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Evaluating Intracerebral Injections of Radiation
Nanomedicine in a Preclinical Mouse Model of
Glioblastoma
Constantine Georgiou
PhD Candidate, Department of Pharmaceutical Sciences
University of Toronto
Outline
1. Introduction to Glioblastoma (GBM) and treatment
2. What is radiation nanomedicine?
3. Animal models, intracerebral injections, methods
4. Biodistribution, SPECT/CT imaging, dosimetry, toxicity
5. Therapeutic evaluation
6. Future directions
2
Glioblastoma (GBM)
2/10 Canadians diagnosed
with any brain tumour will
survive 5 years
<1/10 Canadians
diagnosed with GBM
will survive 5 years
• GBM is the most aggressive and most common malignant brain tumour
• Classified as a high grade (IV) astrocytoma
• While rare compared to other cancers, GBM is always fatal
• GBM incidence: 3-4 per 100,000
• GBM median OS: 12-15 months
Glioblastomas
56.60%
Diffuse
astrocytomas
Glioma
malignant
Ependymal
tumors
Anaplastic
astrocytomas
Oligodendrogliomas
Pilocytic
astrocytomas
Oligoastrocytic
tumors
All others
gliomas
3
Background Rationale Results Future Directions Conclusion
Louis, D., et al. Acta Neuropathologica (2016)
GBM Standard-of-Care
Background Rationale Results Future Directions Conclusion
Surgical
Resection
60 Gy External
Beam
Radiotherapy
Temozolomide
Chemotherapy
4
Treatment Challenges – Residual Disease
The BBB prevents the
majority of chemotherapies
from being effective
Molecular resistance
to Temozolomide
chemotherapy
Complete resection
is impossible
Limited to 60 Gy by external
beam radiotherapy
5
Background Rationale Results Future Directions Conclusion
1. Treatment fails to eliminate residual disease
2. Recurrence occurs within 2-4 cm of the
original tumour
3. No standard treatment for recurrent
disease
What strategies are
available to solve this
problem?
Convection Enhanced Delivery (CED)
• Most therapeutic agents do not
reach effective concentrations
after oral or I.V. administration
• CED catheters are inserted into
the tumour region
• External infusion pump creates a
pressure gradient that infuses
the therapeutic agent
• Compatible with wide range of
therapeutic agents
6
Mehta, A.M., et al. Neurotherapeutics (2017)
Background Rationale Results Future Directions Conclusion
Background Rationale Results Future Directions Conclusion
Selecting a Therapeutic Agent for CED
7
AuNP Chelator Radionuclide
Radiolabeled AuNP
Functionalizing Gold Nanoparticles (AuNP)
• Functionalization is a key ability of AuNPs
• AuNP drug delivery alters the PK of the
therapeutic agent
• Compatible with a wide variety of
therapeutic molecules
• Radionuclides are uniquely positioned
for treating GBM residual disease
