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<td align="center" width="513"><b class="font3">Irinotecan©MCisplatin显¥Ü对¤p¤I脑胶质½F¦³§Ö³t¤Ï应</b></td>
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<p>¦è¯Z¤ú¤Ú¶ë¶©纳Sant Joan de Deu医°|ªº¤p¤I肿½F¬ì¥D¥ôJaume Mora医师ªí¥Ü¡A¤@个¦è¯Z¤úªº¬ã¨s团队¨Ö¥Îcisplatin©Mirinotecan¡A获±o¥Ø«e对¤p¤I脑胶质½F(brain gliomas)³Ì¦nªº¤Ï应¡F¦b18个恶¤Æ¯fµ£¤¤¡A14 ¦ì(77%)¦bªv疗¦Z显¥Ü肿½F缩¤p¡A这¬O¦¹¤@¯f±w类«¬¤¤ÌåªN¥Xªº¤Ï应¡C <br>
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¡@¡@Mora医师¤W¶g¦b¤Ú¶ë¶©纳举¦æªº²Ä14届欧¬wÀù¯g¬ã讨会(ECCO 14)¤¤发ªí这¨Ç结ªG¡F¦b该项¬ã¨sªº记ªÌ会¤¤¡AECCO总µô¡B²ü兰Erasmus¤j学ªºAlexander Eggermont医师ªí¥Ü¡A¦b¥H«e¥¼´¿发现过这Ïú结ªG¡A这¬Oªì¨B观¹î¡A¦ý18个¯f±w¤w经¨¬¥H证©ú¦¹¤@·s论点¦³®Ä¡A§Ú们还¥¼§ï变临§É实务 ¡A¦ý§Ú们¥²须继续±´¯Á¦¹¤@·sªv疗¤è¦¡¡C<br>
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¡@¡@Mora医师¸Ñ释¡A¦b过¥h¡A脑胶质½Fªº¥Dnªv疗¤è¦¡¬O©ñ®g线ªv疗¡A¤â术¦}«D实际选项¡A¦]¬°肿½F³q±`¦ì©ó«Â胁¥Í©Rªº¸ÑåÌÛ³y内¡A¦ÓºË·Ç脑³¡ªº©ñ®g线ªv疗会¦³长´Áªº¦Z遗¯g¡A¦]¦¹´Â¦V¬ã发对这¨Ç¯f±w¤Æ疗¡A¤£过¡A这类试验¤j¦h数³£¥¢败¤F¡A¤j³¡¤Àªº医学¤¤¤ß继续¨Ï¥Î©ñ®g线ªv疗°ªµ¥级ªº胶质½F(high-grade gliomas)¡A对©ó§Cµ¥级ªº胶质½F(low-grade gliomas)¡A¥u¦³¤Ö数¨Ö¥Î处¤è¦³显µÛ®ÄªG¡A¥Ø«e©Ò¥Îªº¬O¬ü国§ù§J¤j学发ªíªºvincristine ©Mcarboplatin¡A¥t¥~¦³¤@个义¤j§Qªº¬ã¨s团队«ü¥Xcisplatin ©MVP-16对§Cµ¥级ªº胶质½F¦³¦nªº结ªG¡C<br>
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¡@¡@Mora医师¦bECCO 14¤¤©Ò报§iªº结ªG¡A来¦Û¤@项¥Îirinotecan©Mcisplatin©ó18¦ì恶¤Æ¬P状细M½F(astrocytoma)¯fµ£ªº²Ä¤G´Á试验¡A这¨Ç¯f±w¤¤¡A6¦ì¯fµ£¦³¯á¯Á肿½F¡G2¦ì¦³§¹¾ã¤Ï应(CR)¡A4 ¦ì¦³³¡¤À¤Ï应(PR)¡F4¦ì¤p«Ä¦³¤j脑¤Ñ¹õ¤W(supratentorial)肿½F¡A¨ä¤¤2¦ì¬OPR¡B2¦ì¯f±¡稳©w(SD)¡F¥t¥~2¦ì¯fµ£¬O¤p脑肿½F(cerebellar tumors)¡A¨ä¤¤¤@¦ìCR¡B¥t¦ì¤@¦ì¬OPR¡C<br>
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¡@¡@³Ñ¤Uªº6¦ì¯f±w¦³脑¤z胶质½F(brain stem gliomas)¡A¨ä¤¤4¦ì属©ó°ªµ¥级(2¦ì扩´²¡B2 ¦ì¥¼扩´²)¡A¥t¥~2¦ì¬O§Cµ¥级ªº¤¤脑肿½F(mid-brain tumors)¡FMora医师ªí¥Ü¡A脑¤z胶质½F¤Ö见¡A¦ý¬O³Ì±`发¥Í©ó6¨ì10岁¤p«ÄªºÀù¯g¡A¦s¬¡²v¤£¨Î¡A°ªµ¥级脑¤z胶质½F©¹©¹会P©R¡A¦Ó§Cµ¥级胶质½Fªº¯f±w³q±`¥i©µ长¦s¬¡¡F¦¹试验¤¤¡A给¤©°ªµ¥级肿½Fªº¤p«Ä§Ü¦åºÞ·s¥Íªv疗药bevacizumab¥H¤Î©ñ®g线ªv疗¡A¥t¥~¥[¤Wirinotecan©Mcisplatin¡C <br>
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<p>Irinotecan and Cisplatin Show Rapid Response in Child Brain Gliomas <br>
<br>
The best responses seen to date in childhood brain gliomas have been reported by a Spanish group using a combination of cisplatin with irinotecan. Of 18 children with progressive disease, 14 (77%) showed a decrease in tumor size after treatment, which is an \"outstanding\" response in this patient group, says Jaume Mora, MD, PhD, head of pediatric oncology, Hospital Sant Joan de Deu, in Barcelona, Spain. <br>
<br>
<br>
Dr. Mora presented these results last week at the 14th European Cancer Conference (ECCO 14), in Barcelona. At a press conference at which the work was highlighted, Alexander Eggermont, MD, PhD, from Erasmus University, in Rotterdam, the Netherlands, and incoming ECCO president, said: \"This has never been seen before. It\'s an early observation, but 18 patients is a big enough group to make a statement that this is truly new and promising. We\'re not there yet in terms of changing clinical practice, but we should carry on exploring this new approach to treatment.\"<br>
<br>
