Abstract
To increase the therapeutic efficacy of recombinant tumor necrosis factor alpha (rTNFα) and reduce the systemic side effects, a protocol was designed using isolation perfusion of the limbs with hyperthermia for in transit metastases of melanoma. A triple combination of high dose rTNFα + recombinant interferon-gamma (rIFN-γ) + melphalan was chosen because of a synergistic anti-tumor effect of rTNFα with rIFN-γ and of rTNFα with alkylating agents reported in the literature. Twenty-nine patients of mean age 60 years (range 22–82 years) entered the study after informed consent and received a total of 31 isolation perfusions with the triple combination. There were 24 women and 5 men with multiple progressivein transit melanoma metastases of the lower limb (stage IIIa or IIIab). rTNFα at the unique dose of 4 mg was injected as a bolus in the arterial line, under mild hyperthermic conditions (40 to 40.5°C) for 90 minutes. rIFN-γ was given subcutaneously on days −2 and −1 and in the perfusate, with rTNFα, at the dose of 0.2 mg. Melphalan was administered in the perfusate at dose giving a concentration of 40 µg/ml.
In all the 31 isolation perfusions performed in the triple combination protocol, in order to prevent a septic shock-like syndrome which had been encountered in 2 patients treated outside this protocol for sarcoma and carcinoma, the patients received dopamine continuous infusion at 3 µg/kg/min from the start of isolation perfusion and for 48 hours, and only showed mild hyptension and very transient chills and temperature. Regional toxicity attributable to rTNFα was minimal. There have been 16 patients with hematologic toxicity consisting of neutropenia (11 cases, 1 case grade 4 and 1 case grade 3) and neutropenia with thrombocytopenia (12 cases, 1 case grade 4 and 4 cases grade 2). Eighteen of 29 patients had been previously treated with melphalan in isolation perfusion (n=13) or with cisplatinum (n=2), rTNFα-Melphalan (n=1), or rTNFα alone (n=2). Median follow-up has been 41 weeks. The 29 patients are evaluable: there have been 26 (90%) complete remissions (CR), 3 (10%) partial remissions (PR), and no failures. Actuarial disease-free survival and total survival have been 63% and 73%, respectively, at 12 months. In all cases, softening of the nodules was obvious within 3 days after isolation perfusion and time to definite response ranged between day 6 and 22.
This interim analysis of a phase II study suggests that high dose of rTNFα can be administered with acceptable toxicity by isolation perfusion with dopamine and hyperhydration. Tumor responses can be evidenced in all patients, with 90% CR. Furthermore, combination of rTNFα, rIFN-γ, and melphalan seems to achieve high efficacy with minimal toxicity, even after failure of prior therapy with melphalan alone.
Résumé
Pour augmenter l'efficacité thérapeutique du facteur recombinant de nécrose tumorale alpha (rTNFα) et pour réduire les effets secondaires, on a élaboré un protocole utilisant une perfusion isolée des extrémités associée à une hyperthermie chez les patients atteints de métastases d'un mélanome. En raison d'un effet synergique antitumoral, de rTNFα et de l'interféron gamma recombinant (rIFN) d'une part et de rTNFα et des agents alkylisants d'autres part (effet rapporté dans la littérature), on a utilisé une triple combinaison de rTNFα à hautes doses, rIFN et melphalan. Vingt neuf patients d'âge moyen de 60 ans (extrêmes 