• Cancer has reduced capability to repair DNA
damage caused by ionizing radiation
• Generates a predictable therapeutic field
8
Her, S., Jaffray, D.A., Allen, C. Adv. Drug Deliv. Rev. 2017
Inside Particle
Range
Outside
Particle Range
Background Rationale Results Future Directions Conclusion
AuNP Functionalization – Metal Chelating Polymer
• Coat AuNP surface with di-block
metal chelating polymer (MCP)
• Section 1: PEG 2kDa
• Increases stability, reduces
aggregation and MPS uptake
• Section 2: poly-glutamine peptide
with 8 pendant DOTA
• Chelates large amounts of activity
• Section 3: poly-glutamine peptide
with 4 pendant Lipoic Acid groups
• High number of Au-S bonds
increases stability
1 2 3 Dr. Mitch Winnik
Department of
Chemistry
U of T
9
Background Rationale Results Future Directions Conclusion
Radiation Nanomedicine – Radionuclide
10
Pouget, J.P., et al. Nat. Rev. Clin. Oncol. (2011)
β- α
Auger Electron
Physical
Parameter
β- Particle α Particle
Auger
Electron (AE)
Energy 0.05 – 2 MeV 5 – 9 MeV <25 keV
Range in
Tissue
mm – cm
pathlength
Many cell
diameters
μm – mm
pathlength
Several cell
diameters
nm – µm
pathlength
≤ 1 cell
diameter
Linear Energy
Transfer
0.1 – 1.0
keV/µm
50 -230
keV/μm
4 – 26
keV/µm
Best Suited
For:
Small to
medium
tumours
Small volume
metastases
Single cells,
micro-
metastases
Radionuclide 177Lu 225Ac 111In
Background Rationale Results Future Directions Conclusion
Radiation Nanomedicine – Hypothesis
CED of AuNPs radiolabeled with 177Lu will be effective in controlling GBM recurrence
AuNP
Metal Chelating
Polymer (MCP) 177Lu 177Lu-MCP-AuNP
Intraoperative
Administration for
Residual Tumour
11
Background Rationale Results Future Directions Conclusion
Animal Model and Experiments
Inoculate NRG mouse
with U251-Luc Human
GBM cells (2x105
cells/mouse)
Inject with 5 µL of
177Lu-AuNP or
control
SPECT/CT +
MRI + BLI
12
Biodistribution
Toxicity
Therapy
Background Rationale Results Future Directions Conclusion
Single Photon Emission Computed
Tomography (SPECT)
13
Gamma Photon
Emitting Radionuclide
(e.g. 177Lu)
γ
SPECT/CT
Background Rationale Results Future Directions Conclusion
Biodistribution – microSPECT/CT Imaging
14
177
Lu-MCP-AuNP
177
Lu-MCP
Day 0 Day 7 Day 14 Day 21
Day 0 Day 1 Day 2 Day 3
Representative
1 MBq 177Lu
CED injection,
not decay
corrected
Georgiou, C. et al. Mol. Pharm. (2022)
Background Rationale Results Future Directions Conclusion
Biodistribution – Whole Body Retention
15
0 5 10 15 20
0
25
50
75
100
125
Whole Body Retention After Intracranial Injection
Days Post Injection
%ID
(Decay
Corrected)
177
Lu-MCP
177
Lu-AuNP
*
Background Rationale Results Future Directions Conclusion
Dose Calibrator
Biodistribution & Radiation Dosimetry
