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Aktuelle Ausschreibungen der Hiege-Stiftung gegen Hautkrebs - 2018

Gerne machen wir auf die diesjährigen Ausschreibungen der Hiege-Stiftung gegen Hautkrebs aufmerksam. Die Details finden Sie in den beiliegenden PDF-Dokumenten.

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NUB-Anträge 2017/8 verfügbar

Die aktuellen Template für die NUB-Anträge 2017/8 sind online.

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Präsentation der Studiensitzung verfügbar

Die Folien mussten leider von der Seite entfernt werden.

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Hautkrebskongress 2017: Neue Erkenntnisse und aktuelle Therapiemöglichkeiten in der Dermato-Onkologie

Beim 27. Deutschen Hautkrebskongress der ADO und der Deutschen Dermatologischen Gesellschaft, der vom 21. - 23. September 2017 in Mainz stattfindet, werden vielversprechende aktuelle Erkenntnisse und Forschungsergebnisse in Prävention, Diagnostik und Therapie in der Dermato-Onkologie vorgestellt und von internationalen Experten diskutiert.

Nicht nur in der Therapie des fortgeschrittenen Melanoms, des Basalzellkarzinoms und in der Behandlung aktinischer Keratosen, auch bei anderen Hautkrebsarten gibt es hoffnungsvolle Fortschritte. Herr Prof. Stephan Grabbe und Frau PD Dr. med. Carmen Loquai geben Einblick in Highlights des Kongresses.

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Nationale Versorgungskonferenz Hautkrebs verabschiedet Ziele zur besseren Patientenversorgung bis 2021

Die Nationale Versorgungskonferenz Hautkrebs (NVKH) hat ihre Versorgungsziele 2017-2021 verabschiedet. Gemeinsam mit Patientenvertretern haben die beteiligten Fachgesellschaften und Verbände fünf nationale Versorgungsziele gegen den Hautkrebs definiert. Übergeordnetes Ziel ist es, die Prävention und Versorgung von Hautkrebs bundesweit zu verbessern.

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PubMed – Neue Publikationen

Determinants of illness-specific social support and its relation to distress in long-term melanoma survivors.

Related Articles

Determinants of illness-specific social support and its relation to distress in long-term melanoma survivors.

BMC Public Health. 2018 Apr 17;18(1):511

Authors: Fischbeck S, Weyer-Elberich V, Zeissig SR, Imruck BH, Blettner M, Binder H, Beutel ME

Abstract
BACKGROUND: Social support is considered to be one of the most important resources for coping with cancer. However, social interactions may also be detrimental, e. g. disappointing or discouraging. The present study explored: 1. the extent of illness-specific positive aspects of social support and detrimental interactions in melanoma survivors, 2. their relationships to mental health characteristics (e. g. distress, quality of life, fatigue, coping processes, and dispositional optimism) and 3. Combinations of positive social support and detrimental interactions in relation to depression and anxiety.
METHODS: Based on the cancer registry of Rhineland-Palatinate, Germany, melanoma patients diagnosed at least 5 years before the survey were contacted by their physicians. N = 689 melanoma patients filled out the Illness-specific Social Support Scale ISSS (German version) and standardised instruments measuring potential psychosocial determinants of social support.
RESULTS: Using principal component analysis, the two factor structure of the ISSS could be reproduced with acceptable reliability; subscales were "Positive Support" (PS) and "Detrimental Interactions" (DI); Cronbach's α = .95/.72. PS was rated higher than DI. Multivariable linear regressions identified different associations with psychosocial determinants. Survivors living in a partnership and those actively seeking out support had a higher probability of receiving PS, but not DI. PS and DI interacted regarding their association with distress: Survivors reporting high DI but low PS were the most depressed and anxious. High DI was partly buffered by PS. When DI was low, high or low PS made no difference regarding distress.
CONCLUSION: Psycho-oncologic interventions should take into account both positive and negative aspects of support in order to promote coping with the disease.

PMID: 29665805 [PubMed - in process]

The Great Debate at "Melanoma Bridge", Napoli, December 2nd, 2017.

Related Articles

The Great Debate at "Melanoma Bridge", Napoli, December 2nd, 2017.

J Transl Med. 2018 Apr 17;16(1):101

Authors: Ascierto PA, Caracò C, Gershenwald JE, Hamid O, Ross M, Sullivan RJ, Puzanov I

Abstract
As part of the 2017 Melanoma Bridge congress (November 30-December 2, 2017, Napoli, Italy), the great debate session featured counterpoint views from leading experts on three contemporary controversial clinical issues in the care of the melanoma patient. These were: (1) whether complete lymph node dissection should be routinely offered to all melanoma patients with sentinel lymph node-positive disease; (2) whether first-line treatment of BRAF-mutated melanoma should consist of BRAF-targeted therapy or immunotherapy with checkpoint inhibitors; and (3) whether combined or sequential administration of treatments should be the preferred option in the management of patients with advanced melanoma. Discussion of these three important issues and audience responses are reported here.