22–82 ans) ont été inclus dans cette étude après avoir donné leur consentement éclairé. Ils ont reçu un total de 31 perfusions de la tripe association. Il y avait 24 femmes et 5 hommes ayant des métastases multiples extensives des membres inférieurs (stade III a ou II ab). rTNFα a été administré à une dose unique de 4 mg injectée en bolus par voie artérielle, dans des conditions d'hyperthermie modérée (40 à 40.5°C) pendant 90 minutes. rTNFα a été donné en souscutanée aux jours −2 et −1 mélangé à la perfusion de rTNFα à la dose de 0.2 mg. Le melphalan a été administré à la concentration de 40 mg/ml. Pour éviter un syndrome de choc rencontré chez deux patients traités hors protocole pour sarcome et carcinome, tous les patients de ce protocole ont reçu de la dopamine en perfusion continue à la dose de 3 µg/kg/mn depuis le début de la perfusion et pendant 48 heures, et n'ont eu qu'une hypotension modérée avec des frissons transitoires. La toxicité attribuée au rTNFα était minime. On a eu 16 cas de toxicité hématologique comprenant une neutropénie (11 cas, 1 grade 4, 1 grade 3) et neutropénie avec thrombopénie (12 cas, 1 grade 4, 4 grade 2). Dix huit patients avaient déjà été traités par Melphalane en perfusion isolée (13/39) ou en association avec du cisplatinium (2/29) ou par l'association rTNFα-melphalan (1/29) ou le rTNFα seul (2/29). Le suivi moyen était de 41 semaines. Sur les 29 patients évalués, il y a eu 26 rémissions complètes (RC) (90%), 3 rémissions partielles (RP) (10%) et ancun décès. Les survies actuarielles sans maladie et globale à 12 mois sont respectivement de 63 et de 73%. Dans tous les cas, les nodules se sont assouplis en moins de 3 jours après le début de la perfusion. Le délai de réponse au traitement variait entre 6 et 22 jours. L'analyse intermédiaire de l'étude de phase II suggère que de fortes doses de rTNFα peuvent être administrées avec une faible toxicité en perfusion associées à la dopamine et à une hyperhydratation. La réponse tumorale était évidente chez tous les patients avec une CR de 90%. De plus, l'association de rTNFα, IFN et melphalan semble donner une grande efficacité avec une toxicité minime, même en cas d'échec antérieur avec le melphalan utilisé seul.
Resumen
Se diseñó un protocolo que utiliza la perfusión aislada de las extremidades con hipertermia a fin de incrementar la eficacia terapéutica del factor necrotizante tumoral alfa recombinante (rFNTα) y reducir sus efectos secundarios sistémicos, en el tratamiento de metástasis en tránsito del melanoma. Se escogió una combinación triple de alta dosis de rFNTα + interferóngamma recombinante (rIFN-γ) + melfalán en virtud del efecto sinergístico antitumoral del rTNFα con el IFN-γ y del rTNFα con los agentes alquilantes informados en la literatura. Veintinueve pacientes con edad promedio de 60 años (rango 22–82) ingresaron al estudio bajo consentimiento informado y recibieron un total de 31 perfusiones aisladas con la triple combinación. Hubo 24 mujeres y 5 hombres con metástasis en tránsito de melanoma de la extremidad inferior (estado IIa o IIIab). El rTNFα en la dosis única de 4 mg fue inyectado en bolo en la línea arterial, bajo condiciones levemente hipertermicas (40 a 50°C) por 90 minutos. El rIFN-γ fue administrado en los días −2 y −1 en el líquido perfusión, con rTNFα en la dosis de 0.2 mg. El melfalán fue administrado en el líquido de perfusión en una dosis para proveer una concentración de 40 µg/ml.