• Measure cumulative
radioactivity (Ã) in
critical organs from
1 h – 14 d
• Obtain published S
values
• Estimate absorbed
dose per organ using
MIRD equation
16
𝐷 = 𝐴 × 𝑆
1
2
3
4
6
7
A B
Georgiou, C. et al. Mol. Pharm. (2022)
Background Rationale Results Future Directions Conclusion
Biodistribution of 177Lu-AuNP
17
Right
Left
Cerebellum
B
l
o
o
d
H
e
a
r
t
L
u
n
g
L
i
v
e
r
S
p
l
e
e
n
P
a
n
c
r
e
a
s
S
t
o
m
a
c
h
S
m
a
l
l
i
n
t
e
s
t
i
n
e
K
i
d
n
e
y
s
M
u
s
c
l
e
B
o
n
e
S
k
i
n
B
r
a
i
n
(
R
i
g
h
t
)
B
r
a
i
n
(
L
e
f
t
)
B
r
a
i
n
(
C
e
r
e
b
e
l
l
u
m
)
0
2
4
6
8
200
300
400
500
177
Lu-AuNP Biodistribution
%ID/g
1 HPI
24 HPI
72 HPI
168 HPI
336 HPI
Georgiou, C. et al. Mol. Pharm. (2022)
Background Rationale Results Future Directions Conclusion
Radiation Dose Estimates of 177Lu-AuNP
• Intratumoural injections in the
brain stay localized at injection
site
• Highest dose delivery to tumour
• Little irradiation of other brain
regions
• Negligible dose to peripheral
organs
18
Organ/Region Absorbed Dose (Gy)
Heart 0.08 ± 0.01
Lungs 0.06 ± 0.01
Liver 0.15 ± 0.03
Spleen 0.22 ± 0.05
Pancreas 0.07 ± 0.02
Stomach 0.09 ± 0.02
Intestine 0.05 ± 0.01
Kidneys 0.08 ± 0.01
Carcass 0.03 ± 0.01
Whole Brain 16.2 ± 5.8
Cerebellum 0.2 ± 0.1
Left Hemisphere (non-tumour bearing) 0.3 ± 0.1
Right Hemisphere (excluding tumour) 6.4 ± 3.3
Tumour 599 ± 311
Background Rationale Results Future Directions Conclusion
Toxicity Evaluation
A
L
T
(
U
/
L
)
C
R
E
(
u
m
o
l
/
L
)
G
L
U
(
m
m
o
l
/
L
)
T
P
(
g
/
L
)
W
B
C
(
1
0
9
/
L
)
R
B
C
(
1
0
1
2
/
L
)
H
G
B
(
g
/
d
L
)
P
L
T
(
1
0
9
/
L
)
A
L
P
(
U
/
L
)
B
U
N
(
m
m
o
l
/
L
)
H
C
T
(
%
)
0
25
50
75
100
300
400
500
600
Toxicity - Blood Measurements
Control
1.5 MBq 177
Lu-AuNP
1 3 6 8 10 13
0.5
0.6
0.7
0.8
0.9
1.0
1.1
Weight
Time (days)
Body
Weight
Index
(BWI)
Control
1.5 MBq 177
Lu-AuNP
19
Georgiou, C. et al. Mol. Pharm. (2022)
Background Rationale Results Future Directions Conclusion
Audience Poll
Tumour Growth – Bioluminescence Imaging
21
Mezzanotte, L. et al. Trends Biotechnol. (2017)
Background Rationale Results Future Directions Conclusion
Tumour Growth – T2 Weighted MRI
22
M3 Aspect 1T System
RF
In-Phase
Precession
37%
T2 Time (msecs)
100%
Background Rationale Results Future Directions Conclusion
Tumour Growth – BLI
0 7 14 21
0
20
40
60
80
100
Bioluminescent Signal
Days Post Injection
Tumour
Growth
Index
Saline
Non-Radioactive AuNP
177
Lu-AuNP (1.0 MBq)
23
Georgiou, C. et al. Mol. Pharm. (2022)
Background Rationale Results Future Directions Conclusion
Tumour Growth – MRI & Histology
Saline Control
Non-Radioactive
AuNP
177Lu-AuNP
MRI 4 Weeks Post Treatment
S
a
l
i
n
e
N
o
n
-
R
a
d
i
o
a
c
t
i
v
e
A
u
N
P
1
7
7
L
u
-
A
u
N
P
(
1
.