Dr. Mora explained that, in the past, the main treatment for brain gliomas has been radiotherapy. Surgery is not really an option, because the tumors are often situated within life-threatening anatomical structures, but radiotherapy aimed at the brain has long-term adverse consequences, and so there has been a move toward exploring chemotherapy for these patients. \"However, most of these trials have failed,\" Dr. Mora commented, and most centers continue to use radiotherapy for high-grade gliomas. For low-grade gliomas, few combination regimens have shown significant changes in the natural history of the disease, but vincristine and carboplatin (pioneered in the United States at Duke University) are the current protocol, and an Italian group has reported good results in low-grade gliomas with cisplatin and VP-16, he said.<br>
<br>
The results that Dr. Mora reported at ECCO 14 came from a phase 2 trial of irinotecan and cisplatin in 18 children with progressing astrocytoma. Of these, 6 children had spinal cord tumors: 2 showed a complete response (CR), and 4 had a partial response (PR). Four children had supratentorial tumors, and 2 of these had a PR and 2 had stable disease (SD). Another 2 patients had cerebellar tumors, of which 1 had a CR and 1 had a PR. <br>
<br>
The remaining 6 patients had brain stem gliomas, 4 of which were high-grade (2 diffuse and 2 nondiffuse), and 2 had low-grade mid-brain tumors. Brain stem gliomas are rare, but they are among the commonest cancers to occur in children between 6 and 10 years old, Dr. Mora commented. Survival rates are poor, and high-grade brain stem gliomas are uniformly fatal, although children with low-grade gliomas have a more prolonged survival. In this trial, children with high-grade tumors were given the antiangiogenic therapy bevacizumab and radiotherapy in addition to irinotecan and cisplatin. <br>
<br>
All of the 6 children with brain stem gliomas showed a rapid clinical response to the irinotecan and cisplatin regimen. \"Remarkably, the irinotecan/cisplatin regimen achieved a reduction in tumor size greater than 20% in all the children at the end of therapy, including those with the worst brain stem gliomas, the intrinsic diffuse tumors. No chemotherapy has ever achieved this grade of early response in high-grade brain stem gliomas.\"<br>
<br>
However, between 9 and 12 months after the therapy, 3 of the high-grade tumors started to progress. <br>
<br>
\"This early response is promising, but the brain stem patients eventually progress regardless of the maintenance therapy we have given them. We need to rethink these results and find out how to better consolidate these initial responses,\" Dr. Mora said. <br>
<br>
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Irinotecan and Cisplatin Show Rapid Response in Child Brain Gliomas
The best responses seen to date in childhood brain gliomas have been reported by a Spanish group using a combination of cisplatin with irinotecan. Of 18 children with progressive disease, 14 (77%) showed a decrease in tumor size after treatment, which is an \"outstanding\" response in this patient group, says Jaume Mora, MD, PhD, head of pediatric oncology, Hospital Sant Joan de Deu, in Barcelona, Spain.
