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Lorem Sit Amet Dolor
Researcher: Lorem Sit Amet

123 abc lane, Townsville, ZZ 00000, USA
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Determine the efficacy of BMP and MEK inhibitors with RT to treat ACVR1 mutant DIPG
Clinical
DIPG, Childhood (Brain Cancer)
Lay Summary

We and others co-discovered the presence of activating mutations in ACVR1 in 25% of human DIPGs in 2014. Subsequently, my laboratory has developed a murine DIPG model incorporating R206H ACVR1 and observed that R206H ACVR1 significantly accelerates brainstem gliomagenesis. In addition, short-term treatment with a bone morphogenetic protein pathway inhibitor (LDN-212854), significantly reduced proliferation in this model. Furthermore, we have preliminary data that the MAPK pathway is upregulated in human DIPGs with ACVR1 mutations and that the MAPK pathway remains activated in our murine DIPG model despite BMP pathway inhibition.

Therefore, we hypothesize that inhibiting both the BMP pathway and the MAPK pathway will significantly prolong survival of ACVR1 mutant DIPG-bearing mice. Here are proposing to test two treatment strategies: 1) LDN-212854 (a BMP pathway inhibitor) in combination with a MEK inhibitor (PD-0325901), and 2) E6201, a small molecule inhibitor that inhibits both the BMP pathway and the MAPK pathway. Of note, both PD-0325901 and E6201 are already in clinical trials in adult cancers.

Disease Impact

DIPG is an incurable brain tumor that arises in children. The standard of care today in 2017 is the same as it was in the 1960s. This is due, in part, to the frequent “recycling” of adult brain tumor treatment approaches, which is becoming less common due to the discovery of significant genetic differences between adult and pediatric gliomas, including DIPG. In this proposal, we seek to change this. Here we are proposing to evaluate the in vivo efficacy of a bone morphogenetic protein (BMP) pathway inhibitor in combination with a MEK (MAPK/ERK Kinase) inhibitor in our murine DIPG model that harbors the R206H ACVR1 and H3.1K27M mutations. We will evaluate two treatment regimens; one treatment regimen will be a combination of two drugs (LDN-212854 and PD-0325901) and another will be one drug that inhibits both the BMP and MAPK pathways (E6201). Of note, we will evaluate both treatment regimens in combination with radiation, the standard of care for children with DIPG. Results from this proposal will guide future preclinical work as well as guide the development of a clinical trial for children with DIPG through the PBTC.

Innovation

We have developed a murine DIPG model that incorporates mutant ACVR1 (R206H) and H3.1K27M (two genetic alterations that often co-occur in human DIPG specimens). Using this model, we have observed that R206H ACVR1 accelerates brainstem gliomagenesis and that H3.1K27M accelerates brainstem gliomagenesis only in the presence of ACVR1 R206H. We propose to evaluate inhibitors of the BMP and MAPK pathways in this genetic mouse model to help prioritize therapies for clinical trials in children with DIPG. Furthermore, we will also investigate mechanisms of resistance by comparing the RNAseq of treated and untreated tumors.

Feasibility

We have developed this murine DIPG model and have already started making these tumors at Northwestern. With regards to LDN-212854, we have an ongoing collaboration with Paul Yu (a researcher who studies FOP at Harvard) who provides drug to our lab for preclinical testing. We will purchase PD-0325901 from Selleck Chemicals and will receive E6201 from Strategia Therapeutics (See letter of Support).

Expertise

My laboratory has developed these murine models of DIPG and we are experienced in preclinical testing of targeted therapies using this model.

Total Grant Amount Requested

$100,000

Executive Summary

We and others co-discovered the presence of activating mutations in ACVR1 in 25% of human DIPGs in 2014. Subsequently, my laboratory has developed a murine DIPG model incorporating R206H ACVR1 and observed that R206H ACVR1 significantly accelerates brainstem gliomagenesis. In addition, short-term treatment with a bone morphogenetic protein pathway inhibitor (LDN-212854), significantly reduced proliferation in this model. Furthermore, we have preliminary data that the MAPK pathway is upregulated in human DIPGs with ACVR1 mutations and that the MAPK pathway remains activated in our murine DIPG model despite BMP pathway inhibition.