0
M
B
q
)
0
10
20
30
40
50
60
Tumor
Volume
(mm
3
)
A B C
24
Georgiou, C. et al. Mol. Pharm. (2022)
Background Rationale Results Future Directions Conclusion
Tumour Growth – MRI & Histology
Saline Control
Non-Radioactive
AuNP
177Lu-AuNP
A B C
25
Georgiou, C. et al. Mol. Pharm. (2022)
Background Rationale Results Future Directions Conclusion
T: Residual Tumour
M: Tumour Margin
Contralateral (Left)
Hemisphere
Tumour Growth – Long Term Survival
26
Georgiou, C. et al. Mol. Pharm. (2022)
Background Rationale Results Future Directions Conclusion
0
7
1
4
2
1
2
8
3
5
4
2
4
9
5
6
6
3
7
0
7
7
8
4
9
1
9
8
0.7
0.8
0.9
1.0
1.1
1.2
1.3
Body Weight
Days Post Injection
Body
Weight
Index
(BWI)
Saline
Non-Radioactive AuNP
177
Lu-AuNP (1.0 MBq)
0 50 100 150
0
50
100
Kaplan-Meier Curve
Days Post Injection
Percent
Survival
Saline
Non-Radioactive AuNP
177
Lu-AuNP
Summary
• Glioblastoma remains difficult to effectively treat
• Convection enhanced delivery can be used to bypass the BBB
• Radiolabeled gold nanoparticles are uniquely suited for CED
• SPECT/CT and biodistribution can be used to track 177Lu-AuNP in vivo
• Local delivery confined to tumour with large radiation absorbed dose
• 177Lu-AuNP did not cause acute toxicity
• Molecular imaging (BLI + MRI) can be used to evaluate tumour
growth
• 177Lu-AuNP was extremely effective in controlling GBM growth
27
Background Rationale Results Future Directions Conclusion
Future Directions
Checkpoint Immunotherapy Combination
28
Background Rationale Results Future Directions Conclusion
Immune System Activation in Cancer
29
Background Rationale Results Future Directions Conclusion
PD-1 Immune Checkpoint
30
Background Rationale Results Future Directions Conclusion
Anti-PD-1 Immune Checkpoint Inhibitor
31
Background Rationale Results Future Directions Conclusion
32
Bernstein, M.B., et. al. Nat. Rev. Clin. Oncol. (2016)
Background Rationale Results Future Directions Conclusion
Isolate Tumour
Infiltrating
Immune Cells
Collect Whole
Brain from
Treated Mice
Stain and Sort
Immune Cells
(FACS)
Acknowledgements
Reilly Lab
Dr. Zhongli Cai
Dr. Conrad Chan
Valerie Facca
Rella Liu
Misaki Kondo
Felix Ho
Madeline Brown
Stephanie Borlase
Rutka Lab
Carlyn Figueiredo
Supervisor
Dr. Raymond Reilly
Committee Members
Dr. Christine Allen
Dr. James Rutka
Dr. Mitchell Winnik
STTARR
Teesha Komal
Deborah Scollard
CPO
Dr. Azza Al-Mahrouki
Scintica
Tonya Coulthard
33
Q&A Session
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INFO@SCINTICA.COM
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in the Q&A section.
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(March 29, 2023) Webinar: Evaluating Intracerebral Injections of Radiation Nanomedicine in a Preclinical Mouse Model of Glioblastoma​

  • 1. Evaluating Intracerebral Injections of Radiation Nanomedicine in a Preclinical Mouse Model of Glioblastoma Constantine Georgiou PhD Candidate, Department of Pharmaceutical Sciences University of Toronto
  • 2. Outline 1. Introduction to Glioblastoma (GBM) and treatment 2. What is radiation nanomedicine? 3. Animal models, intracerebral injections, methods 4. Biodistribution, SPECT/CT imaging, dosimetry, toxicity 5. Therapeutic evaluation 6. Future directions 2
  • 3. Glioblastoma (GBM) 2/10 Canadians diagnosed with any brain tumour will survive 5 years <1/10 Canadians diagnosed with GBM will survive 5 years • GBM is the most aggressive and most common malignant brain tumour • Classified as a high grade (IV) astrocytoma • While rare compared to other cancers, GBM is always fatal • GBM incidence: 3-4 per 100,000 • GBM median OS: 12-15 months Glioblastomas 56.60% Diffuse astrocytomas Glioma malignant Ependymal tumors Anaplastic astrocytomas Oligodendrogliomas Pilocytic astrocytomas Oligoastrocytic tumors All others gliomas 3 Background Rationale Results Future Directions Conclusion Louis, D., et al. Acta Neuropathologica (2016)
  • 4. GBM Standard-of-Care Background Rationale Results Future Directions Conclusion Surgical Resection 60 Gy External Beam Radiotherapy Temozolomide Chemotherapy 4
  • 5. Treatment Challenges – Residual Disease The BBB prevents the majority of chemotherapies from being effective Molecular resistance to Temozolomide chemotherapy Complete resection is impossible Limited to 60 Gy by external beam radiotherapy 5 Background Rationale Results Future Directions Conclusion 1. Treatment fails to eliminate residual disease 2. Recurrence occurs within 2-4 cm of the original tumour 3. No standard treatment for recurrent disease What strategies are available to solve this problem?
