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Application Brief – Breast Cancer Research

Executive Summary

Breast cancer research in animal models has long been hindered by the lack of a fast, portable,
high resolution, research and animal focused imaging system that can visualize 2D tumor size, 3D
tumor volume, neoangiogenesis and blood perfusion in vivo, in real-time and most importantly,
non-invasively.

In order to ameliorate this problem, VisualSonics has introduced a revolutionary micro-ultrasound
system that allows researchers to collect a plethora of important data over the lifespan of animals,
thereby significantly reducing the number of animals needed. Furthermore, this system is designed
for high-throughput research and is able to image both subcutaneous (xenograft) and orthotopic
tumors. 3D tumor volume and tumor vascularity can be quickly quantified, while MicroMarker™
contrast agents allow the quantification of perfusion kinetics and also the possibility to track
endothelial cell markers such as VEGFR and integrins.

Hundreds of satisfied cancer researchers using Vevo® micro-ultrasound systems, from institutions
such as Vanderbilt, Stanford and Oxford are publishing articles in leading journals such as Science,
Clinical Cancer Research, PNAS and Cancer Research. This is a testament of the power and
versatility of high-resolution ultrasound.




                       Pre-Palpable Tumor Sizing in a Transgenic WAP-TAg Mouse Model.
                      Image courtesy of Lombardi Cancer Center, Georgetown University.

Application Brief: Breast Cancer ver1.0                                                       Page 1
Background on Breast Cancer Research

Breast cancer is a highly prevalent disease in the female population, affecting 1 in 8 women in the
United States.1 It is no wonder that breast cancer is currently one of the key focuses in biomedical
research. Over the past few decades, breast cancer incidence and mortality have decreased
steadily, due in part to chemotherapy such as tamoxifen and novel biologics such as Herceptin and
Avastin.

Although there have been numerous small triumphs over breast cancer, much work still needs to
be done. There were about 40,000 deaths in 2009 due to breast cancer in the United States alone.1
Small animal research in solid or metastatic breast cancer is a key part of the battle against this
disease. In order to facilitate this research, in vivo imaging methods are needed to track disease
progression in cancer models over a period of time. This offers significant advantages over
traditional methods of calipers and histology. By using animals as their own controls, not only can
researchers save much time, but also fewer mice are needed for statistical significance and results
are less affected by confounding factors. Moreover, these imaging modalities allow the study of
effects of therapeutic interventions such as change in tumor volume and angiogenesis. However,
many conventional methods such as micro-MRI or micro-CT have significant drawbacks associated,
such as significant costs, radioactivity and slow image acquisition.

In today’s research, time is of the essence. To test novel hypotheses and discover new drugs,
scientists need access to an imaging modality that will grant them the possibility of quickly
visualizing tumor growth and blood flow in vivo, non-invasively, and in real-time. This is where the
Vevo high-frequency micro-ultrasound comes in.




Application Brief: Breast Cancer ver1.0                                                       Page 2
Micro-Ultrasound in Breast Cancer Research

Micro-ultrasound using high-frequency probes and intravenous contrast agent has been regarded
by many of the world’s top researchers as an attractive technique for accessing tumor size and
angiogenic activity. Most research in this area is done using mice, because of their wide availability,
variety of strains and close similarities to human biology. Micro-ultrasound is especially suitable to
study mice as they are the perfect size to take advantage of the maximum resolution Vevo systems
offer.

For example, micro-ultrasound has been demonstrated to be a quick and accurate way of tracking
tumor sizes non-invasively over a longitudinal study. Dong et al. and Wang et al. both published
recently in Cancer Research of tracking breast tumor growth in vivo with administration of Vitamin
E analogues,2 and a conjugate peptide target of α-tocopheryl succinate (α-TOS).3 The authors
found that these compounds were able to selectively kill angiogenic endothelial cells,2 or induce
rapid apoptosis in erbB2-positive breast tumors,3 respectively. These results were achieved non-
invasively using the Vevo 770 system, which quantified tumor sizes accurately and was shown to
be superior to digital calipers.3 Furthermore, percent vascularization of individual tumors were
assessed using the Power Doppler Mode, which monitors blood flow in real-time.2 In conclusion, the
authors found that micro-ultrasound imaging allowed both visualization and quantification of non-
invasive tracking of tumor size and angiogenesis with mice models.

