Viktoria Florentine Köhler scite author profile

Viktoria Florentine Köhler

3Publications

8Citation Statements Received

125Citation Statements Given

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119

Affiliations

Goethe University Frankfurt, Bethesda Spital, Charité - Universitätsmedizin Berlin

Publications

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Clinical Outcome and Toxicity in the Treatment of Anaplastic Thyroid Cancer in Elderly Patients

Augustin

Oliinyk

Köhler

et al. 2020

JCM

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Background: The present study aims to evaluate the outcomes and toxicity of elderly anaplastic thyroid cancer (ATC) patients receiving (chemo)radiotherapy, as well as to identify prognostic factors. Patients and methods: A systematic review using the MEDLINE/PubMed and Cochrane databases was performed. Individual data from all eligible studies were extracted, and a pooled analysis (n = 186) was conducted to examine patient characteristics and treatment. All consecutive ATC patients (≥65 years) treated between 2009 and 2019 at our institution were evaluated for outcomes concerning progression-free survival (PFS), overall survival (OS) probabilities and treatment-related toxicity. Results: The systematic review and pooled analysis identified age as a prognostic factor. The median OS of our patient cohort (n = 26) was three months (range = 0–125). The 6-, 12- and 24-month survival rates were 35%, 22% and 11%, respectively. In the univariate analysis, a Karnofsky performance status of >70%, the Union for International Cancer Control Tumor–Node–Metastasis classification, multimodal therapy and an EQD2 of >49 Gy were correlated with longer OS and PFS. The acute grade 3 toxicity of dysphagia, dyspnea, dermatitis, mucositis and dysphonia was found in 23%, 15%, 12%, 12% and 8% of patients. Conclusion: Age appears to be a prognostic factor in ATC. Elderly ATC patients can tolerate multimodal treatment and achieve a promising outcome. Prospective studies need to confirm our findings.

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Biotin Interference in the Measurement of Thyroid Hormone

Köhler¹,

Mann²,

Mann³

2018

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Biotin Interference in the Measurement of Thyroid Hormone A 47-year-old man with multiple sclerosis (MS) presented for routine follow-up and underwent a battery of laboratory tests because of a change in his drug therapy for MS. He was found to have hyperthyroidism with positive thyroid-specific autoantibodies. This determination was made by an immunoassay based on streptavidin-biotin interaction. As the laboratory finding was not correlated with any clinical abnormality, no thyrostatic treatment was initiated. On further questioning, the patient stated that he was taking 300 mg of biotin daily to treat his MS. Another test with a non-biotinylated assay yielded normal findings. It should be borne in mind that discrepancies between the clinical presentation and the laboratory findings of patients taking biotin may be due to biotin interference with the test. The test values that may be affected include endocrinological parameters, tumor markers, and myocardial lesion markers. There is some evidence for the efficacy of high-dose biotin intake against progressive MS; as clinical trials of this question are currently ongoing, it must be assumed that an increasing number of patients are high-dose biotin users. Biotin intake should be paused two to five days before streptavidin-biotin-based assays are used. Non-biotinylated assays are an alternative.

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Medulläres Schilddrüsenkarzinom

Kroiß

Köhler

Spitzweg

2021

Dtsch Med Wochenschr

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Was ist neu? Diagnose und Prognose Calcitonin ist ein sensitiver und spezifischer Tumormarker zur Früherkennung und Verlaufskontrolle des MTC. Daneben kommt dem Ultraschall der Schilddrüse eine entscheidende Rolle zu. Rolle des RET-Proto-Onkogens Das medulläre Schilddrüsenkarzinom (MTC) nimmt seinen Ursprung aus den parafollikulären Calcitonin-produzierenden C-Zellen. Es macht nur ca. 3–8 % aller Schilddrüsenkarzinome aus. Aktivierende Mutationen im RET (rearranged during transfection)-Gen liegen bei etwa 25 % der Patienten in der Keimbahn vor, werden aber auch beim sporadischen MTC als somatische Mutationen in ca. 60 % der Fälle beobachtet. Bei metastasierter Erkrankung findet sich in 90 % eine RET-Mutation. RET-Mutationen gelten als Treibermutationen und schließen weitere Treibermutationen weitestgehend aus. Seltener sind somatische Mutationen der RAS-Gene. Chirurgische Therapie Die chirurgische Resektion ist bis heute der einzige kurative Therapieansatz. Entscheidend für eine frühzeitige Diagnosestellung ist die Bestimmung des Serum-Calcitonins bei Nachweis von Schilddrüsenknoten. Die chirurgische Therapie steht auch bei der Behandlung lokoregionärer Rezidive oder lokal angehbarer Metastasen im Zentrum. Systemtherapie Bei irresektabel fortgeschrittener und progredienter Erkrankung mit signifikanter Tumorlast kann eine systemische Therapie erforderlich werden. Neuerdings ist die Kenntnis einer RET-Mutation im Tumorgewebe therapeutisch relevant, da mit den selektiven RET-Inhibitoren Selpercatinib und zukünftig Pralsetinib neue, effektive und gut verträgliche Systemtherapien zur Verfügung stehen. Ihr Einsatz ist nach Vortherapie mit einem der Multityrosinkinase-Inhibitoren Vandetanib oder Cabozantinib zugelassen und wird derzeit in der Erstlinientherapie in klinischen Studien untersucht.

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