  • 6. Convection Enhanced Delivery (CED) • Most therapeutic agents do not reach effective concentrations after oral or I.V. administration • CED catheters are inserted into the tumour region • External infusion pump creates a pressure gradient that infuses the therapeutic agent • Compatible with wide range of therapeutic agents 6 Mehta, A.M., et al. Neurotherapeutics (2017) Background Rationale Results Future Directions Conclusion
  • 7. Background Rationale Results Future Directions Conclusion Selecting a Therapeutic Agent for CED 7 AuNP Chelator Radionuclide Radiolabeled AuNP
  • 8. Functionalizing Gold Nanoparticles (AuNP) • Functionalization is a key ability of AuNPs • AuNP drug delivery alters the PK of the therapeutic agent • Compatible with a wide variety of therapeutic molecules • Radionuclides are uniquely positioned for treating GBM residual disease • Cancer has reduced capability to repair DNA damage caused by ionizing radiation • Generates a predictable therapeutic field 8 Her, S., Jaffray, D.A., Allen, C. Adv. Drug Deliv. Rev. 2017 Inside Particle Range Outside Particle Range Background Rationale Results Future Directions Conclusion
  • 9. AuNP Functionalization – Metal Chelating Polymer • Coat AuNP surface with di-block metal chelating polymer (MCP) • Section 1: PEG 2kDa • Increases stability, reduces aggregation and MPS uptake • Section 2: poly-glutamine peptide with 8 pendant DOTA • Chelates large amounts of activity • Section 3: poly-glutamine peptide with 4 pendant Lipoic Acid groups • High number of Au-S bonds increases stability 1 2 3 Dr. Mitch Winnik Department of Chemistry U of T 9 Background Rationale Results Future Directions Conclusion
  • 10. Radiation Nanomedicine – Radionuclide 10 Pouget, J.P., et al. Nat. Rev. Clin. Oncol. (2011) β- α Auger Electron Physical Parameter β- Particle α Particle Auger Electron (AE) Energy 0.05 – 2 MeV 5 – 9 MeV <25 keV Range in Tissue mm – cm pathlength Many cell diameters μm – mm pathlength Several cell diameters nm – µm pathlength ≤ 1 cell diameter Linear Energy Transfer 0.1 – 1.0 keV/µm 50 -230 keV/μm 4 – 26 keV/µm Best Suited For: Small to medium tumours Small volume metastases Single cells, micro- metastases Radionuclide 177Lu 225Ac 111In Background Rationale Results Future Directions Conclusion
  • 11. Radiation Nanomedicine – Hypothesis CED of AuNPs radiolabeled with 177Lu will be effective in controlling GBM recurrence AuNP Metal Chelating Polymer (MCP) 177Lu 177Lu-MCP-AuNP Intraoperative Administration for Residual Tumour 11 Background Rationale Results Future Directions Conclusion
  • 12. Animal Model and Experiments Inoculate NRG mouse with U251-Luc Human GBM cells (2x105 cells/mouse) Inject with 5 µL of 177Lu-AuNP or control SPECT/CT + MRI + BLI 12 Biodistribution Toxicity Therapy Background Rationale Results Future Directions Conclusion
