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  1. Article ; Online: Novel mouse strains to study circulating permeability factor(s) in primary focal segmental glomerulosclerosis.

    den Braanker, Dirk / Maas, Rutger / Parr, Naomi / Deegens, Jeroen / Smeets, Bart / Wetzels, Jack / van der Vlag, Johan / Nijenhuis, Tom

    PloS one

    2022  Volume 17, Issue 9, Page(s) e0274959

    Abstract: Recurrence of proteinuria after kidney transplantation in primary focal segmental glomerulosclerosis (FSGS) is unpredictable. Several putative circulating permeability factors (CPFs) have been suggested, but none have been validated. A clinically ... ...

    Abstract Recurrence of proteinuria after kidney transplantation in primary focal segmental glomerulosclerosis (FSGS) is unpredictable. Several putative circulating permeability factors (CPFs) have been suggested, but none have been validated. A clinically relevant experimental model is required that demonstrates the presence of CPF(s) in patient material, to study CPF(s) and possibly predict recurrence in patients. We aimed to develop a FSGS-prone Thy-1.1 transgenic mouse model with accelerated proteinuria after injection of samples from patients with FSGS. The Thy-1.1 transgene was backcrossed into 5 mouse strains. The age of onset and severity of spontaneous proteinuria varied between the different genetic backgrounds. 129X1/SvThy-1.1 and 129S2/SvPasThy-1.1 mice displayed proteinuria at 4 weeks, whereas Balb/cThy-1.1 and C57BL/6JThy-1.1 mice developed proteinuria from 6 weeks, and were used further. We determined the maximum protein dose that could be injected without causing protein overload in each background. Balb/cThy-1.1 and C57BL/6JThy-1.1 males and females were injected with presumably CPF-containing plasmapheresis effluent from 6 FSGS patients, which induced albuminuria particularly in Balb/cThy-1.1 males. Unfortunately, no response could be detected when using sera instead of plasmapheresis effluent, serum being more clinically relevant in the context of predicting FSGS recurrence. Considering the differences between responses elicited by serum and plasmapheresis effluent, simultaneously collected serum, plasma, and plasmapheresis effluent were tested. Whereas we could detect responses using a validated in vitro model, none of these presumably CPF-containing samples induced proteinuria in Balb/cThy-1.1 males. Thus, we have extensively tested the Thy-1.1 mouse model on different genetic backgrounds with proteinuria after injection of FSGS patient material as clinically relevant readout. The Balb/cThy-1.1 male mouse strain demonstrated the most promising results, but to detect CPF activity in FSGS serum e.g. prior to kidney transplantation, this strain clearly lacks sensitivity and is therefore not yet clinically applicable. It could, however, still be used as research tool to study CPFs in patient samples that did induce proteinuria.
    MeSH term(s) Animals ; Female ; Glomerulosclerosis, Focal Segmental/genetics ; Male ; Mice ; Mice, Inbred C57BL ; Permeability ; Plasmapheresis ; Proteinuria/etiology ; Recurrence
    Language English
    Publishing date 2022-09-22
    Publishing country United States
    Document type Journal Article ; Research Support, Non-U.S. Gov't
    ZDB-ID 2267670-3
    ISSN 1932-6203 ; 1932-6203
    ISSN (online) 1932-6203
    ISSN 1932-6203
    DOI 10.1371/journal.pone.0274959
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  2. Article: Glycosaminoglycans and fucoidan have a protective effect on experimental glomerulonephritis.

    Buijsers, Baranca / Maciej-Hulme, Marissa / Jacobs, Maaike / Bebber, Marinka Bakker-van / de Graaf, Mark / Salmenov, Rustem / Parr, Naomi / Rabelink, Ton J / Nijenhuis, Tom / van der Vlag, Johan

    Frontiers in molecular biosciences

    2023  Volume 10, Page(s) 1223972

    Abstract: Background: ...

    Abstract Background:
    Language English
    Publishing date 2023-07-05
    Publishing country Switzerland
    Document type Journal Article
    ZDB-ID 2814330-9
    ISSN 2296-889X
    ISSN 2296-889X
    DOI 10.3389/fmolb.2023.1223972
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  3. Article ; Online: Peer emotion socialization and somatic complaints in adolescents.

