ming-Kuan, Lundqvist, Hans, Tolmachev, Vladimir, Wilbur, D. Scott, Carlsson, Jörgen, Steffen, Ann-Charlott, Almqvist, Ylva, Chyan, Ming-Kuan, Lundqvist, Hans, Tolmachev, Vladimir, Wilbur, D. Scott, and Carlsson, Jörgen

Abstract

The size of affibody molecules makes them suitable as targeting agents for targeted radiotherapy with the alpha-emitter 211At, since their biokinetic properties match the short physical half-live of 211At. In this study, the potential for this approach was investigated in vivo. Two different HER-2 binding affibody molecules were radiolabeled with 211At using both the linker PAB (N-succinimidyl-para-astatobenzoate) and a decaborate-based linker, and the biodistribution in tumor-bearing nude mice was investigated. The influence of L-lysine and Na-thiocyanate on the 211At uptake in normal tissues was also studied. Based on the biokinetic information obtained, the absorbed dose was calculated for different organs. Compared with a previous biodistribution with 125I, the 211At biodistribution using the PAB linker showed higher uptake in lungs, stomach, thyroid and salivary glands, indicating release of free 211At. When the decaborate-based linker was used, the uptake in those organs was decreased, but instead, high uptake in kidneys and liver was found. The uptake, when using the PAB linker, could be significantly reduced in some organs by the use of L-lysine and/or Na-thiocyanate. In conclusion, affibody molecules have suitable blood-kinetics for targeted radionuclide therapy with 211At. However, the labeling chemistry affects the distribution in normal organs to a high degree and needs to be improved to allow clinical use.

Published
2007

93. Food interaction of oral uptake of iron : a clinical trial using 59Fe

Author

Lundqvist, Hans, Sjöberg, Folke, Lundqvist, Hans, and Sjöberg, Folke

Abstract

OBJECTIVES: A primary objective of the study was to evaluate how food as well as a specific enhancer or an inhibitor of iron uptake affect erythrocyte iron uptake after oral administration of iron(III)-hydroxide polymaltose complex (IPC, Maltofer) in subjects with or without iron deficiency. Secondary objectives of the study were 1. to compare the uptake of 59Fe in erythrocytes between subjects with or without iron deficiency, 2. to evaluate the 59Fe activity in plasma after oral administration of IPC and 3. to evaluate the safety of oral administration of IPC by adverse events (AEs), vital signs, and hematological and clinical chemistry parameters. DESIGN: Single-centre study with a crossover design. Each subject participated in two periods where single doses of 100 mg iron as IPC labeled with 59Fe were administered. In one period the subjects were fasting and in the other they were fed (Group A and Group B). Alternatively the study medication was administered in the fed state with an iron absorption enhancer (orange juice) or an iron absorption inhibitor (black tea, Group C and Group D). Eight subjects were included in each group, i.e. 32 subjects were included in total. All subjects completed the study and were included in the analyses of data. RESULTS: In terms of relative incorporation of iron in erythrocytes, both subjects with and without iron deficiency benefited from the concomitant administration of an enhancer with the IPC. In iron deficiency subjects the iron uptake was improved when administered with food whereas for the normal subjects the uptake was greater during fasting conditions. The uptake of 59Fe in erythrocytes was greater in subjects with iron deficiency compared to the normal subjects, except when IPC was administered during fasting conditions. The safety assessments performed in this study did not demonstrate any unexpected observations or safety concerns with IPC. CONCLUSION: In both subjects with and without iron deficiency treated with IP

Published
2007

94. Biodistribution of At-211-Labeled humanized monoclonal antibody A33

Author

Almqvist, Ylva, Steffen, Ann-Charlott, Lundqvist, Hans, Jensen, Holger, Tolmachev, Vladimir, Sundin, Anders, Almqvist, Ylva, Steffen, Ann-Charlott, Lundqvist, Hans, Jensen, Holger, Tolmachev, Vladimir, and Sundin, Anders