Dr. Mora presented these results last week at the 14th European Cancer Conference (ECCO 14), in Barcelona. At a press conference at which the work was highlighted, Alexander Eggermont, MD, PhD, from Erasmus University, in Rotterdam, the Netherlands, and incoming ECCO president, said: \"This has never been seen before. It\'s an early observation, but 18 patients is a big enough group to make a statement that this is truly new and promising. We\'re not there yet in terms of changing clinical practice, but we should carry on exploring this new approach to treatment.\"
Dr. Mora explained that, in the past, the main treatment for brain gliomas has been radiotherapy. Surgery is not really an option, because the tumors are often situated within life-threatening anatomical structures, but radiotherapy aimed at the brain has long-term adverse consequences, and so there has been a move toward exploring chemotherapy for these patients. \"However, most of these trials have failed,\" Dr. Mora commented, and most centers continue to use radiotherapy for high-grade gliomas. For low-grade gliomas, few combination regimens have shown significant changes in the natural history of the disease, but vincristine and carboplatin (pioneered in the United States at Duke University) are the current protocol, and an Italian group has reported good results in low-grade gliomas with cisplatin and VP-16, he said.
The results that Dr. Mora reported at ECCO 14 came from a phase 2 trial of irinotecan and cisplatin in 18 children with progressing astrocytoma. Of these, 6 children had spinal cord tumors: 2 showed a complete response (CR), and 4 had a partial response (PR). Four children had supratentorial tumors, and 2 of these had a PR and 2 had stable disease (SD). Another 2 patients had cerebellar tumors, of which 1 had a CR and 1 had a PR.
The remaining 6 patients had brain stem gliomas, 4 of which were high-grade (2 diffuse and 2 nondiffuse), and 2 had low-grade mid-brain tumors. Brain stem gliomas are rare, but they are among the commonest cancers to occur in children between 6 and 10 years old, Dr. Mora commented. Survival rates are poor, and high-grade brain stem gliomas are uniformly fatal, although children with low-grade gliomas have a more prolonged survival. In this trial, children with high-grade tumors were given the antiangiogenic therapy bevacizumab and radiotherapy in addition to irinotecan and cisplatin.
All of the 6 children with brain stem gliomas showed a rapid clinical response to the irinotecan and cisplatin regimen. \"Remarkably, the irinotecan/cisplatin regimen achieved a reduction in tumor size greater than 20% in all the children at the end of therapy, including those with the worst brain stem gliomas, the intrinsic diffuse tumors. No chemotherapy has ever achieved this grade of early response in high-grade brain stem gliomas.\"
However, between 9 and 12 months after the therapy, 3 of the high-grade tumors started to progress.
\"This early response is promising, but the brain stem patients eventually progress regardless of the maintenance therapy we have given them. We need to rethink these results and find out how to better consolidate these initial responses,\" Dr. Mora said.
14th European Cancer Conference: Abstract 1407. Presented September 25, 2007.
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