    Parr, Naomi J / Zeman, Janice / Braunstein, Kara / Price, Natalee

    Journal of adolescence

    2016  Volume 50, Page(s) 22–30

    Abstract: Somatic symptoms tend to increase during early adolescence and although youth's social environments and emotional functioning play a role in somatic symptoms, few studies have examined mechanisms through which social interaction could influence youth's ... ...

    Abstract Somatic symptoms tend to increase during early adolescence and although youth's social environments and emotional functioning play a role in somatic symptoms, few studies have examined mechanisms through which social interaction could influence youth's somatic wellbeing. Participants were 132 youth (61.6% girls, Mage = 12.61 years, 84.7% Caucasian) and their mothers. Reciprocated best-friend dyads participated in a video-taped problem discussion task to assess peer emotion socialization responses. Two supportive friend responses (i.e., emotion-focused, problem-focused) and two unsupportive responses (i.e., punitive, neglect) were examined. Mothers reported on their child's somatic complaints. Friends who provided emotion-focused, problem-focused, punitive, and neglect responses to their close friend's emotional disclosures had significantly fewer somatic symptoms. However, youth who received punitive responses to their emotional disclosures from their close friends had more somatic complaints. These findings provide initial evidence of a link between emotion socialization responses within close friendships and somatic complaints in early adolescence.
    MeSH term(s) Adolescent ; Age Factors ; Child ; Emotions ; Female ; Friends/psychology ; Humans ; Male ; Models, Psychological ; Mothers/psychology ; Peer Group ; Social Environment ; Socialization ; Somatoform Disorders/psychology ; Surveys and Questionnaires
    Language English
    Publishing date 2016
    Publishing country England
    Document type Journal Article ; Research Support, Non-U.S. Gov't
    ZDB-ID 303529-3
    ISSN 1095-9254 ; 0140-1971
    ISSN (online) 1095-9254
    ISSN 0140-1971
    DOI 10.1016/j.adolescence.2016.04.004
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  4. Article ; Online: Working memory and visual discrimination distraction tasks improve cold pressor pain tolerance in children.

    Dahlquist, Lynnda M / Gaultney, Wendy M / Bento, Samantha P / Steiner, Emily M / Zeroth, Julia A / Parr, Naomi J / Quiton, Raimi L

    Health psychology : official journal of the Division of Health Psychology, American Psychological Association

    2019  Volume 39, Issue 1, Page(s) 10–20

    Abstract: Objective: Distraction is a well-established pain management technique for children experiencing acute pain, although the mechanisms underlying the effectiveness of distraction are not well understood. It has been postulated that engagement of executive ...

    Abstract Objective: Distraction is a well-established pain management technique for children experiencing acute pain, although the mechanisms underlying the effectiveness of distraction are not well understood. It has been postulated that engagement of executive functions, such as working memory, may be a critical factor in attenuating pain via distraction. To test this hypothesis, we compared a 1-back task requiring engagement of working memory with a simple visual discrimination task demanding focused attention, but lower cognitive load (0-back).
    Method: Seventy-nine children (6-12 years old) underwent a baseline cold pressor trial followed by cold pressor trials in which they completed the visual discrimination and 1-back tasks in counterbalanced order. Executive functioning ability was assessed via the Wechsler Intelligence Scale for Children (5th Edition) working memory subscales and by parent report on the Behavior Rating Inventory of Executive Function, Second Edition (BRIEF®2).
    Results: Children's pain tolerance improved in both the visual discrimination and 1-back conditions though a differential response to the 2 tasks was not observed. Age moderated the relation between executive functioning and response to distraction; older children with better executive functioning skills demonstrated greater improvements in both distraction interventions.
    Conclusions: Findings demonstrate the benefits of both visual discrimination and working memory distraction tasks for elementary-aged children experiencing acute pain. Further research is required in order to elucidate the role of executive functioning skills and cognitive load in enhancing distraction analgesia in children, with particular focus on determining optimal load and task difficulty in light of emerging executive functioning abilities in this age group. (PsycINFO Database Record (c) 2019 APA, all rights reserved).
    MeSH term(s) Child ; Discrimination, Psychological/physiology ; Female ; Humans ; Male ; Memory, Short-Term/physiology ; Pain/psychology ; Pain Threshold/psychology
    Language English
    Publishing date 2019-08-05
    Publishing country United States
    Document type Journal Article
    ZDB-ID 226369-5
    ISSN 1930-7810 ; 0278-6133
    ISSN (online) 1930-7810
    ISSN 0278-6133
    DOI 10.1037/hea0000789
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  5. Article ; Online: A mutation in the kringle domain of human factor XII that causes autoinflammation, disturbs zymogen quiescence, and accelerates activation.

