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1. BRD4 amplification facilitates an oncogenic gene expression program in high-grade serous ovarian cancer and confers sensitivity to BET inhibitors.

Author

Garrett W Rhyasen, Yi Yao, Jingwen Zhang, Austin Dulak, Lillian Castriotta, Kelly Jacques, Wei Zhao, Farzin Gharahdaghi, Maureen M Hattersley, Paul D Lyne, Edwin Clark, Michael Zinda, Stephen E Fawell, Gordon B Mills, and Huawei Chen

Subjects
Medicine, Science
Abstract

BRD4 is a transcriptional co-activator functioning to recruit regulatory complexes to acetylated chromatin. A subset of High-grade Serous Ovarian Cancer (HGSOC) patients are typified by focal, recurrent BRD4 gene amplifications. Despite previously described cancer dependencies, it is unclear whether BRD4 amplification events are oncogenic in HGSOC. We find that physiologically relevant levels of expression of BRD4 isoforms in non-transformed ovarian cells result in cellular transformation. Transcriptional profiling of BRD4-transformed ovarian cells, and BRD4-amplified HGSOC patient samples revealed shared expression patterns, including enriched MYC, and E2F1 gene signatures. Furthermore, we demonstrate that a novel BET inhibitor, AZD5153, is highly active in BRD4-amplified patient derived xenografts and uncover Neuregulin-1 as a novel BRD4 effector. Experiments involving Neuregulin-1 inhibition and exogenous addition, demonstrate Neuregulin-1 as necessary and sufficient for BRD4-mediated transformation. This study demonstrates the oncogenic potential of BRD4 amplification in cancer and establishes BRD4-amplified HGSOC as a potential patient population that could benefit from BET inhibitors.

Published
2018
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2. Gay spirituality

Author

Johnson, Edwin Clark. and Johnson, Edwin Clark.

Published
2007

3. Gay perspective

Author

Johnson, Edwin Clark. and Johnson, Edwin Clark.

Published
2008

7. Edwin Clark University,2023/2024 Admission Form Is Out Call 07063666272 Transfer Form,Post Utme Form,Direct Entry{07063666272} DR. Mr MARCUS. For Admission Processing, Post utme form, Pre-Degree / REMEDIAL Form, CALL PROF MARCUS {07063666272} Jupeb form IJMB Form, Masters form, Ph.D. Form, Sandwich Form, Diploma Form, Change of institution form, Transfer form, Change of course Form are all out Call on {07063666272} on how to purchase the form and register online, For Admission Process on how to be admitted and mode of payment of School Fee And Acceptances Fee Contact Office of the registrar on 07063666272 for more Inquiry On GUIDELINES AND ADMISSION ASSISTANCE CALL PROF. MR MARCUS A A ON 07063666272

Author

University, Edwin Clark

Abstract

Edwin Clark University,2023/2024 Admission Form Is Out Call 07063666272 Transfer Form,Post Utme Form,Direct Entry{07063666272} DR. Mr MARCUS. For Admission Processing, Post utme form, Pre-Degree / REMEDIAL Form, CALL PROF MARCUS {07063666272} Jupeb form IJMB Form, Masters form, Ph.D. Form, Sandwich Form, Diploma Form, Change of institution form, Transfer form, Change of course Form are all out Call on {07063666272} on how to purchase the form and register online, For Admission Process on how to be admitted and mode of payment of School Fee And Acceptances Fee Contact Office of the registrar on 07063666272 for more Inquiry On GUIDELINES AND ADMISSION ASSISTANCE CALL PROF. MR MARCUS A A ON 07063666272

Published
2023
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9. Supplementary Figures 1-5 from AZD5153: A Novel Bivalent BET Bromodomain Inhibitor Highly Active against Hematologic Malignancies

Author

Huawei Chen, Edwin Clark, Michael Zinda, Michael J. Waring, Stephen E. Fawell, Gordon B. Mills, Paul Lyne, Corinne Reimer, Jonathan R. Dry, Alfred A. Rabow, Tammie C. Yeh, Greg O'Connor, Graeme Walker, Miika J. Ahdesmaki, Larry Bao, Michael Collins, Deborah Lawson, Lillian Castriotta, Shenghua Wen, Jingwen Zhang, Tony Cheung, Scott Boiko, Ian L. Dale, Philip Petteruti, Wenxian Wang, Austin Dulak, Yi Yao, Maureen M. Hattersley, and Garrett W. Rhyasen