  • 13. Single Photon Emission Computed Tomography (SPECT) 13 Gamma Photon Emitting Radionuclide (e.g. 177Lu) γ SPECT/CT Background Rationale Results Future Directions Conclusion
  • 14. Biodistribution – microSPECT/CT Imaging 14 177 Lu-MCP-AuNP 177 Lu-MCP Day 0 Day 7 Day 14 Day 21 Day 0 Day 1 Day 2 Day 3 Representative 1 MBq 177Lu CED injection, not decay corrected Georgiou, C. et al. Mol. Pharm. (2022) Background Rationale Results Future Directions Conclusion
  • 15. Biodistribution – Whole Body Retention 15 0 5 10 15 20 0 25 50 75 100 125 Whole Body Retention After Intracranial Injection Days Post Injection %ID (Decay Corrected) 177 Lu-MCP 177 Lu-AuNP * Background Rationale Results Future Directions Conclusion Dose Calibrator
  • 16. Biodistribution & Radiation Dosimetry • Measure cumulative radioactivity (Ã) in critical organs from 1 h – 14 d • Obtain published S values • Estimate absorbed dose per organ using MIRD equation 16 𝐷 = 𝐴 × 𝑆 1 2 3 4 6 7 A B Georgiou, C. et al. Mol. Pharm. (2022) Background Rationale Results Future Directions Conclusion
  • 18. Radiation Dose Estimates of 177Lu-AuNP • Intratumoural injections in the brain stay localized at injection site • Highest dose delivery to tumour • Little irradiation of other brain regions • Negligible dose to peripheral organs 18 Organ/Region Absorbed Dose (Gy) Heart 0.08 ± 0.01 Lungs 0.06 ± 0.01 Liver 0.15 ± 0.03 Spleen 0.22 ± 0.05 Pancreas 0.07 ± 0.02 Stomach 0.09 ± 0.02 Intestine 0.05 ± 0.01 Kidneys 0.08 ± 0.01 Carcass 0.03 ± 0.01 Whole Brain 16.2 ± 5.8 Cerebellum 0.2 ± 0.1 Left Hemisphere (non-tumour bearing) 0.3 ± 0.1 Right Hemisphere (excluding tumour) 6.4 ± 3.3 Tumour 599 ± 311 Background Rationale Results Future Directions Conclusion
  • 19. Toxicity Evaluation A L T ( U / L ) C R E ( u m o l / L ) G L U ( m m o l / L ) T P ( g / L ) W B C ( 1 0 9 / L ) R B C ( 1 0 1 2 / L ) H G B ( g / d L ) P L T ( 1 0 9 / L ) A L P ( U / L ) B U N ( m m o l / L ) H C T ( % ) 0 25 50 75 100 300 400 500 600 Toxicity - Blood Measurements Control 1.5 MBq 177 Lu-AuNP 1 3 6 8 10 13 0.5 0.6 0.7 0.8 0.9 1.0 1.1 Weight Time (days) Body Weight Index (BWI) Control 1.5 MBq 177 Lu-AuNP 19 Georgiou, C. et al. Mol. Pharm. (2022) Background Rationale Results Future Directions Conclusion
  • 21. Tumour Growth – Bioluminescence Imaging 21 Mezzanotte, L. et al. Trends Biotechnol. (2017) Background Rationale Results Future Directions Conclusion
  • 22. Tumour Growth – T2 Weighted MRI 22 M3 Aspect 1T System RF In-Phase Precession 37% T2 Time (msecs) 100% Background Rationale Results Future Directions Conclusion
  • 23. Tumour Growth – BLI 0 7 14 21 0 20 40 60 80 100 Bioluminescent Signal Days Post Injection Tumour Growth Index Saline Non-Radioactive AuNP 177 Lu-AuNP (1.0 MBq) 23 Georgiou, C. et al. Mol. Pharm. (2022) Background Rationale Results Future Directions Conclusion