Therefore, we hypothesize that inhibiting both the BMP pathway and the MAPK pathway will significantly prolong survival of ACVR1 mutant DIPG-bearing mice. Here are proposing to test two treatment strategies: 1) LDN-212854 (a BMP pathway inhibitor) in combination with a MEK inhibitor (PD-0325901), and 2) E6201, a small molecule inhibitor that inhibits both the BMP pathway and the MAPK pathway. Of note, both PD-0325901 and E6201 are already in clinical trials in adult cancers.

Disease Impact

DIPG is an incurable brain tumor that arises in children. The standard of care today in 2017 is the same as it was in the 1960s. This is due, in part, to the frequent “recycling” of adult brain tumor treatment approaches, which is becoming less common due to the discovery of significant genetic differences between adult and pediatric gliomas, including DIPG. In this proposal, we seek to change this. Here we are proposing to evaluate the in vivo efficacy of a bone morphogenetic protein (BMP) pathway inhibitor in combination with a MEK (MAPK/ERK Kinase) inhibitor in our murine DIPG model that harbors the R206H ACVR1 and H3.1K27M mutations. We will evaluate two treatment regimens; one treatment regimen will be a combination of two drugs (LDN-212854 and PD-0325901) and another will be one drug that inhibits both the BMP and MAPK pathways (E6201). Of note, we will evaluate both treatment regimens in combination with radiation, the standard of care for children with DIPG. Results from this proposal will guide future preclinical work as well as guide the development of a clinical trial for children with DIPG through the PBTC.

Innovation

We have developed a murine DIPG model that incorporates mutant ACVR1 (R206H) and H3.1K27M (two genetic alterations that often co-occur in human DIPG specimens). Using this model, we have observed that R206H ACVR1 accelerates brainstem gliomagenesis and that H3.1K27M accelerates brainstem gliomagenesis only in the presence of ACVR1 R206H. We propose to evaluate inhibitors of the BMP and MAPK pathways in this genetic mouse model to help prioritize therapies for clinical trials in children with DIPG. Furthermore, we will also investigate mechanisms of resistance by comparing the RNAseq of treated and untreated tumors.

Feasibility

We have developed this murine DIPG model and have already started making these tumors at Northwestern. With regards to LDN-212854, we have an ongoing collaboration with Paul Yu (a researcher who studies FOP at Harvard) who provides drug to our lab for preclinical testing. We will purchase PD-0325901 from Selleck Chemicals and will receive E6201 from Strategia Therapeutics (See letter of Support).

Expertise

My laboratory has developed these murine models of DIPG and we are experienced in preclinical testing of targeted therapies using this model.

Total Grant Amount Requested

$100,000

Description of Research Proposal

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Class aptent taciti sociosqu ad litora torquent per conubia nostra, per inceptos himenaeos. Donec faucibus, turpis sit amet maximus dapibus, sapien nisl bibendum turpis, pharetra commodo tellus libero vel nulla. Sed nec velit viverra, congue sapien et, gravida libero. Proin eget ante eget turpis egestas accumsan. Aliquam arcu nibh, aliquam rhoncus vulputate in, pellentesque at sem. Maecenas cursus tempus nibh id tempus. Mauris dolor sapien, lacinia sit amet condimentum at, dapibus eget lectus. Phasellus vel pellentesque ex. Nunc aliquam in ligula at tristique. In mollis suscipit felis eu finibus. Nullam non dignissim nibh, nec suscipit ex. Suspendisse tincidunt et mauris id finibus. Aliquam vehicula a sem quis venenatis.

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Sed at tortor et tortor tincidunt feugiat id in dui. Vivamus eget justo nisl. Aenean congue laoreet nisl a elementum. Nunc consectetur velit non ligula sollicitudin, quis eleifend urna sollicitudin. Sed tincidunt, nisl quis varius venenatis, dui massa condimentum tellus, sed sollicitudin diam magna mollis augue. Sed venenatis commodo purus id malesuada. Aenean volutpat elit vel gravida consectetur. Vestibulum diam quam, lacinia ac tortor eget, tincidunt dapibus dui. Pellentesque habitant morbi tristique senectus et netus et malesuada fames ac turpis egestas. Proin nisl leo, pretium sed arcu imperdiet, hendrerit sollicitudin sem. Duis non magna at nunc sagittis ullamcorper a id est. Maecenas cursus nisl in faucibus hendrerit.