En todos los casos de perfusión aislada en el protocolo de triple combinación, y con el objeto de prevenir un cuadro del tripo de “shock-syndrome” que había sido observado en 2 pacientes tratados por sarcoma y carcinoma por fuera de este protocolo, se administró dopamina en infusión continua a una rata de 3 µg/kg/min desde el comienzo de la pefusión aislada y, por 48 horas; los pacientes sólo exhibieron hipotensión leve y escalofríos y fiebre transitorios. La toxicidad regional atribuible as rTNFα fue mínima. Se han presentado 16 casos con toxicidad hematológica consistente en nuetropenia (11 casos, uno grado 4 y uno grado 3) y neutropenia con trombocitopenia (12 casos, uno grado 4 y cuatro grado 2). Dieciocho de 29 pacientes habían sido previamente tratados con melfalán en perfusión aislada (13/29) o con cisplatino (2/29), rTNFα-melfalán (1/29) or rTNFα solamente (2/29). El promedio del sequimiento fue 41 semanas. Los 29 pacientes son valorables: ha habido 26 remisiones completas (90%), 3 remisiones parciales (10%) y ninguna falla. Las tasas de sobrevida actuarial libre de enfermedad y de sobrevida total han sido 63% y 73%, respectivamente, a 12 meses. En la totalidad de los casos apareció evidente el ablandamiento de los nódulos en los primeros 21 días después de la perfusión aislada y el intervalo hasta la respuesta difinitiva varió entre el día 6 y el día 22.
El análisis interim de un estudio de fase II sugiere que la alta dosis de rTNFα puede ser administrada con aceptable toxicidad por perfusión aislada con dopamina e hiperhidratación. Las respuestas tumorales pueden ser evidenciadas en la totalidad de los pacientes, con 90% de remisión completa. Además, la combinación de rTNFα, rIFN-γ y melfalán parece ser de elevada eficacia con toxicidad mínima, aún después de una falla terapéutica con melfalán sólo.
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References
Balkwill, F., Lee, A., Aldam, G., Moodie, E., Thomas, J.A., Tavernier, J., Fiers, W.: Human tumor xenografts treated with human TNF alone or in combination with IF. Cancer Res.46:3990, 1986
Balkwill, F., Ward, B.G., Moodie, E., Fiers W.: Therapeutic potential of tumour necrosis factor alpha and gamma interferon in experimental human ovarian cancer. Cancer Res.47:4755, 1987
Tracey, K., Beutler, B., Lowry, S., Merryweather, J., Wolpe, S., Milsark, I., Hariri, R., Fahey, T., Zentella, A., Albert, J., Shires, T., Cerami, A.: Shock and tissue injury induced by recombinant human cachectin. Science234:470, 1986
Tracey, K., Fong, Y., Hesse, D., Manogue, K.R., Lee, A.T., Duo, G.C., Lowry, S.F., Cerami, A.: Anti-cachectin/TNF antibodies prevent septic shock during lethal bacteremia. Nature330:662, 1987
Abbruzzese, J., Levin, B., Ajani, J., Faintuch, J.S., Saks, S., Patt, Y.Z., Edwards, C., Ende, KI, Gutterman, J.U.: Phase I trial of recombinant human gamma-interferon and recombinant human tumor necrosis factor in patients with advanced gastrointestinal cancer. Cancer Res.49:4057, 1989
Pfreundschuh, M., Steinmetz, H., Tüschen, R., Schenk, V., Diehl, V., Schaadt, M.: Phase I study of intratumoral application of recombinant human tumor recrosis factor. Eur. J. Cancer Clin. Oncol.25:379, 1989
Retsas, S., Leslie, M., Bottomiley, D.: Intralesional tumor necrosis factor combined with interferon gamma in metastatic melanoma. Br. Med. J.298:1290, 1989
