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DOI: 10.1055/s-0031-1281743
© Georg Thieme Verlag KG Stuttgart · New York
Transarterial Hepatic Chemoperfusion of Uveal Melanoma Metastases: Survival and Response to Treatment
Transarterielle hepatische Chemoperfusion bei Aderhautmelanommetastasen: Überlebensdauer und TherapieansprechenPublication History
received: 12.3.2011
accepted: 9.8.2011
Publication Date:
27 October 2011 (online)
Zusammenfassung
Ziel: Evaluation der Überlebensdauer von Patienten mit hepatisch meastasierten Aderhautmelanomen unter sequentieller hepatischer Chemoperfusion. Material und Methoden: 61 Patienten (mittleres Alter: 60,3 ± 13,8 Jahre) wurden mit insgesamt 249 hepatischen Chemoperfusionen (Mittelwert: 4 Chemoperfusionen/Patient, Min.: 1 Chemoperfusion, Max.: 7 Chemoperfusionen, Standardabweichung: 2,3 Chemoperfusionen) behandelt. Bei allen Patienten wurde die Therapie mit Melphalan begonnen. Im Falle eines Progresses wurde Melphalan durch ein alternatives Chemoperfusionspräparat ersetzt. 38 Patienten wurden ausschließlich mit Melphalan behandelt, 23 Patienten wurden mit Melphalan, gefolgt von einer Chemoperfusion mit anderen Substanzen behandelt. Die mediane Überlebenszeit wurde für die gesamte Population und unterschiedliche Subgruppen errechnet. Es wurden statistisch signifikante Unterschiede bezüglich der Überlebensdauer zwischen den Subgruppen ermittelt. Die Komplikationsrate wurde ermittelt. Ergebnisse: Die mittlere Überlebensdauer der Gesamtpopulation betrug 10 Monate. Die Patienten der Subgruppe, die an maximal 9 hepatischen Metastasen litt, sowie die der Subgruppe, die keine extrahepatischen Metastasen zu Beginn der Therapie aufwies, überlebten statistisch signifikant länger als die Patienten mit mehr als 9 Metastasen/extrahepatischen Metastasen (p = 0,019, p = 0,008). Ein Patient (0,4 %) verstarb im Leberversagen nach initialer Chemoperfusion mit Melphalan. Schlussfolgerung: Sequenzielle intraarterielle hepatische Chemoperfusionen stellen eine minimalinvasive Behandlungsmöglichkeit mit guten Überlebensdauern und einer akzeptablen Major-Komplikationsrate bei Patienten mit hepatischen metastasierten Aderhautmelanomen dar.
Abstract
Purpose: To assess the survival of patients with hepatic uveal melanoma metastases undergoing sequential transarterial hepatic chemoperfusion. Materials and Methods: 61 patients (mean age, 60.3 ± 13.8y) underwent a total of 249 hepatic chemoperfusion procedures (mean: 4 chemoperfusion procedures; range, 1 – 7 chemoperfusion procedures; standard deviation, 2.3 chemoperfusion procedures). All patients started with melphalan. In the case of progressive disease, melphalan was replaced by a different chemoperfusion agent. 38 patients were treated with melphalan only, 23 patients were treated with a combination of melphalan and other drugs. The median overall survival time was calculated for the overall population and several sub-groups. Differences in the survival rate between the sub-groups were assessed for statistical significance. The complication rate was assessed. Results: The median overall survival of the entire population was 10 months. The patients in the subgroups with a maximum number of 9 hepatic metastases as well as the patients in the subgroup without extrahepatic metastases at the beginning of therapy survived significantly longer than patients with more than 9 metastases/extrahepatic metastases (p = 0.019, p = 0.008). One patient (0.4 %) died from liver failure after initial infusion of melphalan. Conclusion: Intraarterial sequential hepatic chemoperfusion offers a minimally invasive treatment in patients with hepatic uveal melanoma metastases with good survival times and an acceptable major complication rate.
Key words
angiography - interventional procedures - uveal melanoma - ocular melanoma - melphalan - chemoperfusion
References
- 1
Virgili G, Gatta G, Ciccolallo L et al.
Incidence of uveal melanoma in Europe.
Ophthalmology.
2007;
114
2309-2315
MissingFormLabel
- 2
Egan K M, Seddon J M, Glynn R J et al.
Epidemiologic aspects of uveal melanoma.
Surv Ophthalmol.
1988;
32
239-251
MissingFormLabel
- 3
Eskelin S, Pyrhonen S, Summanen P et al.