    Hofman, Zonne L M / Clark, Chantal C / Sanrattana, Wariya / Nosairi, Aziz / Parr, Naomi M J / Živkovic, Minka / Krause, Karoline / Mahnke, Niklas A / Scheffel, Jörg / Hack, C Erik / Maurer, Marcus / de Maat, Steven / Maas, Coen

    The Journal of biological chemistry

    2019  Volume 295, Issue 2, Page(s) 363–374

    Abstract: Coagulation factor XII (FXII) drives production of the inflammatory peptide bradykinin. Pathological mutations in ... ...

    Abstract Coagulation factor XII (FXII) drives production of the inflammatory peptide bradykinin. Pathological mutations in the
    MeSH term(s) Amino Acid Substitution ; Catalytic Domain ; Enzyme Activation ; Factor XII/chemistry ; Factor XII/genetics ; Factor XII/metabolism ; HEK293 Cells ; Humans ; Kringles ; Point Mutation
    Chemical Substances Factor XII (9001-30-3)
    Language English
    Publishing date 2019-11-26
    Publishing country United States
    Document type Journal Article ; Research Support, Non-U.S. Gov't
    ZDB-ID 2997-x
    ISSN 1083-351X ; 0021-9258
    ISSN (online) 1083-351X
    ISSN 0021-9258
    DOI 10.1074/jbc.RA119.009788
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  6. Article ; Online: Design and characterization of α1-antitrypsin variants for treatment of contact system-driven thromboinflammation.

    de Maat, Steven / Sanrattana, Wariya / Mailer, Reiner K / Parr, Naomi M J / Hessing, Martin / Koetsier, Robert M / Meijers, Joost C M / Pasterkamp, Gerard / Renné, Thomas / Maas, Coen

    Blood

    2019  Volume 134, Issue 19, Page(s) 1658–1669

    Abstract: The contact system produces the inflammatory peptide bradykinin and contributes to experimental thrombosis. C1 esterase-inhibitor (C1INH) deficiency or gain-of-function mutations in factor XII (FXII) cause hereditary angioedema, a life-threatening tissue ...

    Abstract The contact system produces the inflammatory peptide bradykinin and contributes to experimental thrombosis. C1 esterase-inhibitor (C1INH) deficiency or gain-of-function mutations in factor XII (FXII) cause hereditary angioedema, a life-threatening tissue swelling disease. C1INH is a relatively weak contact system enzyme inhibitor. Although α1-antitrypsin (α1AT) does not naturally inhibit contact system enzymes, a human mutation (M358R; α1AT-Pittsburgh) changes it into a powerful broad-spectrum enzyme inhibitor. It blocks the contact system, but also thrombin and activated protein C (APC), making it an unattractive candidate for therapeutic contact system blockade. We adapted the reactive center loop of α1AT-Pittsburgh (AIPR/S) to overcome these obstacles. Two α1AT variants (SMTR/S and SLLR/S) strongly inhibit plasma kallikrein, activated FXII, and plasmin. α1AT-SMTR/S no longer inhibits thrombin, but residually inhibits APC. In contrast, α1AT-SLLR/S residually inhibits thrombin, but no longer APC. Additional modification at the P1' position (S→V) eliminates residual inhibition of thrombin and APC for both variants, while retaining their properties as contact system inhibitors. Both α1AT-SMTR/V and -SLLR/V are superior to C1INH in reducing bradykinin production in plasma. Owing to their capacity to selectively block contact system-driven coagulation, both variants block vascular occlusion in an in vivo model for arterial thrombosis. Furthermore, both variants block acute carrageenan-induced tissue edema in mice. Finally, α1AT-SLLR/V, our most powerful candidate, suppresses epithelial leakage of the gut in a mouse model of colitis. Our findings confirm that redesign of α1AT strongly alters its inhibitory behavior and can be used for the treatment of contact system-mediated thrombosis and inflammation.
    MeSH term(s) Angioedemas, Hereditary ; Animals ; Blood Coagulation/drug effects ; Blood Coagulation/physiology ; Humans ; Inflammation ; Mice ; Mice, Inbred BALB C ; Thrombosis ; alpha 1-Antitrypsin/pharmacology
    Chemical Substances alpha 1-Antitrypsin ; alpha 1-antitrypsin Pittsburgh
    Language English
    Publishing date 2019-07-29
    Publishing country United States
    Document type Journal Article ; Research Support, Non-U.S. Gov't
    ZDB-ID 80069-7
    ISSN 1528-0020 ; 0006-4971
    ISSN (online) 1528-0020
    ISSN 0006-4971
    DOI 10.1182/blood.2019000481
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  7. Article ; Online: Platelet function is disturbed by the angiogenesis inhibitors sunitinib and sorafenib, but unaffected by bevacizumab.

