Chemotherapy response assessment in stage IV melanoma patients—comparison of 18F-FDG-PET/CT, CT, brain MRI, and tumormarker S-100B

Strobel, Klaus; Dummer, Reinhard; Steinert, H.; Conzett, Katrin Baumann; Schad, Karin; Lago, Marisol Pérez; Soyka, Jan; Veit-Haibach, Patrick; Seifert, Burkhardt; Kalff, Victor

doi:10.1007/s00259-008-0806-1

Cited by 45 publications

(18 citation statements)

References 33 publications

(38 reference statements)

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“…In patients with many different cancers including melanoma, the early response to chemotherapy correlates with the significant decrease in [ 18 F]FDG tumor uptake during PET due to an inability of dying or dead cells to actively take up glucose and predicts the overall response to therapy (20). Likewise, in tumor-bearing mice treated with chemotherapy, the decrease in [ 18 F]FDG tumor uptake in comparison with the baseline value was much less pronounced than in mice treated with RIT alone.…”

Section: Discussionmentioning

confidence: 99%

Radioimmunotherapy of Experimental Human Metastatic Melanoma with Melanin-Binding Antibodies and in Combination with Dacarbazine

Revskaya¹,

Jongco

Sellers³

et al. 2009

Clinical Cancer Research

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Purpose: Melanin has emerged as an attractive target for radioimmunotherapy (RIT) of melanoma, and a radiolabeled monoclonal antibody (mAb) 6D2 to melanin is currently in clinical evaluation. We investigated two approaches to improve the targeting of radiation to tumors using melanin-binding mAbs: (a) the use of an additional mAb to melanin could provide information on whether using antibodies to melanin can serve as a general approach to development of therapeutics for melanoma, and (b) as melanin targeting involves the antibody binding to extracellular melanin released from necrotic melanoma cells, we hypothesized that the administration of a chemotherapeutic agent followed by RIT would facilitate the delivery of radiation to the tumors due to the increased presence of free melanin. Experimental Design: We evaluated the therapeutic efficacy of two melanin-binding IgM mAbs labeled with 188 Re (6D2 and 11B11). We compared the efficacy of RIT with 188Re-6D2 to chemotherapy with dacarbazine (DTIC) and to combined chemotherapy and RIT in human metastatic melanoma-bearing nude mice. Results: Therapeutic efficacy of 188 Re-labeled 6D2 and 11B11 was comparable despite differences in their affinity and binding site numbers. Comparison of chemotherapy with DTIC and RITrevealed that RIT was more effective in slowing tumor growth in mice. Administration of DTIC followed by RITwas more effective than either modality alone. Conclusions: These results provide encouragement for the development of RIT for melanoma with melanin-binding mAbs and suggest that combining chemotherapy and RIT may be a promising approach for the treatment of metastatic melanoma.

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Section: Discussionmentioning

confidence: 99%

Radioimmunotherapy of Experimental Human Metastatic Melanoma with Melanin-Binding Antibodies and in Combination with Dacarbazine

Revskaya¹,

Jongco

Sellers³

et al. 2009

Clinical Cancer Research

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“…There is a significantly longer progression-free survival of PET/CT responders compared with PET/CT nonresponders. As chemotherapy response assessment with serum S-100B tumor marker fails to show correlation with survival, 18F-FDG PET/CT may present a promising tool (Strobel et al 2008). Strobel et al also reached to the same conclusion.…”

Section: Melanomamentioning

confidence: 99%

Assessment of Response to Therapy

Gholamrezanezhad

Chirindel

Subramaniam

2012

PET-CT and PET-MRI in Oncology

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“…Both 18 F-FDG PET/CT and MRI are sensitive to changes under local and systemic therapy. 18 F-FDG PET/CT has been shown to outperform the tumor marker S100 in the discrimination of responders from nonresponders in a study on stage IV melanoma patients (48). Responders to chemotherapy identified by 18 F-FDG PET/CT in a retrospectively performed evaluation have been proven to have a longer progression-free and overall survival than nonresponders (48).…”