Tumor doubling times in metastatic malignant melanoma of the uvea: tumor progression
before and after treatment.
Ophthalmology.
2000;
107
1443-1449
MissingFormLabel
- 4
Bedikian A Y, Legha S S, Mavligit G et al.
Treatment of uveal melanoma metastatic to the liver: a review of the M. D. Anderson
Cancer Center experience and prognostic factors.
Cancer.
1995;
76
1665-1670
MissingFormLabel
- 5
Herman P, Machado M A, Montagnini A L et al.
Selected patients with metastatic melanoma may benefit from liver resection.
World J Surg.
2007;
31
171-174
MissingFormLabel
- 6
Gragoudas E S, Egan K M, Seddon J M et al.
Survival of patients with metastases from uveal melanoma.
Ophthalmology.
1991;
98
383-389
; discussion 390
MissingFormLabel
- 7
Kath R, Hayungs J, Bornfeld N et al.
Prognosis and treatment of disseminated uveal melanoma.
Cancer.
1993;
72
2219-2223
MissingFormLabel
- 8
Rajpal S, Moore R, Karakousis C P.
Survival in metastatic ocular melanoma.
Cancer.
1983;
52
334-336
MissingFormLabel
- 9
Peters S, Voelter V, Zografos L et al.
Intra-arterial hepatic fotemustine for the treatment of liver metastases from uveal
melanoma: experience in 101 patients.
Ann Oncol.
2006;
17
578-583
MissingFormLabel
- 10
Lane A M, Egan K M, Harmon D et al.
Adjuvant interferon therapy for patients with uveal melanoma at high risk of metastasis.
Ophthalmology.
2009;
116
2206-2212
MissingFormLabel
- 11
Sato T, Eschelman D J, Gonsalves C F et al.
Immunoembolization of malignant liver tumors, including uveal melanoma, using granulocyte-macrophage
colony-stimulating factor.
J Clin Oncol.
2008;
26
5436-5442
MissingFormLabel
- 12
Yamamoto A, Chervoneva I, Sullivan K L et al.
High-dose immunoembolization: survival benefit in patients with hepatic metastases
from uveal melanoma.
Radiology.
2009;
252
290-298
MissingFormLabel
- 13
Mavligit G M, Charnsangavej C, Carrasco C H et al.
Regression of ocular melanoma metastatic to the liver after hepatic arterial chemoembolization
with cisplatin and polyvinyl sponge.
Jama.
1988;
260
974-976
MissingFormLabel
- 14
Bates D A, Mackillop W J.
The effect of hyperthermia in combination with melphalan on drug-sensitive and drug-resistant
CHO cells in vitro.
Br J Cancer.
1990;
62
183-188
MissingFormLabel
- 15
Zee van der J, Kroon B B, Nieweg O E et al.
Rationale for different approaches to combined melphalan and hyperthermia in regional
isolated perfusion.
Eur J Cancer.
1997;
33
1546-1550
MissingFormLabel
- 16
Hafstrom L R, Holmberg S B, Naredi P L et al.
Isolated hyperthermic liver perfusion with chemotherapy for liver malignancy.
Surg Oncol.
1994;
3
103-108
MissingFormLabel
- 17
Rothbarth J, Pijl M E, Vahrmeijer A L et al.
Isolated hepatic perfusion with high-dose melphalan for the treatment of colorectal
metastasis confined to the liver.
Br J Surg.
2003;
90
1391-1397
MissingFormLabel
- 18
Vahrmeijer A L, Dierendonck J H, Keizer H J et al.
Increased local cytostatic drug exposure by isolated hepatic perfusion: a phase I
clinical and pharmacologic evaluation of treatment with high dose melphalan in patients
with colorectal cancer confined to the liver.
Br J Cancer.
2000;
82
1539-1546
MissingFormLabel
- 19
Voelter van V, Schalenbourg A, Pampallona S et al.
Adjuvant intra-arterial hepatic fotemustine for high-risk uveal melanoma patients.
Melanoma Res.
2008;
18
220-224
MissingFormLabel
- 20
Egerer G, Lehnert T, Max R et al.
Pilot study of hepatic intraarterial fotemustine chemotherapy for liver metastases
from uveal melanoma: a single-center experience with seven patients.
Int J Clin Oncol.
2001;
6
25-28
MissingFormLabel
- 21
Fety R, Lucas C, Solere P et al.
Hepatic intra-arterial infusion of fotemustine: pharmacokinetics.