    Walraven, Maudy / Homs, Marjolein Y V / van der Veldt, Astrid A M / Dekker, Henk / Koldenhof, Jose / Honeywell, Richard / Barendrecht, Arjan / Sebastian, Silvie A E / Parr, Naomi / Koekman, Arnold C / Voest, Emile E / Roest, Mark / Korporaal, Suzanne J A / Verheul, Henk M W

    Angiogenesis

    2018  Volume 21, Issue 2, Page(s) 325–334

    Abstract: Introduction: At the clinical introduction of antiangiogenic agents as anticancer agents, no major toxicities were expected as merely just endothelial cells (ECs) in tumors would be affected. However, several (serious) toxicities became apparent, of ... ...

    Abstract Introduction: At the clinical introduction of antiangiogenic agents as anticancer agents, no major toxicities were expected as merely just endothelial cells (ECs) in tumors would be affected. However, several (serious) toxicities became apparent, of which underlying mechanisms are largely unknown. We investigated to what extent sunitinib (multitargeted antiangiogenic tyrosine kinase inhibitor (TKI)), sorafenib (TKI) and bevacizumab [specific antibody against vascular endothelial growth factor (VEGF)] may impair platelet function, which might explain treatment-related bleedings.
    Materials and methods: In vitro, the influence of sunitinib, sorafenib, and bevacizumab on platelet aggregation, P-selectin expression and fibrinogen binding, platelet-EC interaction, and tyrosine phosphorylation of c-Src was studied by optical aggregation, flow cytometry, real-time perfusion, and western blotting. Ex vivo, platelet aggregation was analyzed in 25 patients upon sunitinib or bevacizumab treatment. Concentrations of sunitinib, VEGF, and platelet and EC activation markers were measured by LC-MS/MS and ELISA.
    Results: In vitro, sunitinib and sorafenib significantly inhibited platelet aggregation (20 μM sunitinib: 71.3%, p < 0.001; 25 μM sorafenib: 55.8%, p = 0.042). Sorafenib and sunitinib significantly inhibited P-selectin expression on platelets. Exposure to both TKIs resulted in a reduced tyrosine phosphorylation of c-Src. Ex vivo, within 24 h sunitinib impaired platelet aggregation (83.0%, p = 0.001, N = 8). Plasma concentrations of sunitinib, VEGF, and platelet/EC activation markers were not correlated with disturbed aggregation. In contrast, bevacizumab only significantly impaired platelet aggregation in vitro at high concentrations, but not ex vivo.
    Conclusion: Sunitinib significantly inhibits platelet aggregation in patients already after 24 h of first administration, whereas bevacizumab had no effect on aggregation. These findings may explain the clinically observed bleedings during treatment with antiangiogenic TKIs.
    MeSH term(s) Angiogenesis Inhibitors/pharmacology ; Bevacizumab/pharmacology ; Blood Platelets/metabolism ; Endothelial Cells/metabolism ; Female ; Humans ; Male ; P-Selectin/metabolism ; Platelet Aggregation/drug effects ; Sorafenib/pharmacology ; Sunitinib/pharmacology ; src-Family Kinases/metabolism
    Chemical Substances Angiogenesis Inhibitors ; P-Selectin ; Bevacizumab (2S9ZZM9Q9V) ; Sorafenib (9ZOQ3TZI87) ; CSK tyrosine-protein kinase (EC 2.7.10.2) ; src-Family Kinases (EC 2.7.10.2) ; Sunitinib (V99T50803M)
    Language English
    Publishing date 2018-03-12
    Publishing country Germany
    Document type Journal Article ; Research Support, Non-U.S. Gov't
    ZDB-ID 1484717-6
    ISSN 1573-7209 ; 0969-6970
    ISSN (online) 1573-7209
    ISSN 0969-6970
    DOI 10.1007/s10456-018-9598-5
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  8. Article: Thrombotic Events in COVID-19 Are Associated With a Lower Use of Prophylactic Anticoagulation Before Hospitalization and Followed by Decreases in Platelet Reactivity.