  • 24. Tumour Growth – MRI & Histology Saline Control Non-Radioactive AuNP 177Lu-AuNP MRI 4 Weeks Post Treatment S a l i n e N o n - R a d i o a c t i v e A u N P 1 7 7 L u - A u N P ( 1 . 0 M B q ) 0 10 20 30 40 50 60 Tumor Volume (mm 3 ) A B C 24 Georgiou, C. et al. Mol. Pharm. (2022) Background Rationale Results Future Directions Conclusion
  • 25. Tumour Growth – MRI & Histology Saline Control Non-Radioactive AuNP 177Lu-AuNP A B C 25 Georgiou, C. et al. Mol. Pharm. (2022) Background Rationale Results Future Directions Conclusion T: Residual Tumour M: Tumour Margin Contralateral (Left) Hemisphere
  • 26. Tumour Growth – Long Term Survival 26 Georgiou, C. et al. Mol. Pharm. (2022) Background Rationale Results Future Directions Conclusion 0 7 1 4 2 1 2 8 3 5 4 2 4 9 5 6 6 3 7 0 7 7 8 4 9 1 9 8 0.7 0.8 0.9 1.0 1.1 1.2 1.3 Body Weight Days Post Injection Body Weight Index (BWI) Saline Non-Radioactive AuNP 177 Lu-AuNP (1.0 MBq) 0 50 100 150 0 50 100 Kaplan-Meier Curve Days Post Injection Percent Survival Saline Non-Radioactive AuNP 177 Lu-AuNP
  • 27. Summary • Glioblastoma remains difficult to effectively treat • Convection enhanced delivery can be used to bypass the BBB • Radiolabeled gold nanoparticles are uniquely suited for CED • SPECT/CT and biodistribution can be used to track 177Lu-AuNP in vivo • Local delivery confined to tumour with large radiation absorbed dose • 177Lu-AuNP did not cause acute toxicity • Molecular imaging (BLI + MRI) can be used to evaluate tumour growth • 177Lu-AuNP was extremely effective in controlling GBM growth 27 Background Rationale Results Future Directions Conclusion
  • 28. Future Directions Checkpoint Immunotherapy Combination 28 Background Rationale Results Future Directions Conclusion
  • 29. Immune System Activation in Cancer 29 Background Rationale Results Future Directions Conclusion
  • 30. PD-1 Immune Checkpoint 30 Background Rationale Results Future Directions Conclusion
  • 31. Anti-PD-1 Immune Checkpoint Inhibitor 31 Background Rationale Results Future Directions Conclusion
  • 32. 32 Bernstein, M.B., et. al. Nat. Rev. Clin. Oncol. (2016) Background Rationale Results Future Directions Conclusion Isolate Tumour Infiltrating Immune Cells Collect Whole Brain from Treated Mice Stain and Sort Immune Cells (FACS)
  • 33. Acknowledgements Reilly Lab Dr. Zhongli Cai Dr. Conrad Chan Valerie Facca Rella Liu Misaki Kondo Felix Ho Madeline Brown Stephanie Borlase Rutka Lab Carlyn Figueiredo Supervisor Dr. Raymond Reilly Committee Members Dr. Christine Allen Dr. James Rutka Dr. Mitchell Winnik STTARR Teesha Komal Deborah Scollard CPO Dr. Azza Al-Mahrouki Scintica Tonya Coulthard 33
  • 34. Q&A Session WWW.SCINTICA.COM INFO@SCINTICA.COM Please enter your questions in the Q&A section. Thank You!