Cancer Chemother Pharmacol.
1992;
31
118-122
MissingFormLabel
- 22
Etten van B, Wilt J H, Brunstein de F et al.
Isolated hypoxic hepatic perfusion with melphalan in patients with irresectable ocular
melanoma metastases.
Eur J Surg Oncol.
2009;
35
539-545
MissingFormLabel
- 23
Alexander H R, Libutti S K, Pingpank J F et al.
Hyperthermic isolated hepatic perfusion using melphalan for patients with ocular melanoma
metastatic to liver.
Clin Cancer Res.
2003;
9
6343-6349
MissingFormLabel
- 24
Iersel L B, Hoekman E J, Gelderblom van H et al.
Isolated hepatic perfusion with 200 mg melphalan for advanced noncolorectal liver
metastases.
Ann Surg Oncol.
2008;
15
1891-1898
MissingFormLabel
- 25
Noter S L, Rothbarth Jr J, Pijl M E et al.
Isolated hepatic perfusion with high-dose melphalan for the treatment of uveal melanoma
metastases confined to the liver.
Melanoma Res.
2004;
14
67-72
MissingFormLabel
- 26
Leoni C J, Potter J E, Rosen M P et al.
Classifying complications of interventional procedures: a survey of practicing radiologists.
J Vasc Interv Radiol.
2001;
12
55-59
MissingFormLabel
- 27
Rivoire M, Kodjikian L, Baldo S et al.
Treatment of liver metastases from uveal melanoma.
Ann Surg Oncol.
2005;
12
422-428
MissingFormLabel
- 28
Leyvraz S, Spataro V, Bauer J et al.
Treatment of ocular melanoma metastatic to the liver by hepatic arterial chemotherapy.
J Clin Oncol.
1997;
15
2589-2595
MissingFormLabel
- 29
Becker J C, Terheyden P, Kampgen E et al.
Treatment of disseminated ocular melanoma with sequential fotemustine, interferon
alpha, and interleukin 2.
Br J Cancer.
2002;
87
840-845
MissingFormLabel
- 30
Albert M L, Sauter B, Bhardwaj N.
Dendritic cells acquire antigen from apoptotic cells and induce class I-restricted
CTLs.
Nature.
1998;
392
86-89
MissingFormLabel
- 31
Bowen D G, McCaughan G W, Bertolino P.
Intrahepatic immunity: a tale of two sites?.
Trends Immunol.
2005;
26
512-517
MissingFormLabel
- 32
Fiorentini G, Aliberti C, Del Conte A et al.
Intra-arterial hepatic chemoembolization (TACE) of liver metastases from ocular melanoma
with slow-release irinotecan-eluting beads. Early results of a phase II clinical study.
In Vivo.
2009;
23
131-137
MissingFormLabel
- 33
Vogl T, Eichler K, Zangos S et al.
Preliminary experience with transarterial chemoembolization (TACE) in liver metastases
of uveal malignant melanoma: local tumor control and survival.
J Cancer Res Clin Oncol.
2007;
133
177-184
MissingFormLabel
- 34
Osuga K, Hori S, Hiraishi K et al.
Bland embolization of hepatocellular carcinoma using superabsorbent polymer microspheres.
Cardiovasc Intervent Radiol.
2008;
31
1108-1116
MissingFormLabel
- 35
Gonsalves C F, Eschelman D J, Sullivan K L et al.
Radioembolization as salvage therapy for hepatic metastasis of uveal melanoma: a single-institution
experience.
Am J Roentgenol.
2011;
196
468-473
MissingFormLabel
- 36
Antoch G, Mueller S P, Hamami M et al.
Selective internal radiotherapy (SIRT) for hepatocellular carcinoma.
Fortschr Röntgenstr.
2010;
182
660-670
MissingFormLabel
- 37
Hamami M E, Poeppel T D, Muller S et al.
SPECT/CT with 99mTc-MAA in radioembolization with 90Y microspheres in patients with
hepatocellular cancer.
J Nucl Med.
2009;
50
688-692
MissingFormLabel
- 38
Heusner T A, Hamami M E, Ertle J et al.
Angiography-based C-arm CT for the assessment of extrahepatic shunting before radioembolization.
Fortschr Röntgenstr.
2010;
182
603-608
MissingFormLabel
Dr. Till-Alexander Heusner
Institut für Diagnostische und Interventionelle Radiologie und Neuroradiologie, Universitätsklinik
Essen
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