    Clark, Chantal C / Jukema, Bernard N / Barendrecht, Arjan D / Spanjaard, Judith S / Jorritsma, Nikita K N / Smits, Simone / de Maat, Steven / Seinen, Cor W / Verhoef, Sandra / Parr, Naomi M J / Sebastian, Silvie A E / Koekman, Arnold C / van Wesel, Annet C W / van Goor, Harriet M R / Spijkerman, Roy / Bongers, Suzanne H / van der Vries, Erhard / Nierkens, Stefan / Boes, Marianne /
    Koenderman, Leo / Kaasjager, Karin A H / Maas, Coen

    Frontiers in medicine

    2021  Volume 8, Page(s) 650129

    Abstract: Background: ...

    Abstract Background:
    Language English
    Publishing date 2021-04-22
    Publishing country Switzerland
    Document type Journal Article
    ZDB-ID 2775999-4
    ISSN 2296-858X
    ISSN 2296-858X
    DOI 10.3389/fmed.2021.650129
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  9. Article ; Online: Human pluripotent stem cell-derived kidney organoids for personalized congenital and idiopathic nephrotic syndrome modeling.

    Jansen, Jitske / van den Berge, Bartholomeus T / van den Broek, Martijn / Maas, Rutger J / Daviran, Deniz / Willemsen, Brigith / Roverts, Rona / van der Kruit, Marit / Kuppe, Christoph / Reimer, Katharina C / Di Giovanni, Gianluca / Mooren, Fieke / Nlandu, Quincy / Mudde, Helmer / Wetzels, Roy / den Braanker, Dirk / Parr, Naomi / Nagai, James S / Drenic, Vedran /
    Costa, Ivan G / Steenbergen, Eric / Nijenhuis, Tom / Dijkman, Henry / Endlich, Nicole / van de Kar, Nicole C A J / Schneider, Rebekka K / Wetzels, Jack F M / Akiva, Anat / van der Vlag, Johan / Kramann, Rafael / Schreuder, Michiel F / Smeets, Bart

    Development (Cambridge, England)

    2022  Volume 149, Issue 9

    Abstract: Nephrotic syndrome (NS) is characterized by severe proteinuria as a consequence of kidney glomerular injury due to podocyte damage. In vitro models mimicking in vivo podocyte characteristics are a prerequisite to resolve NS pathogenesis. The detailed ... ...

    Abstract Nephrotic syndrome (NS) is characterized by severe proteinuria as a consequence of kidney glomerular injury due to podocyte damage. In vitro models mimicking in vivo podocyte characteristics are a prerequisite to resolve NS pathogenesis. The detailed characterization of organoid podocytes resulting from a hybrid culture protocol showed a podocyte population that resembles adult podocytes and was superior compared with 2D counterparts, based on single-cell RNA sequencing, super-resolution imaging and electron microscopy. In this study, these next-generation podocytes in kidney organoids enabled personalized idiopathic nephrotic syndrome modeling, as shown by activated slit diaphragm signaling and podocyte injury following protamine sulfate, puromycin aminonucleoside treatment and exposure to NS plasma containing pathogenic permeability factors. Organoids cultured from cells of a patient with heterozygous NPHS2 mutations showed poor NPHS2 expression and aberrant NPHS1 localization, which was reversible after genetic correction. Repaired organoids displayed increased VEGFA pathway activity and transcription factor activity known to be essential for podocyte physiology, as shown by RNA sequencing. This study shows that organoids are the preferred model of choice to study idiopathic and congenital podocytopathies.
    MeSH term(s) Female ; Humans ; Kidney/metabolism ; Male ; Nephrotic Syndrome/genetics ; Nephrotic Syndrome/metabolism ; Nephrotic Syndrome/pathology ; Organoids ; Pluripotent Stem Cells/metabolism ; Podocytes/metabolism ; Podocytes/pathology
    Language English
    Publishing date 2022-05-06
    Publishing country England
    Document type Journal Article ; Research Support, Non-U.S. Gov't
    ZDB-ID 90607-4
    ISSN 1477-9129 ; 0950-1991
    ISSN (online) 1477-9129
    ISSN 0950-1991
    DOI 10.1242/dev.200198
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