Editor's Notes

  1. Fastest growing and most aggressive grade of astrocytoma (WHO grade IV) Most common glioma: 56.6% Astrocytic tumours (including GBM) make up >75% of all gliomas Glioblastoma incidence: approximately 3 in 100,000 Five year survival: Pilocytic astrocytoma (I) – 94.1% Glioblastoma (IV) – 5.6%
  2. Surgical resection to the greatest possible extent Depending on location within the brain External beam radiotherapy delivered in 2 Gy fractions TMZ given concurrently and after radiation
  3. Surgery While a large resection can be possible, 100% resection is impossible due to the invasive nature of GBM Resistance Approx 50% of GBM tumours have an epigenetic silencing that confers resistance to TMZ Efflux transporters at the BBB block the penetration of chemotherapeutic drugs Established and novel drugs must effectively bypass the BBB Attempted chemotherapies have failed during clinical trials
  4. CED is capable of injecting a wide range of therapeutics since delivery relies on convection (pressure gradient) not diffusion Means that infusion is not correlated with molecular weight
  5. Optical, thermal, radiation dose enhancement Control over physical characteristics Size, shape, surface Useful physicochemical properties Easily modifiable surface provides endless functionalization options Gold-thiol conjugation chemistry AuNPs often used as a liquid drug delivery vehicle DNA repair pathways are usually impaired in cancer cells, additionally rapidly dividing cells expose DNA more often making them more susceptible to damage Radionuclide does not need to enter every cell, the effective range depends on the radionuclide
  6. MPS (mononuclear phagocyte system) Made up of Monocytes and macrophages (immune cells) that accumulate in the lymph nodes, spleen Kupffer cells in the liver
  7. Beta particle stuff Beta particle decay occurs in neutron rich nuclei, where a neutron is converted to a proton and an electron is released 197Hg stuff Auger electrons are released by proton rich nuclei by electron capture and or internal conversion Electron capture Inner shell electron is absorbed into the nucleus and combines with a proton which transforms into a neutron and releases an electron neutrino Outer shell electron replaces the captured inner one and energy must be released, usually in the form of an xray or that energy is given to another electron and is ejected Atomic number is reduced by 1 since the proton is lost but the mass number doesn’t change
  8. NRG mice chosen since they are more radioresistant than NOD/SCID mice but can still receive the tumour xenograft Carry two mutations: Targeted knockout mutation of the recombination activating gene 1 Renders the mice B and T cell deficient Immunodeficiency lets tumour cells be engrafted Complete null allele of the IL2 receptor common gamma chain Prevents cytokine signalling in multiple receptors so that NK cells are deficient Scid backgrounds have a mutuation in the DNA repair enzyme Prkdc (DNA-dependent protein kinases) which makes them more sensitive to radiation and drugs
  9. MIP bone scan
  10. Representative images, data on next slide not from the same mice/experiment Not decay corrected, loss of intensity is a combination of radioactive decay and redistribution
  11. Learn PK models
  12. MIRD = Medical internal radiation dose
  13. Alanine Aminotransferase Creatinine Glucose Total Protein White blood Red blood Hemoglobin Platlets Alkaline phosphatase Blood urea nitrogen Hematocrit
  14. When the radiofrequency energy is stopped, another effect is that the protons lose their in-phase spin or precession, and begin to precess out-of-phase again as shown on the left of this slide. This process is called spin-spin relaxation. The graph at the right shows the proportion of protons exhibiting in-phase precession vs. time in msec after the radiofrequency energy is stopped. The time taken for 63% of the protons to lose their in-phase precession, or in other words, 37% of the protons retaining their in-phase precession is known as T2. This will be important to understand when I discuss T2-weighted MRI later in the lecture.
  15. Right 177Lu-AuNP treated mouse, residual tumour identified with normal brain tissue (no radiation necrosis) outside on the margins Contralateral side is completely normal
  16. Ideal immune system activation against cancer Antigens are picked up by dendritic cells and presented to T Cells for activation Activated T cell finds tumour and recognizes the antigen Leads to cell death
  17. Binding of PD-1 to PD-L1 on cancer cells deactivate the T Cell and leads to immune system evasion Tumour cells often upregulate PD-L1 Associated with increased tumour aggressiveness and lower survival
  18. Use of anti-PD-1 antibody blocks the PD-1/PD-L1 binding and keeps the T cell activated The immune system can attack the tumour cell