Abstract

Supplementary Figure 1. AZD5153 shows reduced BRD4 binding activity when BD2 function is abolished; Supplementary Figure 2. AZD5153 modulates MYC protein levels across hematologic cancer cell lines; Supplementary Figure 3. Gene Ontology (GO) analysis of the down-regulated transcripts by AZD5153 across all cell line types; Supplementary Figure 4. IC50 and percent maximal cell kill by AZD5153 and I-BET762 in five hematologic cell lines; Supplementary Figure 5. Tumor growth inhibition across six hematological xenograft Models

Published
2023

10. Supplementary Table 3 from AZD5153: A Novel Bivalent BET Bromodomain Inhibitor Highly Active against Hematologic Malignancies

Author

Huawei Chen, Edwin Clark, Michael Zinda, Michael J. Waring, Stephen E. Fawell, Gordon B. Mills, Paul Lyne, Corinne Reimer, Jonathan R. Dry, Alfred A. Rabow, Tammie C. Yeh, Greg O'Connor, Graeme Walker, Miika J. Ahdesmaki, Larry Bao, Michael Collins, Deborah Lawson, Lillian Castriotta, Shenghua Wen, Jingwen Zhang, Tony Cheung, Scott Boiko, Ian L. Dale, Philip Petteruti, Wenxian Wang, Austin Dulak, Yi Yao, Maureen M. Hattersley, and Garrett W. Rhyasen

Abstract

Protein modulation by AZD5153 in hematological cell lines

Published
2023

11. Supplementary Table 1 from AZD5153: A Novel Bivalent BET Bromodomain Inhibitor Highly Active against Hematologic Malignancies

Author

Huawei Chen, Edwin Clark, Michael Zinda, Michael J. Waring, Stephen E. Fawell, Gordon B. Mills, Paul Lyne, Corinne Reimer, Jonathan R. Dry, Alfred A. Rabow, Tammie C. Yeh, Greg O'Connor, Graeme Walker, Miika J. Ahdesmaki, Larry Bao, Michael Collins, Deborah Lawson, Lillian Castriotta, Shenghua Wen, Jingwen Zhang, Tony Cheung, Scott Boiko, Ian L. Dale, Philip Petteruti, Wenxian Wang, Austin Dulak, Yi Yao, Maureen M. Hattersley, and Garrett W. Rhyasen

Abstract

Cell line authentication information

Published
2023

12. Data from AZD5153: A Novel Bivalent BET Bromodomain Inhibitor Highly Active against Hematologic Malignancies

Author

Huawei Chen, Edwin Clark, Michael Zinda, Michael J. Waring, Stephen E. Fawell, Gordon B. Mills, Paul Lyne, Corinne Reimer, Jonathan R. Dry, Alfred A. Rabow, Tammie C. Yeh, Greg O'Connor, Graeme Walker, Miika J. Ahdesmaki, Larry Bao, Michael Collins, Deborah Lawson, Lillian Castriotta, Shenghua Wen, Jingwen Zhang, Tony Cheung, Scott Boiko, Ian L. Dale, Philip Petteruti, Wenxian Wang, Austin Dulak, Yi Yao, Maureen M. Hattersley, and Garrett W. Rhyasen

Abstract

The bromodomain and extraterminal (BET) protein BRD4 regulates gene expression via recruitment of transcriptional regulatory complexes to acetylated chromatin. Pharmacological targeting of BRD4 bromodomains by small molecule inhibitors has proven to be an effective means to disrupt aberrant transcriptional programs critical for tumor growth and/or survival. Herein, we report AZD5153, a potent, selective, and orally available BET/BRD4 bromodomain inhibitor possessing a bivalent binding mode. Unlike previously described monovalent inhibitors, AZD5153 ligates two bromodomains in BRD4 simultaneously. The enhanced avidity afforded through bivalent binding translates into increased cellular and antitumor activity in preclinical hematologic tumor models. In vivo administration of AZD5153 led to tumor stasis or regression in multiple xenograft models of acute myeloid leukemia, multiple myeloma, and diffuse large B-cell lymphoma. The relationship between AZD5153 exposure and efficacy suggests that prolonged BRD4 target coverage is a primary efficacy driver. AZD5153 treatment markedly affects transcriptional programs of MYC, E2F, and mTOR. Of note, mTOR pathway modulation is associated with cell line sensitivity to AZD5153. Transcriptional modulation of MYC and HEXIM1 was confirmed in AZD5153-treated human whole blood, thus supporting their use as clinical pharmacodynamic biomarkers. This study establishes AZD5153 as a highly potent, orally available BET/BRD4 inhibitor and provides a rationale for clinical development in hematologic malignancies. Mol Cancer Ther; 15(11); 2563–74. ©2016 AACR.