Lyshchik et al. used targeted contrast-enhanced high-frequency micro-ultrasound to monitor
in vivo VEGFR2 expression on tumor vascular endothelium.4 The authors used ultrasound
microbubbles conjugated with an anti-VEGFR2 monoclonal antibody to examine the vasculature of
adult nu/nu mice injected subcutaneously with 4T1 and 67NR breast cancer cells.4 The authors
found that micro-ultrasound is effective when compared with immunohistochemistry and
immunoblotting to quantify the relative expression of VEGFR2 in tumor vasculature. The authors
also concluded that micro-ultrasound has significant advantages over micro-MRI and micro-CT for
this purpose, as the system is portable and readily available. Furthermore, it provides high
resolution (40 μm) images and uses contrast agents that are specifically intravascularly confined,
thus minimizing nonspecific signals from extravasated contrast agents.4

Loveless et al. also examined the use of micro-ultrasound to assess tumor vascularity in mice
injected with 67NR breast cancer cells.5 The authors were able to visualize and quantify
microvasculature at the capillary level with high repeatability and minimal background noise.5 The
authors found that micro-ultrasound not only had the distinct advantages of speed and


Application Brief: Breast Cancer ver1.0                                                          Page 3
accessibility, but also created high-resolution 3-dimensional images of tumor vessels. Thus, they
are ideal for studying anti-angiogenic activity of therapeutic compounds on preclinical models.5

Many other researchers in recent years have also been using Vevo systems as an easily accessible,
applicable, fast and superior way to image tumor volume and angiogenesis. For an extended list of
publications, please refer to document titled Top Cancer Research Papers with the Vevo®
Systems.




                         4T1 Orthotopic Tumor Model in Mouse with Surrounding Tissue.
                         Image courtesy of Robarts Research Institute, London, Canada.




Application Brief: Breast Cancer ver1.0                                                        Page 4
VisualSonics’ Value Proposition

Cancer research and tumor imaging has traditionally been associated with modalities such as MRI,
CT, PET and SPECT. However, despite their various strengths, many of these systems suffer from
significant drawbacks, including significant costs and radiation. Furthermore, none of the above
imaging modalities is real-time per se, compared with the Vevo system which can capture images
instantaneously and construct 3D tumor images in seconds. In fact, it has been demonstrated by
Loveless et al. that micro-ultrasound produces images eclipsing MRI resolution and that the two
imaging systems can be combined to validate each other’s results.6

Below is a summary of the unique value proposition VisualSonics delivers to researchers with the
Vevo micro-ultrasound systems:

    1. Non-invasive, in vivo, real-time imaging for quick screening (in seconds) and early tumor
        detection (pre-palpable sizes, >1x10-4 mm3). This allows high-throughput sorting of study
        animals to optimize homogeneity of test subjects for longitudinal studies.

    2. Sophisticated quantification of tumor volumes in 3D. Together with stunning clarity of down
        to 30 μm, the researcher is given maximum flexibility in choosing from a wide variety of
        tumor models in small animals.

    3. Quantification of a plethora of perfusion kinetic parameters associated with angiogenesis
        and blood flow.

    4. Targeted biomarker molecular imaging with antibody-bound contrast agents (VEGFR,
        integrins, VE-Cadherin, etc.). The unique property of these contrast agents to stay in the
        vasculature provides unparalleled power for angiogenesis biomarker research.

    5. Guidance of micro-injections of stem cells, drugs, interstitial pressure probes etc. into
        tumors or vasculature, without need for invasive surgery.

    6. Detection and quantification of cardiotoxicity in response to cancer therapy. The
        incomparable image acquisition speed and huge variety of software analysis tools allows for
        elaborate assessment of cardiac function.

    7. Dedicated animal platform to monitor ECG, heart rate, body temperature and respiration
        rates. The researcher is able to keep track of different parameters of the animal physiology
        in real-time throughout the imaging session and to maintain the animal under ideal


Application Brief: Breast Cancer ver1.0                                                       Page 5
conditions. Together with our specially designed anesthesia system, this also allows
        researchers to spend minimal time on preparatory work and thus optimize throughput.