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Pellentesque nibh erat, egestas sit amet sagittis malesuada, rhoncus at neque. Mauris maximus commodo tortor, non egestas magna finibus vitae. Sed hendrerit nulla vel venenatis tempor. Suspendisse tristique tincidunt libero et placerat. Nam tincidunt condimentum lorem, vel pharetra est iaculis sed. Nullam ac tincidunt orci. Quisque pharetra ut sem sit amet aliquam. Phasellus risus libero, varius in condimentum vel, commodo id ipsum. Aliquam in metus cursus, mattis diam ut, aliquam magna. Suspendisse facilisis dui et orci varius, suscipit facilisis augue dapibus. In eget nibh ipsum. Suspendisse eget pharetra est, quis condimentum felis. Fusce scelerisque congue libero, sed aliquam mi elementum a. Etiam scelerisque ante non auctor porta. Nam eu nunc id ex finibus dictum. Praesent dui ex, dictum ac massa eget, rutrum gravida nisi.

Sed egestas arcu in dui euismod, eget faucibus massa iaculis. Etiam efficitur lectus et purus lobortis, ac blandit eros rutrum. Proin bibendum consectetur leo vel gravida. Etiam et ultricies sapien. Nam lacinia tellus erat, id facilisis est consequat et. Morbi quis risus in neque iaculis pharetra ut consectetur libero. Aenean feugiat tempor mi eu posuere.

Budget

Lorem ipsum dolor sit amet, consectetur adipiscing elit. Integer gravida non felis non euismod. Fusce finibus aliquet consequat. Nam ac metus bibendum, iaculis purus sed, suscipit ligula. Proin et nisi libero. Mauris non urna urna. Nullam augue eros, fringilla sed mauris vitae, porta tincidunt risus. Aliquam sed tincidunt sem. Quisque lacinia quam tortor, imperdiet efficitur odio iaculis in. Sed ultricies condimentum volutpat. Vivamus dignissim faucibus porta.

Curabitur ut ipsum non odio malesuada vulputate. Morbi maximus, est eu lobortis molestie, tortor sapien hendrerit nisi, in cursus odio diam ut odio. Fusce pulvinar volutpat velit. Aliquam erat volutpat. Integer rhoncus mollis suscipit. Praesent non ipsum mollis, finibus nunc a, scelerisque nibh. In feugiat iaculis velit, eu semper lacus dignissim nec. Praesent vitae nisi leo. Cras venenatis dictum magna ut semper. Sed eget eros nibh. Sed vitae quam sed dolor faucibus elementum. Curabitur interdum porttitor finibus. Nullam tincidunt odio lectus, sit amet rhoncus libero dapibus sed. Sed mollis egestas enim, vel porta tortor volutpat eget.

Morbi orci urna, ornare non pretium eget, pulvinar eget magna. Ut consectetur efficitur varius. Fusce ac aliquet mauris, at mattis ligula. Quisque est libero, interdum id orci et, ornare luctus diam. Proin commodo lectus id accumsan blandit. Nulla eu turpis interdum, luctus ante ac, imperdiet tellus. In semper enim eu tristique aliquam.

Collaborations and Conflicts of Interest

Lorem ipsum dolor sit amet, consectetur adipiscing elit. Integer gravida non felis non euismod. Fusce finibus aliquet consequat. Nam ac metus bibendum, iaculis purus sed, suscipit ligula. Proin et nisi libero. Mauris non urna urna. Nullam augue eros, fringilla sed mauris vitae, porta tincidunt risus. Aliquam sed tincidunt sem. Quisque lacinia quam tortor, imperdiet efficitur odio iaculis in. Sed ultricies condimentum volutpat. Vivamus dignissim faucibus porta.

Curabitur ut ipsum non odio malesuada vulputate. Morbi maximus, est eu lobortis molestie, tortor sapien hendrerit nisi, in cursus odio diam ut odio. Fusce pulvinar volutpat velit. Aliquam erat volutpat. Integer rhoncus mollis suscipit. Praesent non ipsum mollis, finibus nunc a, scelerisque nibh. In feugiat iaculis velit, eu semper lacus dignissim nec. Praesent vitae nisi leo. Cras venenatis dictum magna ut semper. Sed eget eros nibh. Sed vitae quam sed dolor faucibus elementum. Curabitur interdum porttitor finibus. Nullam tincidunt odio lectus, sit amet rhoncus libero dapibus sed. Sed mollis egestas enim, vel porta tortor volutpat eget.