Creaven, P., Brenner, D., Cowens, J., Huben, R.P., Wolf, R.M., Takita, H., Arbruck, S.G., Razack, M.S., Proefrock, A.D.: A phase I clinical trial of recombinant human tumor necrosis factor given daily for five days. Cancer Chemother. Pharmacol.23:186, 1989
Bartsch, H., Pfizenmaeier, K., Schroeder, M., Nagel, G.A.: Intralesional application of recombinant human tumor necrosis factor alpha induces local tumor regression in patients with advanced malignancies. Eur. J. Cancer Clin. Oncol.25:287, 1989
Carswell, E.A., Old, L.J., Kassel, R.L., Green, S., Fiore, N., Williamson, B.: An endotoxin-induced serum factor that causes necrosis of tumors. Proc. Natl. Acad. Sci.72:3666, 1975
Morton, D.L., Eilber, F.R., Joseph, W.L., Wood, W.C., Trahan, E., Ketcham, A.S.: Immunological factors in human sarcomas and melanomas: A rational basis for immunotherapy. Ann. Surg.172:740, 1970
Palladino, M.A., Shalaby, M.R., Kramer, S.M., Ferraiolo, B., Baughman, R., DeLeo, A., Crase, D., Marafino, B., Aggarwal, B., Figari, I., Liggitt, D., Patton, J.: Characterization of the antitumor activities of human tumor necrosis factor-α and the comparison with other cytokines: Induction of tumor-specific immunity. J. Immunol.138:4023, 1987
Old, L.J.: General discussion II. In Tumour Necrosis Factor and Related Cytokines, Ciba Foundation Symposium 131, Chichester, John Wiley & Sons, 1987, pp. 185–191
Henson, P.M., Johnston, R.B. Jr.: Tissue injury inflammation: Oxidants proteinases, and cationic proteins. J. Clin. Invest.79:669, 1986
Smedly, L.A., Tonnesen, M.G., Sandhaus, R.A., Haslett, C., Guthrie, L.A., Johnston, R.B., Henson, P.M., Worthen, G.S.: Neutrophil-mediated injury to endothelial cells: Enhancement by endotoxin and essential role of neutrophil elastase. J. Clin. Invest. 77:1233, 1986
Aggarwal, B.B., Eessalu, T.E., Hass, P.E.: Characterization of receptors for human tumor necrosis factor and their regulation by gamma-interferon. Nature318:665, 1985
Ruggiero, V., Tavernier, J., Fiers, W., Baglioni, C.: Induction of the synthesis of tumor necrosis factor receptors by interferongamma. J. Immunol.136:2445, 1986
Fiers, W., Brouckaert, P., Guisez, Y.: Recombinant interferon gamma and its synergism with tumor necrosis factor in the human and mouse systems. In The Biology of the Interferon System, H. Schellekens, W.E. Stewart, editors, Amsterdam, Elsevier Science, 1986, pp. 241–248
Sohmura, Y.: Antitumor effect of recombinant human tumor necrosis factor alpha and its augmentation in vitro and in vivo. In Tumor Necrosis Factor/Cachectin and Related Cytokines, B. Bonavida, G.E. Gifford, H. Kirchner, L.J. Old, editors, Basel, Karger, 1988, pp. 189–195
Soehnlen, B., Liu, R., Salmon, S.: Recombinant TNF exhibit antitumor activity against clonogenic human tumor cells and synergism with gamma interferon. Proc. Am. Ass. Cancer Res.26:303, 1985
Watanabe, N., Niitsu, Y., Umeno, H., Sone, H., Neda, H., Yamauchi, N., Maeda, M., Urushizaki, I.: Synergistic cytotoxic and antitumor effects of recombinant human tumor necrosis factor and hyperthermia. Cancer Res.48:650, 1988
Niitsu, Y., Watanabe, N., Umeno, H., Sone, H., Neda, H., Yamauchi, N., Maeda, M., Urushizaki, I.: Synergistic effects of recombinant human tumor necrosis factor and hyperthermia on in vitro cytoxicity and artificial metastasis. Cancer Res.48:654, 1988
Mutch, D.G., Powell, C.B., Kao, M.S., Collins, J.L.: In vitro analysis of the anticancer potential of tumor necrosis factor in combination with cisplatin. Gynecol. Onc.34:328, 1989