Abstract

Radioimmunotherapy (RIT) could be a possible adjuvant treatment method for patients with colorectal carcinoma. The A33 antigen is a promising RIT target, as it is highly and homogenously expressed in 95% of all colorectal carcinomas. In this study, the humanized monoclonal antibody A33 (huA33), targeting the A33 antigen, was labeled with the therapeutic nuclide 211At, and the biodistribution and in vivo targeting ability of the conjugate was investigated in an athymic mouse xenograft model. There was an accumulation of 211At in tumor tissue over time, but no substantial accumulation was seen in any organ apart from the skin and thyroid, indicating no major release of free 211At in vivo. At all time points, the uptake of 211At-huA33 was higher in tumor tissue than in most organs, and at 8 hours postinjection (p.i.), no organ had a higher uptake than tumor tissue. The tumor-to-blood ratio of 211At-huA33 increased with time, reaching 2.5 after 21 hours p.i. The highest absorbed dose was found in the blood, but the tumor received a higher dose than any organ other than the thyroid. An in vivo blocking experiment showed that 211At-huA33 binds specifically to human tumor xenografts in athymic mice. In conclusion, the favorable biodistribution and specific in vivo targeting ability of 211At-huA33 makes it a potential therapeutic agent for the RIT of metastatic colorectal carcinoma.

Published
2007
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95. Evaluation of [(111/114m)In]CHX-A'-DTPA-ZHER2:342, an affibody ligand coniugate for targeting of HER2-expressing malignant tumors

Author

Orlova, Anna, Rosik, Daniel, Sandström, Mattias, Lundqvist, Hans, Einarsson, L., Tolmachev, Vladimir, Orlova, Anna, Rosik, Daniel, Sandström, Mattias, Lundqvist, Hans, Einarsson, L., and Tolmachev, Vladimir

Abstract

AIM: Radionuclide imaging of the HER2 receptor, which is a target for trastuzumab therapy, can provide important diagnostic information. Further, targeting radionuclide therapy might be an option for treatment of HER2 expressing tumors. The phage-display selected Affibody ligand Z(HER2:342), which binds to HER2 with an affinity of 22 pM, may here play an important role. The small size of the Z(HER2:342), 7.5 kDa, enables quick tumor localization and fast blood clearance. Earlier, successful targeting of HER2-expressing xenografts using Z(HER2:342) labeled using [(111)In]benzyl-DTPA was reported. By changing to the CHX-A''-DTPA chelator, the stability and labeling kinetics of the radiometal-Z(HER2:342) conjugate can be improved. The aim of this study was to evaluate the labeling of the CHX-A''-DTPA-Z(HER2:342) conjugate with (111)In for diagnostic imaging and with (114m)In for locoregional radionuclide therapy. METHODS: The isothiocyanate derivative of CHX-A''-DTPA was coupled to Z(HER2:342) in alkaline conditions at 37 degrees C. The conjugate was labeled with both (111)In and (114m)In and evaluated in vitro and in vivo. RESULTS: Labeling with (111)In and (114m)In provided >95% yield after 30 min at RT. Specific radioactivity was 0.5 and 12 MBq/nmol, for (114m)In and (111)In, respectively. The radiolabeled conjugates demonstrated specific binding to HER2 expressing SKOV-3 cells. In mice bearing SKOV-3 xenografts, the tumor uptake of [(111)In]CHX-A''-DTPA-Z(HER2:342) 4 h postinjection was 10.3+/-3.6% IA/g and tumor-to-blood ratio about 190. CONCLUSION: [(111)In]CHX-A''-DTPA-Z(HER2:342) is a promising candidate for the visualization of HER2 expression in malignant tumors. Labeled with (114m)In it could also be used for locoregional treatment of HER2 expressing tumors.

