ABSTRACT
Introducción: La carmustina es un agente antineoplásico alquilante utilizado en el tratamiento de mielomas, linfomas y otros tipos de cáncer. La cardiotoxicidad por carmustina es una reacción adversa muy rara, por lo que debe ser identificada oportunamente para prevenir desenlaces fatales. Reporte de caso: Se presenta un caso inusual de una paciente con cardiotoxicidad aguda grave reversible posterior a la administración endovenosa de carmustina. Al suspenderla exposición a este producto e iniciar tratamiento sintomatológico, la paciente se recupera satisfactoriamente sin nueva manifestación cardiaca. El caso fue notificado como reacción adversa medicamentosa y al evaluarse la causalidad entre la cardiotoxicidad y la carmustina, resultó probable (puntaje final =7). Conclusiones: El presente caso puede ser considerado una señal en farmacovigilancia, por lo que, los clínicos deben ser conscientes del riesgo potencial de cardiotoxicidad en pacientes expuestos a carmustina. Se recomienda realizar farmacovigilancia activa a los fármacos oncológicos.
Background: Carmustine is an alkylating agent used in the treatment of myeloma, lymphomas and other cancers. Cardiotoxicity due to carmustine is a rare adverse reaction that must be identified early to prevent fatal outcomes. Report case: We present an unusual case of acute cardiac toxicity related to the intravenous administration of carmustine. After stopping the carmustine, patient received symptomatic treatment and, finally was fully recovered. The case was reported as adverse drug reaction and we performed a pharmacovigilance causality assessment between carmustine and cardiotoxicity, resulting in probable (final score = 7). Conclusions: This case might be considered as a signal in pharmacovigilance. Clinicians should be aware of the potential risk of cardiotoxicity in patients exposed to carmustine. It is recommended to implement active pharmacovigilance to chemotherapy.
ABSTRACT
Background: Despite several therapeutic options available for bladder cancer, the outcomes are less satisfactory. To find a more effective modality, we were interested in the bioactive mushroom extract, PDF, which has been shown to sensitize certain anticancer drugs. Accordingly, we investigated if cytotoxic effects of several anticancer drugs used on bladder cancer patients could be enhanced with PDF in vitro.Methods: Human bladder cancer T24 cells were treated with four anticancer drugs, carmustine (BCNU), 5-fluorouracil (5FU), cisplatin (CPL), and doxorubicin (DOX) alone, their combinations, or in combination with PDF, and cell viability was determined. To explore the anticancer mechanism, the status of glyoxalase I (Gly-I), an enzyme involved in the drug resistance of cancer cells, and oxidative stress that can cause severe cellular injury/damage was also assessed.Results: BCNU and 5FU alone resulted in a >50% reduction in cell viability but CPL and DOX had no such effects. Only a combination of BCNU and PDF led to a drastic (~90%) cell viability reduction, accompanied by inactivation of Gly-I and an increase in oxidative stress. However, any combinations of other drugs and PDF had little effects on cell viability, Gly-I activity, or severity of oxidative stress.Conclusions: This study shows that anticancer activity of BCNU is significantly potentiated with PDF in T24 cells. This is rather attributed to inactivated Gly-I and increased oxidative stress. Therefore, PDF appears to have a chemosensitizing effect capable of enhancing BCNU cytotoxicity, which may offer an alternative, improved therapeutic option for bladder cancer.
ABSTRACT
RESUMEN Se expone el caso de una mujer de 19 años a quien se le realizó el diagnóstico de un xantoastrocitoma pleomórfico anaplásico parietooccipital izquierdo, neoplasia poco frecuente que suele presentarse en la población pediátrica y en los adultos jóvenes. Dicho tumor debuta generalmente con crisis convulsivas y sus características histológicas patognomónicas son el pleomorfismo celular, la vacuolización lipídica de su citoplasma y la reactividad a la proteína ácida fibrilar glial (PAFG) y S100. El estudio de nuevos marcadores que puedan brindar otras oportunidades terapéuticas ha permitido encontrar mutaciones en el oncogén BRAF. Este tumor presenta una variante anaplásica más agresiva que se trata con cirugía y quimiorradiación. En nuestro caso, después de varias progresiones a otras intervenciones, se utilizó bevacizumab y carmustine como tratamiento de segunda línea con respuesta completa.
SUMMARY The case of a young woman of 19-years-old is presented; whom the diagnosis was made of a left parietal-occipital xanthoastrocytoma pleomorphic anaplastic; this neoplasia is rare and usually affects the pediatric and young adult population. This generally debuts with seizures and their pathognomonic histologic characteristics are the pleomorphic cells with cytoplasmatic lipid vacuolation and the reactivity of glial fibrillary acidic protein (GFAP) and S100. The study of new markers that may provide other therapeutic opportunities has allowed finding mutations in the BRAF oncogene. This tumor has a more aggressive anaplastic variant that is treated with surgery and chemoradation. In our case after several progressions to other interventions, we used bevacizumab and carmustine as second-line treatment obtaining complete response.