Regenass, U., Müller, M., Curschellas, E., Matter, A.: Anti-tumor effects of tumor necrosis factor in combination with chemotherapeutic agents. Int. J. Cancer39:266, 1987
Krementz, E.T., Ryan, R.F., Carter, R.D., Sutherland, C.M., Reed, R.J.: Hyperthermic regional perfusion for melanoma of the limbs. In Cutaneous Melanoma: Clinical Management and Treatment Results Worldwide, C.M. Balch, G.W. Milton, editors, Philadelphia, J.B. Lippincott, 1985, pp. 171–195
Schraffordt Koops, H., Kroon, B.B.R., Lejeune, F.J.: Isolated regional perfusion in the treatment of local recurrence, satellites and in transit metastases of extremity melanomas. In Therapy of Advanced Malignant Melanom, Vol. 10, Pigment Cell Series, P. Rümke, editor, Basel, Karger, 1990, pp. 67–78
Lejeune, F.J.: Is isolation perfusion with chemotherapy an improvement in the management of malignant melanoma. In Oncologisch Kabinet, Amsterdam, 1984, pp. 71–78
Honess, D.J., Bleehen, N.M.: Heat potentiation of melphalan: Studies on melphalan transport systems. In Hyperthermic Oncology, Vol. 1, J. Overgaard, editor, London, Taylor Francis, 1984, pp. 441–448
Lejeune, F.J., Ghanem, G.: A simple and accurate new method for cytostatics dosimetry in isolation perfusion of the limbs based on exchangeable blood volume determination. Cancer Res.47:639, 1987
Liénard, D., Lejeune, F.J., Ewalenko, P., Delmotte, J-J.: Isolation perfusion (IP) with high dose tumour necrosis factor (rTNFα) and chemotherapy for melanoma. In Cytokines: Basic Principles and Clinical Applications, S. Romagnani, A.K. Abbas, editors, New York, Raven Press, 1990, pp. 87–89
Wieberdink, J., Benckhuizen, C., Braat, R.P., Van Slooten, E.A., Olthuis, G.A.A.: Dosimetry in isolation perfusion of the limbs by assessment of perfused tissue volume and grading of toxic tissue reactions. Eur. J. Cancer Clin. Oncol.18:905, 1982
Hoogstraten, B.: Reporting treatment results in solid tumors. In Cancer Clinical Trials, Methods and Practice, M.E. Buyse, M.J. Staquet, R.J. Sylvester, editors, Oxford, Oxford University Press, 1988, pp. 139–156
Lejeune, F.J., Ghanem, G., Liénard, D., Ewalenko, P.: Assessment of the haematocrit method for dosimetry of cytostatics in isolation perfusion. Reg. Cancer Treat.2:82, 1989
Lejeune, F.J., Liénard, D., El Douaihy, M., Vadoud Seyedi, J., Ewalenko, P.: Results of 206 isolated limb perfusions for malignant melanoma. Eur. J. Surg. Oncol.15:510, 1989
Lejeune, F.J., Deloof, T., Ewalenko, P., Frühling, J., Jabri, M., Mathieu, M., Nogaret, J-M, Verhest, A.: Objective regression of unexcised melanoma in transit metastases after hyperthermic isolation perfusion of the limbs with melphalan. In Recent Results in Cancer Research, Vol. 86, K. Schwemmle, K. Aigner, editors, Berlin-Heidelberg, Springer Verlag, 1983, pp. 268–276
Robertson, P.A., Ross, H.J., Figlin, R.A.: Tumor necrosis factor induces hemorrhagic necrosis of a sarcoma. Ann. Intern. Med.111:682, 1989
Springgs, D.R., Sherman, M.L., Frei III, E., Kufe, D.W.: Clinical studies with tumour necrosis factor. In Tumour Necrosis Factor and Related Cytokines, Ciba Foundation Symposium 131, Chichester, John Wiley & Sons, 1987, pp. 206–227
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Liénard, D., Lejeune, F.J. & Ewalenko, P. In transit metastases of malignant melanoma treated by high dose rTNFα in combination with interferon-γ and melphalan in isolation perfusion. World J. Surg. 16, 234–240 (1992). https://doi.org/10.1007/BF02071526
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DOI: https://doi.org/10.1007/BF02071526