For a full list of cancer applications with the Vevo, together with examples from literature, please
consult White Paper: High Resolution Micro-Ultrasound for Small Animal Cancer Imaging.




                                Vevo 2100 Micro-Ultrasound Imaging System




Application Brief: Breast Cancer ver1.0                                                       Page 6
References

    1. American Cancer Society. Cancer Facts and Figures 2009. Atlanta, Ga: American Cancer
       Society; 2009.

    2. Dong LF, Swettenham E, Eliasson J, Wang XF, Gold M, Medunic Y, Stantic M, Low P,
       Prochazka L, Witting PK, Turanek J, Akporiaye ET, Ralph SJ, Neuzil J. Vitamin E analogues
       inhibit angiogenesis by selective induction of apoptosis in proliferating endothelial cells: the
       role of oxidative stress. Cancer Res 2007 Dec 15;67(24):11906-13.

    3. Wang XF, Birringer M, Dong LF, Veprek P, Low P, Swettenham E, Stantic M, Yuan LH,
       Zobalova R, Wu K, Ledvina M, Ralph SJ, Neuzil J. A peptide conjugate of vitamin E succinate
       targets breast cancer cells with high ErbB2 expression. Cancer Res 2007 Apr 1;67(7):3337-
       44.

    4. Lyshchik A, Fleischer AC, Huamani J, Hallahan DE, Brissova M, Gore JC. Molecular imaging
       of vascular endothelial growth factor receptor 2 expression using targeted contrast-
       enhanced high-frequency ultrasonography. J Ultrasound Med 2007 Nov;26(11):1575-86.

    5. Loveless ME, Li X, Huamani J, Lyshchik A, Dawant B, Hallahan D, Gore JC, Yankeelov TE. A
       method for assessing the microvasculature in a murine tumor model using contrast-
       enhanced ultrasonography. J Ultrasound Med 2008 Dec;27(12):1699-709.

    6. Loveless ME, Whisenant JG, Wilson K, Lyshchik A, Sinha TK, Gore JC, Yankeelov TE.
       Coregistration of ultrasonography and magnetic resonance imaging with a preliminary
       investigation of the spatial colocalization of vascular endothelial growth factor receptor 2
       expression and tumor perfusion in a murine tumor model. Mol Imaging 2009;8(4):187-98.




Application Brief: Breast Cancer ver1.0                                                           Page 7

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Application Brief - Breast Cancer Research

