Download cripto-1 a possible new biomarker in glioblastoma multiforme

Survey
yes no Was this document useful for you?
   Thank you for your participation!

* Your assessment is very important for improving the workof artificial intelligence, which forms the content of this project

page
1
page
2
page
3
page
4
page
5
page
6
page
7
page
8
page
9
page
10
page
11
page
12
page
13
page
14
page
15
page
16
page
17
page
18
page
19
page
20
page
21
page
22
page
23
Document related concepts
no text concepts found
Transcript 
CRIPTO-1
A POSSIBLE NEW BIOMARKER IN
GLIOBLASTOMA MULTIFORME
PIA OLESEN, MD, PHD STUDENT
Glioblastoma
• WHO Grade IV Glioma
• Heterogenic
• Undiffenrentiated phenotype
• 50% of all Gliomas
• Around 600 patients each year in Denmark
• Incurable – despite multimodal treatment with both
agressive surgery (Stummer), chemotherapy and
radioation therapy (Stupp)
• Mean life expectancy of 12-14 months
Glioblastoma
• No knowledge about:
• Cause
• Risk behavior
• Prevention
• Focus on:
• Early diagnosis
• Treatment
Glioblastoma growth
• Spreads throughout the surrounding healthy brain tissue:
• Membrane extensions helps find and travel along white matter
tracts and endothelial lining
• Secreting metalloproteases breaks up the extracellular
components
• Normal brain structure provides the perfect
microenvironment facilitating migration of glioblastoma
cells
Cancer stem cells
• Cancer stem cells (CSC) – cancer initiating cells:
• Acute myeloid leukaemia:
• AML cells have limited proliferative capacity
• The leukaemia clone is maintained by a rare populations of stem
cells
•
Lapidot, T., et al., A cell initiating human acute myeloid leukaemia after transplantation into
SCID mice. Nature, 1994
• Breastcancer:
•
Al-Hajj, M., et al., Prospective identification of tumorigenic breast cancer cells. Proc Natl Acad Sci U S
A, 2003
CSC in Glioblastoma
• Have not yet been identified – numerous candidates
• CD133 (prominin-1, a cell membrane protein)
• Cell membrane growthfactor receptors
• What is being done to find these?
• Relate cell surface characteristics to functional characteristics
such as migration and tumoregenecity.
Or not
• Only a minority of cells have the ability to form tumors –
but CD133- can also do that
• Several markers are needed
• Analyzing premalignant stages to identify the cancer cell
of origin
Gameplan
Cure Glioblastoma
Gameplan
• A way to identify tumor initiating cells
• A way to sort these cells from the rest of the tumor cells
• Improve treatment
Why Cripto-1
• Because it is there
• Cripto-1 linked to increased proliferation and invasiveness in Glioma
•
Lee, C.C., et al., Nodal promotes growth and invasion in human gliomas. Oncogene, 2010.
• Upregulated in other cancers
•
•
Breast
Colon
• Poorer prognosis and aggressive clinical pathological
parameters:
•
•
•
Elevated depth of invasion
Positive lymph node involvement
metastasis
• Serological marker of malignancy and disease progression
• Targeted therapies showes promising results
Adkins, H.B., et al., Antibody blockade of the Cripto CFC domain suppresses tumor cell growth in vivo. J Clin Invest, 2003
Hypothesis
• The presence of Cripto-1 in Glioblastoma is part of the
underlying mechanism for the invasive growth pattern
and regrowth
• This makes Cripto-1 a possible diagnostic and predicitive
biomarker and a possible candidate for targeted therapy
Studyplan
• Localize and characterize Cripto-1 in Glioblastoma tissue
and in blood:
• Primary cell lines
• Cripto-1 levels
• Relate these levels to:
• Tumor volume
• Clinical status
• Histopathological staining
What is Cripto-1
•
•
•
•
Teratocarcinoma-derived growth factor-1
Glycoprotein
Very low concentrations in normal adult blood and tissue
A soluble ligand and a cellmembrane anchored protein
What is Cripto-1
• Important during embryogenesis:
• Formation of primitive streak
• Patterning anterior/posterior axis
• Establishing left/right symmetri
• Promotes EMT
• Poorly defined
regulatory
mechanisms
Setup
• Inclusion criteria:
• All patients with suspected Glioblastoma on MRI
• Verified by histopatholgical examination