Published
2007

96. Astatinated trastuzumab, a putative agent for radionuclide immunotherapy of ErbB2-expressing tumours

Author

Persson, Mikael I., Gedda, Lars, Jensen, H. J., Lundqvist, Hans, Malmström, Per-Uno, Tolmachev, Vladimir, Persson, Mikael I., Gedda, Lars, Jensen, H. J., Lundqvist, Hans, Malmström, Per-Uno, and Tolmachev, Vladimir

Abstract

The anti-ErbB2 antibody trastuzumab is used for the treatment of patients with advanced breast cancer, resulting in a response rate of 40-60%. Coupling with a cytotoxic nuclide, e.g. alpha-emitting 211At, may further increase tumour response. The tumour-targeting properties of trastuzumab, astatinated using N-succinimidyl-para-(tri-n-methylstannyl)-benzoate, were evaluated and compared with those of radioiodinated trastuzumab in this study. We found that astatinated trastuzumab retains high specificity towards ErbB2. While the immunoreactive fraction of radioiodinated trastuzumab was higher than that of astatinated trastuzumab (76+/-9% versus 54+/-28%), both radioconjugates showed high affinity (KD 0.75+/-0.16 nM versus 1.8+/-0.3 nM). A growth inhibition study indicated a dose-dependent cell deactivation, in which approximately 74 cell-associated astatine decays per cell gave a survival fraction of 4.5+/-0.8x10(-4). Results of a comparative animal study on normal mice gave no indication that astatination would have any adverse effects on the biodistribution of the antibody. In conclusion, the results of the study suggest that astatinated trastuzumab is a promising candidate for treating ErbB2-expressing tumours.

Published
2006

97. Planning for intracavitary anti-EGFR radionuclide therapy of gliomas : Literature review and data on EGFR expression

Author

Carlsson, Jörgen, Ren, Z. P., Wester, K., Sundberg, A. L., Heldin, Nils-Erik, Hesselager, G., Persson, M., Gedda, Lars, Tolmachev, Vladimir, Lundqvist, Hans, Blomquist, Erik, Nistér, M., Carlsson, Jörgen, Ren, Z. P., Wester, K., Sundberg, A. L., Heldin, Nils-Erik, Hesselager, G., Persson, M., Gedda, Lars, Tolmachev, Vladimir, Lundqvist, Hans, Blomquist, Erik, and Nistér, M.

Abstract

Targeting with radionuclide labelled substances that bind specifically to the epidermal growth factor receptor, EGFR, is considered for intracavitary therapy of EGFR-positive glioblastoma multiforme, GBM. Relevant literature is reviewed and examples of EGFR expression in GBM are given. The therapeutical efforts made so far using intracavitary anti-tenascin radionuclide therapy of GBM have given limited effects, probably due to low radiation doses to the migrating glioma cells in the brain. Low radiation doses might be due to limited penetration of the targeting agents or heterogeneity in the expression of the target structure. In this article we focus on the possibilities to target EGFR on the tumour cells instead of an extracellular matrix component. There seems to be a lack of knowledge on the degree of intratumoral variation of EGFR expression in GBM, although the expression seemed rather homogeneous over large areas in most of the examples (n=16) presented from our laboratory. The observed homogeneity was surprising considering the genomic instability and heterogeneity that generally characterises highly malignant tumours. However, overexpression of EGFR is, at least in primary GBMs, one of the steps in the development of malignancy, and tumour cells that lose or downregulate EGFR will probably be outgrown in an expanding tumour cell population. Thus, loss of EGFR expression might not be the critical factor for successful intracavitary radionuclide therapy. Instead, it is likely that the penetration properties of the targeting agents are critical, and detailed studies on this are urgent.

Published
2006
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98. Radio-iodination of monoclonal antibody using potassium [125I]-(4-isothiocyanatobenzylammonio)-iodo-decahydro-closo-dodecaborate (iodo-DABI)

Author

Orlova, Anna, Bruskin, Alexander, Sivaev, Igor, Sjöberg, Stefan, Lundqvist, Hans, Tolmachev, Vladimir, Orlova, Anna, Bruskin, Alexander, Sivaev, Igor, Sjöberg, Stefan, Lundqvist, Hans, and Tolmachev, Vladimir