  • 1. Application Brief – Breast Cancer Research Executive Summary Breast cancer research in animal models has long been hindered by the lack of a fast, portable, high resolution, research and animal focused imaging system that can visualize 2D tumor size, 3D tumor volume, neoangiogenesis and blood perfusion in vivo, in real-time and most importantly, non-invasively. In order to ameliorate this problem, VisualSonics has introduced a revolutionary micro-ultrasound system that allows researchers to collect a plethora of important data over the lifespan of animals, thereby significantly reducing the number of animals needed. Furthermore, this system is designed for high-throughput research and is able to image both subcutaneous (xenograft) and orthotopic tumors. 3D tumor volume and tumor vascularity can be quickly quantified, while MicroMarker™ contrast agents allow the quantification of perfusion kinetics and also the possibility to track endothelial cell markers such as VEGFR and integrins. Hundreds of satisfied cancer researchers using Vevo® micro-ultrasound systems, from institutions such as Vanderbilt, Stanford and Oxford are publishing articles in leading journals such as Science, Clinical Cancer Research, PNAS and Cancer Research. This is a testament of the power and versatility of high-resolution ultrasound. Pre-Palpable Tumor Sizing in a Transgenic WAP-TAg Mouse Model. Image courtesy of Lombardi Cancer Center, Georgetown University. Application Brief: Breast Cancer ver1.0 Page 1
  • 2. Background on Breast Cancer Research Breast cancer is a highly prevalent disease in the female population, affecting 1 in 8 women in the United States.1 It is no wonder that breast cancer is currently one of the key focuses in biomedical research. Over the past few decades, breast cancer incidence and mortality have decreased steadily, due in part to chemotherapy such as tamoxifen and novel biologics such as Herceptin and Avastin. Although there have been numerous small triumphs over breast cancer, much work still needs to be done. There were about 40,000 deaths in 2009 due to breast cancer in the United States alone.1 Small animal research in solid or metastatic breast cancer is a key part of the battle against this disease. In order to facilitate this research, in vivo imaging methods are needed to track disease progression in cancer models over a period of time. This offers significant advantages over traditional methods of calipers and histology. By using animals as their own controls, not only can researchers save much time, but also fewer mice are needed for statistical significance and results are less affected by confounding factors. Moreover, these imaging modalities allow the study of effects of therapeutic interventions such as change in tumor volume and angiogenesis. However, many conventional methods such as micro-MRI or micro-CT have significant drawbacks associated, such as significant costs, radioactivity and slow image acquisition. In today’s research, time is of the essence. To test novel hypotheses and discover new drugs, scientists need access to an imaging modality that will grant them the possibility of quickly visualizing tumor growth and blood flow in vivo, non-invasively, and in real-time. This is where the Vevo high-frequency micro-ultrasound comes in. Application Brief: Breast Cancer ver1.0 Page 2
  • 3. Micro-Ultrasound in Breast Cancer Research Micro-ultrasound using high-frequency probes and intravenous contrast agent has been regarded by many of the world’s top researchers as an attractive technique for accessing tumor size and angiogenic activity. Most research in this area is done using mice, because of their wide availability, variety of strains and close similarities to human biology. Micro-ultrasound is especially suitable to study mice as they are the perfect size to take advantage of the maximum resolution Vevo systems offer. For example, micro-ultrasound has been demonstrated to be a quick and accurate way of tracking tumor sizes non-invasively over a longitudinal study. Dong et al. and Wang et al. both published recently in Cancer Research of tracking breast tumor growth in vivo with administration of Vitamin E analogues,2 and a conjugate peptide target of α-tocopheryl succinate (α-TOS).3 The authors found that these compounds were able to selectively kill angiogenic endothelial cells,2 or induce rapid apoptosis in erbB2-positive breast tumors,3 respectively. These results were achieved non- invasively using the Vevo 770 system, which quantified tumor sizes accurately and was shown to be superior to digital calipers.3 Furthermore, percent vascularization of individual tumors were assessed using the Power Doppler Mode, which monitors blood flow in real-time.2 In conclusion, the authors found that micro-ultrasound imaging allowed both visualization and quantification of non- invasive tracking of tumor size and angiogenesis with mice models. Lyshchik et al. used targeted contrast-enhanced high-frequency micro-ultrasound to monitor in vivo VEGFR2 expression on tumor vascular endothelium.4 The authors used ultrasound microbubbles conjugated with an anti-VEGFR2 monoclonal antibody to examine the vasculature of adult nu/nu mice injected subcutaneously with 4T1 and 67NR breast cancer cells.4 The authors found that micro-ultrasound is effective when compared with immunohistochemistry and immunoblotting to quantify the relative expression of VEGFR2 in tumor vasculature. The authors also concluded that micro-ultrasound has significant advantages over micro-MRI and micro-CT for this purpose, as the system is portable and readily available. Furthermore, it provides high resolution (40 μm) images and uses contrast agents that are specifically intravascularly confined, thus minimizing nonspecific signals from extravasated contrast agents.4 Loveless et al. also examined the use of micro-ultrasound to assess tumor vascularity in mice injected with 67NR breast cancer cells.5 The authors were able to visualize and quantify microvasculature at the capillary level with high repeatability and minimal background noise.5 The authors found that micro-ultrasound not only had the distinct advantages of speed and Application Brief: Breast Cancer ver1.0 Page 3
