Conferences 2010

Conference Date Venue

ISET

ISET 2010

 17-21 Jan 2010 Hollywood, Florida US

ASCO gi

ASCO 2010

 22-24 Jan 2010 Orlando, Florida

SSO

SSO 2010

 3 - 7 March 2010 St. Louis, Missouri US

SIR

SIR 2010

 13-18 March 2010 Tampa, Florida

IHPBA

IHBA 2010

 18-22 April, 2010 Argentina, S Amer

ECIO

ECIO 2010

 21 - 24 April, 2010 Florence, Italy

GEST

GEST 2010

 6-9 May, 2010 San Fransisco, US

APCCVIR

APCCVIR 2010

 1-4 June, 2010 Seoul, Korea

ASCO

ASCO 2010

 4-8 June, 2010 Chicago, IL

WCIO

WCIO 2010

 9-12 June, 2010 Philadelphia, Pennsylvania

WCGIC

WCGIC 2010

 30 June- 3 July, 2010 Barcelona, Spain

ESIR

ESIR 2010

 12 - 16 July 2010 San Diego, CA

AUGIS

AUGIS 2010

 9-10 Sep, 2010 Oxford, UK

ILCA

ILCA 2010

 10-12 Sep, 2010 Montreal, Canada

CIRSE

CIRSE 2010

 2-6 Oct, 2010 Valencia, Spain

 

Regulatory notices and product safety data

Worldwide (excluding USA)

Bead Block™ is CE marked and indicated for the treatment of a variety of hypervascular tumours (including Uterine Fibroids) and arteriovenous malformations (AVMs). For full prescribing information please refer to Bead Block instructions for use.

DC Bead® is CE marked and is indicated for the treatment of malignant hypervascular tumours and loading with doxorubicin drug. DC Bead® is also indicated for loading with irinotecan for the treatment of metastatic colorectal cancer (mCRC). Both indications may not be available in your territory. For full prescribing information please refer to DC Bead instructions for use.

DC BeadM1™ is indicated for loading with irinotecan for the treatment of metastatic colorectal cancer (mCRC). For full prescribing information please refer to DC Bead M1 instructions for use.

USA

In the USA, Bead Block™ is indicated for the treatment of hypervascular tumors and arteriovenous malformations (AVMs). For full prescribing information please refer to Bead Block USA Instructions for use.

LC Bead™ is cleared by the FDA for the embolization of hypervascular tumors and arteriovenous malformations (AVMs). For full prescribing information please refer to LC Bead instructions for use.

LC Bead M1™ is cleared by the FDA for the embolization of hypervascular tumors and arteriovenous malformations (AVMs). For full prescribing information please refer to LC Bead M1 instructions for use.

DC Bead is not currently available for sale or distribution in the USA. Both indications may not be available in your territory. 

DC Bead M1 is not currently available for sale or distributions in the USA. 

Canada

DC Bead® with doxorubicin is indicated for trans-arterial chemoembolization (TACE) of unresectable hepatocellular carcinoma (HCC). DC Bead are also intended to be loaded with irinotecan for the purpose of embolization of vessels supplying malignant colorectal cancer metastasised to the liver (mCRC), and delivery of a local, controlled, sustained dose of irinotecan to the mCRC. For full prescribing information please refer to DC Bead Canada Instructions for Use 

DC BeadM1 is primarily intended as an embolic agent to treat vessels supplying malignant colorectal cancer metastasised to the liver (mCRC). DC BeadM1 is also compatible with irinotecan, which can be loaded prior to embolisation and then, as a secondary action, elute a local, controlled and sustained dose to the mCRC after embolisation. For full prescribing information please refer to DC BeadM1 Canada Instructions for Use  

Tawain

DC Bead is approved by the Department of Health and is intended to be loaded with Mayne (Hospira) doxorubicin HCI for the purpose of embolisation of vessels supplying malignant hypervascularised tumour(s), and delivery of a local, controlled, sustained dose of doxorubicin.  DC Bead is also indicated for the embolisation of nidus vessels without medication.  Approved size ranges in Taiwan are 300-500µm and 500-700µm.

Hong Kong

PRECISION Bead™ is indicated for the delivery of Doxorubicin, a chemotherapeutic agent for the treatment of malignant hypervascular tumours, where Trans Arterial Embolisation (TAE) is not contraindicated.