Section: Melanomamentioning

confidence: 99%

“…18 F-FDG PET/CT has been shown to outperform the tumor marker S100 in the discrimination of responders from nonresponders in a study on stage IV melanoma patients (48). Responders to chemotherapy identified by 18 F-FDG PET/CT in a retrospectively performed evaluation have been proven to have a longer progression-free and overall survival than nonresponders (48). Experimental studies performed mainly ex vivo on melanoma xenografts reported that the amount of tumor cell necrosis and the oxygenation status of tumor cells could be assessed using nuclear MR spectroscopy (49).…”

Section: Melanomamentioning

confidence: 99%

“…Experimental studies performed mainly ex vivo on melanoma xenografts reported that the amount of tumor cell necrosis and the oxygenation status of tumor cells could be assessed using nuclear MR spectroscopy (49). More clinically relevant is the potential of MRI in restaging brain metastases, as these have been proven to be predictive of a poor prognosis (48). Data on the performance of integrated PET/MRI in melanoma restaging and response assessment are awaited but not available at present.…”

Section: Melanomamentioning

confidence: 99%

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Oncologic PET/MRI, Part 2: Bone Tumors, Soft-Tissue Tumors, Melanoma, and Lymphoma

Buchbender

Heusner²,

Lauenstein³

et al. 2012

J Nucl Med

149

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Learning Objectives: On successful completion of this activity, participants should be able to describe (1) the advantages and disadvantages of PET/MRI in oncologic applications in comparison to conventional imaging methods and PET/CT; (2) the limitations of PET/MRI compared with invasive staging procedures (biopsy); and (3) the metabolic-anatomic imaging procedure of choice (PET/MRI vs. PET/CT) based on tumor entity and location.Financial Disclosure: The authors of this article have indicated no relevant relationships that could be perceived as a real or apparent conflict of interest. CME Credit: SNM is accredited by the Accreditation Council for Continuing Medical Education (ACCME) to sponsor continuing education for physicians. SNM designates each JNM continuing education article for a maximum of 2.0 AMA PRA Category 1 Credit. Physicians should claim only credit commensurate with the extent of their participation in the activity.For CE credit, participants can access this activity through the SNM Web site (http://www.snm.org/ce_online) through August 2013.With integrated whole-body PET/MRI, a novel metabolicanatomic imaging technique recently has been introduced into clinical practice. This review addresses PET/MRI of bone tumors, soft-tissue sarcoma, melanoma, and lymphoma. If PET/ MRI literature is not yet available for some types of tumors, potential indications are based on available PET/CT and MRI data. PET/MRI seems to be of benefit in T-staging of primary bone tumors and soft-tissue sarcomas. With regard to N-staging, PET/MRI can be considered similarly accurate to PET/CT when applied as a whole-body staging approach. M-staging will benefit from MRI accuracy in the brain, the liver, and bone. Imagi ng plays a key role in diagnosis and staging in oncology. Evaluation of local tumor extent and detection of potential locoregional lymph node or distant metastases according to the periodically revised standardized TNM cancer staging system (1) directly affects patient care by defining the most suitable therapy. With integrated wholebody PET/MRI, a new metabolic-anatomic imaging modality has been introduced into clinical practice. Despite the fact that the solution of basic problems, such as adequate MRI-based attenuation correction, is still a work in progress (2), reports on initial clinical experiences with PET/MRI in oncology are already available. In this second part of our review on PET/MRI in oncologic applications, we summarize the available first experiences with PET/ MRI in bone tumors, soft-tissue sarcoma, melanoma, and lymphoma. In fields where PET/MRI data are lacking, we outline the potential role of PET/MRI on the basis of the PET/CT and MRI literature. To provide further information on PET/MRI, we refer to our own unpublished experiences with PET

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Chemotherapy response assessment in stage IV melanoma patients—comparison of 18F-FDG-PET/CT, CT, brain MRI, and tumormarker S-100B

Cited by 45 publications

References 33 publications

Radioimmunotherapy of Experimental Human Metastatic Melanoma with Melanin-Binding Antibodies and in Combination with Dacarbazine

Radioimmunotherapy of Experimental Human Metastatic Melanoma with Melanin-Binding Antibodies and in Combination with Dacarbazine

Assessment of Response to Therapy

Oncologic PET/MRI, Part 2: Bone Tumors, Soft-Tissue Tumors, Melanoma, and Lymphoma

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