  • 4. accessibility, but also created high-resolution 3-dimensional images of tumor vessels. Thus, they are ideal for studying anti-angiogenic activity of therapeutic compounds on preclinical models.5 Many other researchers in recent years have also been using Vevo systems as an easily accessible, applicable, fast and superior way to image tumor volume and angiogenesis. For an extended list of publications, please refer to document titled Top Cancer Research Papers with the Vevo® Systems. 4T1 Orthotopic Tumor Model in Mouse with Surrounding Tissue. Image courtesy of Robarts Research Institute, London, Canada. Application Brief: Breast Cancer ver1.0 Page 4
  • 5. VisualSonics’ Value Proposition Cancer research and tumor imaging has traditionally been associated with modalities such as MRI, CT, PET and SPECT. However, despite their various strengths, many of these systems suffer from significant drawbacks, including significant costs and radiation. Furthermore, none of the above imaging modalities is real-time per se, compared with the Vevo system which can capture images instantaneously and construct 3D tumor images in seconds. In fact, it has been demonstrated by Loveless et al. that micro-ultrasound produces images eclipsing MRI resolution and that the two imaging systems can be combined to validate each other’s results.6 Below is a summary of the unique value proposition VisualSonics delivers to researchers with the Vevo micro-ultrasound systems: 1. Non-invasive, in vivo, real-time imaging for quick screening (in seconds) and early tumor detection (pre-palpable sizes, >1x10-4 mm3). This allows high-throughput sorting of study animals to optimize homogeneity of test subjects for longitudinal studies. 2. Sophisticated quantification of tumor volumes in 3D. Together with stunning clarity of down to 30 μm, the researcher is given maximum flexibility in choosing from a wide variety of tumor models in small animals. 3. Quantification of a plethora of perfusion kinetic parameters associated with angiogenesis and blood flow. 4. Targeted biomarker molecular imaging with antibody-bound contrast agents (VEGFR, integrins, VE-Cadherin, etc.). The unique property of these contrast agents to stay in the vasculature provides unparalleled power for angiogenesis biomarker research. 5. Guidance of micro-injections of stem cells, drugs, interstitial pressure probes etc. into tumors or vasculature, without need for invasive surgery. 6. Detection and quantification of cardiotoxicity in response to cancer therapy. The incomparable image acquisition speed and huge variety of software analysis tools allows for elaborate assessment of cardiac function. 7. Dedicated animal platform to monitor ECG, heart rate, body temperature and respiration rates. The researcher is able to keep track of different parameters of the animal physiology in real-time throughout the imaging session and to maintain the animal under ideal Application Brief: Breast Cancer ver1.0 Page 5
  • 6. conditions. Together with our specially designed anesthesia system, this also allows researchers to spend minimal time on preparatory work and thus optimize throughput. For a full list of cancer applications with the Vevo, together with examples from literature, please consult White Paper: High Resolution Micro-Ultrasound for Small Animal Cancer Imaging. Vevo 2100 Micro-Ultrasound Imaging System Application Brief: Breast Cancer ver1.0 Page 6
  • 7. References 1. American Cancer Society. Cancer Facts and Figures 2009. Atlanta, Ga: American Cancer Society; 2009. 2. Dong LF, Swettenham E, Eliasson J, Wang XF, Gold M, Medunic Y, Stantic M, Low P, Prochazka L, Witting PK, Turanek J, Akporiaye ET, Ralph SJ, Neuzil J. Vitamin E analogues inhibit angiogenesis by selective induction of apoptosis in proliferating endothelial cells: the role of oxidative stress. Cancer Res 2007 Dec 15;67(24):11906-13. 3. Wang XF, Birringer M, Dong LF, Veprek P, Low P, Swettenham E, Stantic M, Yuan LH, Zobalova R, Wu K, Ledvina M, Ralph SJ, Neuzil J. A peptide conjugate of vitamin E succinate targets breast cancer cells with high ErbB2 expression. Cancer Res 2007 Apr 1;67(7):3337- 44. 4. Lyshchik A, Fleischer AC, Huamani J, Hallahan DE, Brissova M, Gore JC. Molecular imaging of vascular endothelial growth factor receptor 2 expression using targeted contrast- enhanced high-frequency ultrasonography. J Ultrasound Med 2007 Nov;26(11):1575-86. 5. Loveless ME, Li X, Huamani J, Lyshchik A, Dawant B, Hallahan D, Gore JC, Yankeelov TE. A method for assessing the microvasculature in a murine tumor model using contrast- enhanced ultrasonography. J Ultrasound Med 2008 Dec;27(12):1699-709. 6. Loveless ME, Whisenant JG, Wilson K, Lyshchik A, Sinha TK, Gore JC, Yankeelov TE. Coregistration of ultrasonography and magnetic resonance imaging with a preliminary investigation of the spatial colocalization of vascular endothelial growth factor receptor 2 expression and tumor perfusion in a murine tumor model. Mol Imaging 2009;8(4):187-98. Application Brief: Breast Cancer ver1.0 Page 7