Subject(s)
Radiotherapy , Carmustine , Bevacizumab , Glioma , Antineoplastic AgentsABSTRACT
A aterosclerose é uma doença inflamatória crônica e proliferativa que tem início quando fatores de risco alteram o endotélio vascular. As partículas da nanoemulsão lipídica LDE concentram-se em sítios inflamatórios e de intensa proliferação celular, como acontece nas lesões ateroscleróticas. A carmustina, um fármaco antiproliferativo usado na quimioterapia do câncer, não foi ainda explorada no tratamento da aterosclerose. Em trabalhos anteriores, mostrou-se que a associação com a LDE reduz drasticamente a toxicidade da carmustina, o que já foi demonstrado em pacientes com câncer avançado. O propósito do estudo é avaliar se a carmustina associada à LDE pode promover o efeito antiproliferativo nas lesões ateroscleróticas induzidas em coelhos. No presente trabalho, dezoito coelhos machos da raça New Zealand, receberam dieta rica em colesterol a 1% durante 8 semanas. Depois de 4 semanas foram divididos em dois grupos: grupo controle, que recebeu injeção endovenosa contendo apenas solução salina e grupo tratado, que recebeu LDE-carmustina na dose de 4mg/Kg semanalmente durante 4 semanas. Foram avaliados perfil hematológico, lipídico, bioquímico, ponderal e o consumo de ração. Após a eutanásia, foram medidas as lesões ateroscleróticas macroscópicas. Em seguida, o arco aórtico foi analisado por morfometria e por imunohistoquímica. Observou-se que não houve diferença no perfil ponderal e no consumo de ração entre os grupos de estudo. Não houve toxicidade hematológica, hepática e renal no grupo tratado. No perfil lipídico, ao final do estudo, as concentrações de colesterol total, não HDL-C e triglicerídeos aumentaram em todos os grupos. Portanto, o tratamento com LDE-carmustina inibiu as lesões ateroscleróticas em aproximadamente 90%, comparado ao grupo controle. LDE-carmustina também reduziu a presença de macrófagos, de células de músculo liso e das células reguladoras de linfócitos T na íntima arterial, bem como a expressão protéica de MMP9,...
Atherosclerosis is a chronic inflammatory and proliferative disease that starts when risk factors alter vascular endothelium. The particles of the lipid nanoemulsion LDE concentrate on inflammatory sites and with intense cell proliferation, as occurs in atherosclerotic lesions. The carmustine, an antiproliferative drug used in cancer chemotherapy has not yet been explored for the treatment of atherosclerosis. In previous work, we showed that the association with LDE drastically reduces toxicity of carmustine, which has been demonstrated in patients with advanced cancer. The purpose of this study is to evaluate whether carmustine associated with LDE can promote antiproliferative effect on atherosclerotic lesions induced in rabbits. In this study, eighteen male New Zealand rabbits were given a diet rich in cholesterol 1% for 8 weeks. After 4 weeks they were divided into two groups: control group, which received an intravenous injection containing only saline and treated group receiving LDE-carmustine dose of 4 mg/kg weekly for 4 weeks. Hematology, lipid, biochemical, weight profile and feed intake were evaluated. After euthanasia, macroscopic atherosclerotic lesions were measured. Then, the aortic arch was analyzed by morphology and by immunohistochemistry. It was observed that there was no difference in weight and profile in feed intake between the study groups. There were not hematological, hepatic and renal toxicity in the treated group. Lipid profile at the end of the study, the concentrations of total cholesterol, non-HDL-C and triglycerides increased in all groups. Therefore, treatment with LDE-carmustine inhibit atherosclerotic lesions in approximately 90%, compared to the control group. LDE-carmustine also reduced the presence of macrophages, smooth muscle cells and regulatory T cells in the arterial intima as well as the protein expression of MMP9, inflammatory cytokines and lipoprotein receptors. Treatment of rabbits with induced...
Subject(s)
Animals , Rabbits , Atherosclerosis , Carmustine , Hypercholesterolemia , Inflammation , NanoparticlesABSTRACT
Glioblastoma is a rapidly progressive and extremely fatal form of brain tumor with poor prognosis. It is the most common type of primary brain tumor. Even with the most aggressive conventional treatment that comprises surgery followed by radiotherapy and chemotherapy, most patients die within a year of diagnosis. Developments in molecular and cell biology have led to better understanding of tumor development, leading to novel treatment strategies including biological therapy and immunotherapy to combat the deadly disease. Targeted drug delivery strategies to circumvent the blood-brain barrier have shown efficiency in clinical trials. Gliadel wafer is a new approach to the treatment of glioblastoma, which involves controlled release delivery of carmustine from biodegradable polymer wafers. It has shown promising results and provides a silver lining for glioblastoma patients.