Abstract

BACKGROUND: Negatively-charged polyhedral boron clusters can be easily halogenated with highly stable boron-halogen bonds and are promising in radionuclide diagnostics and cancer therapy. MATERIALS AND METHODS: The radio-iodination conditions for the closo-dodecaborate anion and for the conjugation of its labeled isothiocyanatobenzylammonio derivative to the monoclonal antibody (mAb) were optimized. RESULTS: The labeling yield was about 90% and the overall conjugation yield was 55-60%. The in vitro stability of the radio-iodinated mAb was good under physiological and non-physiological conditions. The immunoreactivity of the labeled mAb (SK-BR-3 cells) was retained in the one-pot two-step labeling. CONCLUSION: Negatively-charged polyhedral boron clusters can be used for indirect radio-iodination of mAbs.

Published
2006

99. Cellular processing in the SW1222 cell line of mAb A33 directly and indirectly radiohalogenated

Author

Höglund, Johanna, Orlova, Anna, Sundin, Anders, Lundqvist, Hans, Tolmachev, Vladimir, Höglund, Johanna, Orlova, Anna, Sundin, Anders, Lundqvist, Hans, and Tolmachev, Vladimir

Abstract

Investigations into the cellular processing of radiolabeled monoclonal antibodies (mAbs) for their further use in radioimmunodiagnosis and cancer therapy are needed in order to understand the fate of internalized and catabolized mAbs. The anti-colorectal cancer mAb, A33, was labelled with 76Br and 125I using the direct Chloramine-T method, or by labelling N-succinimidyl para-(tri-methylstannyl) benzoate and its further conjugation to the mAb. The cellular processing of the four conjugates was investigated in SW1222 cells in vitro. Uptake of mAb was rapid, peaking after 14-16 h. Intracellular degradation was slow and the early loss of radioactivity was due to dissociation of cell-surface bound mAb. The indirect labelling resulted in stronger binding of the mAb as well as prolonged intracellular retention of the radiolabel. Direct and indirect halogen radiolabelling results in different cell-processing patterns of radiolabels, and radioactive catabolic products follow different routes of cellular excretion. The results of this cellular study indicate that indirect labelling is preferable to the direct Chloramine-T method.

Published
2006

100. Gadolinium neutron capture brachytherapy (GdNCB), a new treatment method for intravascular brachytherapy

Author

Enger, Shirin A., Rezaei, Arash, Munck af Rosenschöld, Per, Lundqvist, Hans, Enger, Shirin A., Rezaei, Arash, Munck af Rosenschöld, Per, and Lundqvist, Hans

Abstract

Restenosis is a major problem after balloon angioplasty and stent implantation. The aim of this study is to introduce gadolinium neutron capture brachytherapy (GdNCB) as a suitable modality for treatment of stenosis. The utility of GdNCB in intravascular brachytherapy (IVBT) of stent stenosis is investigated by using the GEANT4 and MCNP4B Monte Carlo radiation transport codes. To study capture rate, Kerma, absorbed dose and absorbed dose rate around a Gd-containing stent activated with neutrons, a 30 mm long, 5 mm diameter gadolinium foil is chosen. The input data is a neutron spectrum used for clinical neutron capture therapy in Studsvik, Sweden. Thermal neutron capture in gadolinium yields a spectrum of high-energy gamma photons, which due to the build-up effect gives an almost flat dose delivery pattern to the first 4 mm around the stent. The absorbed dose rate is 1.33 Gy/min, 0.25 mm from the stent surface while the dose to normal tissue is in order of 0.22 Gy/min, i.e., a factor of 6 lower. To spare normal tissue further fractionation of the dose is also possible. The capture rate is relatively high at both ends of the foil. The dose distribution from gamma and charge particle radiation at the edges and inside the stent contributes to a nonuniform dose distribution. This will lead to higher doses to the surrounding tissue and may prevent stent edge and in-stent restenosis. The position of the stent can be verified and corrected by the treatment plan prior to activation. Activation of the stent by an external neutron field can be performed days after catherization when the target cells start to proliferate and can be expected to be more radiation sensitive. Another advantage of the nonradioactive gadolinium stent is the possibility to avoid radiation hazard to personnel.

Published
2006
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