• Blood and tissue
•
•
•
•
•
16 patients (now more than 40, including relapse)
Median age 57.4
Gender ratio 1:1
Protein concentrations in blood and tissue (ELISA)
Geneproduct in tissue – and primary cell lines (RT-PCR
and qPCR)
• Xenografts – tumorgenicity
Results
Primary cell lines
• Mechanical dissociation and enzymatic digestion. The remaining
nucleated cells are purified by centrifugation and filtration before
seeding.
• Grown in DMEM-F12 with FCS and AB
• Spherecultures without FCS
RT-PCR
A.
Cripto-1 RT-PCR product in GBM tumor
samples depicted on an agarose gel.
A blank control and the embryonic cell line
CLS2 was included as negative and
positive controls respectively.
Expression of the housekeeping gene
GAPDH was used as reference.
Protein
B.
Western Blot: Cripto-1 protein in GBM
tissue was detected.
U87 served as positive control, and a
secondary antibody as negative control.
15-20kDa (not shown)
C.
Cripto-1 protein in GBM tumor samples
(n=12), in blood (n=17) and in control
plasma samples (n=8)
Significantly higher (p<0.05)
Cripto-1 Concentration
in blood from
GBM patients than controls
Xenografts
• Nude mice
• 500.000 cells injected in the flank (primary cell line and
U87 model cell line) or 50.000 cells injected in the
striatum (U87)
• Set to 21 days
• Only spheres form tumors
• Immunohistochemistry
• Cripto-1 in xenograft braintumor and patient samples
• Immunofluorescence
• Cripto-1 and laminin
Results
• Cripto-1 is present in both GBM tissue (gene and protein) and
blood (protein)
• Not all GBM patients have high Cripto-1 levels in tissue and
blood
•
•
Could represent tumor progression???
A distinct subtype of GBM???
• Located along axons and perivascular niche
•
Indicates role in migration and invasion
• Adrenalcorticol hormone (solucortef):
•
No effect on Cripto-1 expression
• Upregulated by hypoxia (2.5 fold) and in spheres (5.5
fold). When combined 19 fold
•
•
In the primary GBM culture – not in model cell line
Indicates role in migration and invasion - can be blocked by knockdown of HIF
•
Mendez, O., et al., Knock down of HIF-1alpha in glioma cells reduces migration in vitro and invasion in vivo and impairs their ability to form tumor spheres.
Mol Cancer, 2010
Keep in mind
• Location in the tumor
• Biopsy – resection
• The small number of patients
Future goals and hopes
• Cripto-1 in relations to:
• Clinical outcome
• Tumor volume
• Ethical application has just been approved
• Primary cell lines
• Sphereformation
• Targeted treatment
• Liposomes – exosomes
Thank you for listening
•
•
•
Laboratory for Cancerbiology, Aalborg University, Denmark
• Meg Duroux, Associate Professor
• Linda Pilgaard, Assistent Professor
• Michael Henriksen, PhD fellow
Department of Neursurgery, Aalborg University Hospital
• Preben Sørensen, MD, Consultant in Neurosurgery, assistent professor
Department of Pathology, Aalborg University Hospital
• Mogens Vyberg, MD, Professor
Related documents
GBM
GBM
Novocure Announces Launch of Recurrent Glioblastoma Product
Novocure Announces Launch of Recurrent Glioblastoma Product
The Role of Alternative Polyadenylation in Glioblastoma
The Role of Alternative Polyadenylation in Glioblastoma
Glioblastoma Multiforme (GBM) – Subtype Analysis
Glioblastoma Multiforme (GBM) – Subtype Analysis
Study Results of Novocure`s Pivotal Phase 3 Trial Published in
Study Results of Novocure`s Pivotal Phase 3 Trial Published in
Brain Tumour Initiative: The Royal Marsden NHS Foundation Trust
Brain Tumour Initiative: The Royal Marsden NHS Foundation Trust
Tumor-Treatment Fields Therapy for Glioblastoma
Tumor-Treatment Fields Therapy for Glioblastoma
CURTANA PHARMACEUTICALS AWARDED NIH SMALL
CURTANA PHARMACEUTICALS AWARDED NIH SMALL
A Patient-Derived, Deeply Characterized
A Patient-Derived, Deeply Characterized
Case Study 55 - University of Pittsburgh
Case Study 55 - University of Pittsburgh
Corporate Ask Letter - Children`s Tumor Foundation
Corporate Ask Letter - Children`s Tumor Foundation
Subcutaneous study on the controlled treatment of Glioma
Subcutaneous study on the controlled treatment of Glioma