PMID: 29665799 [PubMed - in process]

PDQ Cancer Information Summaries

Related Articles

PDQ Cancer Information Summaries

Book. 2002

Authors:

Abstract
This PDQ cancer information summary has current information about the treatment of intraocular melanoma. It is meant to inform and help patients, families, and caregivers. It does not give formal guidelines or recommendations for making decisions about health care. Editorial Boards write the PDQ cancer information summaries and keep them up to date. These Boards are made up of experts in cancer treatment and other specialties related to cancer. The summaries are reviewed regularly and changes are made when there is new information. The date on each summary ("Date Last Modified") is the date of the most recent change. The information in this patient summary was taken from the health professional version, which is reviewed regularly and updated as needed, by the PDQ Adult Treatment Editorial Board.


PMID: 26389277

Phase II Study of Everolimus in Metastatic Malignant Melanoma (NCCTG-N0377, Alliance).

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Phase II Study of Everolimus in Metastatic Malignant Melanoma (NCCTG-N0377, Alliance).

Oncologist. 2018 Apr 17;:

Authors: Vera Aguilera J, Rao RD, Allred JB, Suman VJ, Windschitl HE, Kaur JS, Maples WJ, Lowe VJ, Creagan ET, Erickson LA, Markovic S

Abstract
LESSONS LEARNED: Everolimus does not have sufficient activity to justify its use as single agent in metastatic melanoma.Patients treated with 10 mg per day dose were most likely to require dose reductions.Everolimus appeared to reduce the numbers of regulatory T cells in approximately half of the treated patients; unfortunately, these effects were not correlated with clinical outcomes.
BACKGROUND: Everolimus (RAD-001) is an orally active rapamycin analogue shown in preclinical data to produce cytostatic cell inhibition, which may be potentially beneficial in treating melanoma. We conducted a phase II study to evaluate the efficacy and safety of everolimus in patients with unresectable metastatic melanoma (MM).
METHODS: This study included two cohorts; cohort 1 received 30 mg of everolimus by mouth (PO) weekly, and cohort 2 was dosed with 10 mg of everolimus PO daily. The endpoints of the study were safety, 16-week progression-free survival (PFS), overall survival (OS), and measures of immunomodulatory/antiangiogenic properties with therapy. Tumor samples before therapy and at week 8 of treatment were analyzed. Peripheral blood plasma or mononuclear cell isolates collected prior to therapy and at weeks 8 and 16 and at time of tumor progression were analyzed for vascular endothelial growth factor and regulatory T-cell (Treg) measurements.
RESULTS: A total of 53 patients were enrolled in cohort 1 (n = 24) and cohort 2 (n = 29). Only 2 patients of the first 20 patients enrolled in cohort 2 had treatment responses (25%; 95% confidence interval, 8.6%-49.1%); this result did not allow full accrual to cohort 2, as the study was terminated for futility. Median OS was 12.2 months for cohort 1 versus 8.1 months in cohort 2; no PFS advantage was seen in either group (2.1 months vs. 1.8 months). Dose-limiting toxicities included grade 4 myocardial ischemia (3.4%); grade 3 fatigue, mucositis, and hyperglycemia (10.3%); and anorexia and anemia (6.9%). Everolimus significantly reduced the number of Tregs in approximately half of the treated patients; however, these effects were not correlated with clinical outcomes.
CONCLUSION: Everolimus does not have sufficient single-agent activity in MM; however, we have identified evidence of biological activity to provide a potential rationale for future combination studies.

PMID: 29666297 [PubMed - as supplied by publisher]

Myasthenia Gravis Induced by Ipilimumab in a Patient With Metastatic Melanoma.

Related Articles

Myasthenia Gravis Induced by Ipilimumab in a Patient With Metastatic Melanoma.

Front Neurol. 2018;9:150

Authors: Montes V, Sousa S, Pita F, Guerreiro R, Carmona C

Abstract
In daily clinical practice, there is a growing number of patients receiving new biological agents used in the treatment of malignancies. Ipilimumab is a fully humanized monoclonal antibody approved for patients with melanoma. It acts as an immune checkpoint inhibitor, binding and blocking cytotoxic T-lymphocyte antigen-4 in order to increase the antitumor immune response. There are several reports of autoimmune responses after its use. A 74-year-old man developed a mild rash and pruritus a few hours after the second infusion of ipilimumab and 24 h after the third dose of ipilimumab, he presented with shortness of breath, proximal limb muscle weakness, and diplopia. Repetitive nerve stimulation was consistent with a postsynaptic neuromuscular junction disorder. He began therapy with corticosteroids and pyridostigmine and ipilimumab was discontinued. Following ipilimumab suspension, the patient started to improve gradually. Here, we describe a rare case of myasthenia gravis presumably related with ipilimumab's therapy. A better knowledge of these agents is necessary, in order to identify characteristics or biomarkers that may be associated with the development of potentially serious autoimmune responses.

PMID: 29666602 [PubMed]

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