Subject(s)
Antineoplastic Agents, Alkylating/therapeutic use , Brain Neoplasms/drug therapy , Carmustine/therapeutic use , Delayed-Action Preparations , HumansABSTRACT
Contemporary therapies for patients with glioblastomas remain marginally efficient, and recurrence following surgery, radiation therapy and adjuvant chemotherapy is practically universal. The major obstacles to the successful use of chemotherapy for CNS tumors are the drug delivery to the tumor site and the infusion of chemotherapeutic agents directly into the arterial supply of a tumor. The latter could provide a pharmacokinetic advantage by enhancing drug delivery to the tumor. Sixteen patients with recurrent unilateral glioblastomas treated with intra-arterial BCNU were evaluated retrospectively. During the infusion, eleven patients referred pain in the ipsilateral eye, five patients were nauseated, three reported headache, one patient presented mental confusion, while two presented focal signs. There were two deaths during the course of therapy. Four patients achieved temporary clinical improvement, seven showed disease stability, and three presented clinical deterioration. The median total survival time was 87.9 weeks. Unilateral vision loss and focal signs were observed as delayed complications of this treatment. This study has confirmed previous reports indicating that arterial chemotherapy is clearly not curative, and presents serious toxicity. Only through a randomized prospective study performed in a large series of patients can the questions concerning survival period increment be answered properly.
Os tratamentos atuais para pacientes com glioblastoma permanecem pouco eficientes e a recorrência, acompanhando cirurgia, radioterapia e quimioterapia, é a regra geral. O maior obstáculo para o sucesso da quimioterapia para os tumores do SNC é a disponibilização da droga no sitio do tumor sendo que a infusão do agente quimioterápico diretamente na trama arterial da lesão pode proporcionar vantagens por maior liberação da substância diretamente no tumor. Estudamos retrospectivamente dezesseis pacientes com glioblastomas recorrentes, unilaterais, que foram tratados com BCNU intra-arterial; durante a infusão, onze pacientes sentiram dor no olho ipsilateral, cinco ficaram nauseados, três queixaram-se de cefaléia, um apresentou confusão mental e dois apresentaram sinais focais. Ocorreram duas mortes durante a terapia. Quatro pacientes apresentaram melhora clinica temporária, sete apresentaram estabilização e três apresentaram deterioração. A média de sobrevida total foi de 87,9 semanas. Perda da visão unilateral e sinais focais foram complicações tardias. Este estudo confirmou trabalhos anteriores indicando que a quimioterapia intra-arterial claramente não é curativa, séria toxicidade pode ocorrer e somente um estudo prospectivo e randomizado, realizado em uma serie maior de pacientes, poderá responder questões sobre o aumento do tempo de sobrevida de forma adequada.
Subject(s)
Aged , Female , Humans , Male , Middle Aged , Antineoplastic Agents, Alkylating/administration & dosage , Brain Neoplasms/therapy , Carmustine/administration & dosage , Glioblastoma/therapy , Neoplasm Recurrence, Local/drug therapy , Brain Neoplasms/mortality , Glioblastoma/mortality , Injections, Intra-Arterial , Neoplasm Recurrence, Local/mortality , Retrospective Studies , Survival AnalysisABSTRACT
Objective: To compare the inhibitory effect of carmustine(BCNU) and bleomycin on craniopharyngiomas in vitro. Methods: Cells were successfully cultured in vitro from the fresh specimens, then the culture medium with bleomycin or BCNU at different concentration was added. The tumor inhibitory curve-line was drawn based on the cell number at different time points. After cultured for 144 h, ATP-luminescence assay was applied to test the antitumor effect. Results: The cell number decreased rapidly when the medium was added. The decreasing speed was faster in BCNU medium than that in bleomycin medium at the same concentration. The bleomycin medium showed no significant inhibitory effect except for the one at 1.00 g/L. However, regardless of the concentration, BCNU medium inhibited the cells effectively. Conclusion: BCNU has stronger inhibitory effect on craniopharyngiomas cells than bleomycin, it can be used to treat this tumor
ABSTRACT
We describe a case of mycosis fungoides (infiltrative plaque type) in an 86-year-old male. He had experienced dark erythematous round plaques on the face, trunk, buttock, upper and lower extremities. Histopathologic findings revealed band-like superficial dermal infiltration of atypical lymphocytes, epidermotropism, and Pautrier's microabscess in the epidermis. The infiltrative cells were positivly stained with CD3, but not with a CD20. He was treated with a topical application of 0.2% carmustine, but he died due to poor general condition and septicemia.