Published
2023

13. Supplementary Table 2 from AZD5153: A Novel Bivalent BET Bromodomain Inhibitor Highly Active against Hematologic Malignancies

Author

Huawei Chen, Edwin Clark, Michael Zinda, Michael J. Waring, Stephen E. Fawell, Gordon B. Mills, Paul Lyne, Corinne Reimer, Jonathan R. Dry, Alfred A. Rabow, Tammie C. Yeh, Greg O'Connor, Graeme Walker, Miika J. Ahdesmaki, Larry Bao, Michael Collins, Deborah Lawson, Lillian Castriotta, Shenghua Wen, Jingwen Zhang, Tony Cheung, Scott Boiko, Ian L. Dale, Philip Petteruti, Wenxian Wang, Austin Dulak, Yi Yao, Maureen M. Hattersley, and Garrett W. Rhyasen

Abstract

Differentially expressed genes with AZD5153 treatment

Published
2023

14. Supplementary Figures 1-8 from The Mechanisms of Differential Sensitivity to an Insulin-like Growth Factor-1 Receptor Inhibitor (BMS-536924) and Rationale for Combining with EGFR/HER2 Inhibitors

Author

Joan M. Carboni, Ashok Dongre, Ricardo M. Attar, Lee Helman, Edwin Clark, Marco M. Gottardis, Francis Y. Lee, Aixin Li, Douglas Robinson, Jiwen Chen, Karen Reeves, Gayle M. Wittenberg, Rameh Hafezi, Xia Han, Warren Hurlburt, Ann Greer, and Fei Huang

Abstract

Supplementary Figures 1-8 from The Mechanisms of Differential Sensitivity to an Insulin-like Growth Factor-1 Receptor Inhibitor (BMS-536924) and Rationale for Combining with EGFR/HER2 Inhibitors

Published
2023

15. Supplementary Tables 1-4 from The Mechanisms of Differential Sensitivity to an Insulin-like Growth Factor-1 Receptor Inhibitor (BMS-536924) and Rationale for Combining with EGFR/HER2 Inhibitors

Author

Joan M. Carboni, Ashok Dongre, Ricardo M. Attar, Lee Helman, Edwin Clark, Marco M. Gottardis, Francis Y. Lee, Aixin Li, Douglas Robinson, Jiwen Chen, Karen Reeves, Gayle M. Wittenberg, Rameh Hafezi, Xia Han, Warren Hurlburt, Ann Greer, and Fei Huang

Abstract

Supplementary Tables 1-4 from The Mechanisms of Differential Sensitivity to an Insulin-like Growth Factor-1 Receptor Inhibitor (BMS-536924) and Rationale for Combining with EGFR/HER2 Inhibitors

Published
2023

16. Supplementary Information and Figures 1-3 from Identification of Candidate Molecular Markers Predicting Sensitivity in Solid Tumors to Dasatinib: Rationale for Patient Selection

Author

Edwin Clark, Peter Shaw, Francis Lee, Tai W. Wong, Suso Platero, Craig Fairchild, Xia Han, Karen Reeves, and Fei Huang

Abstract

Supplementary Information and Figures 1-3 from Identification of Candidate Molecular Markers Predicting Sensitivity in Solid Tumors to Dasatinib: Rationale for Patient Selection

Published
2023

17. The integer sequence transform a → b, where bn is the number of real roots of the polynomial a0 + a1x + a2x2 + · · · + anxn.

Author

Edwin Clark, W. and Shattuck, Mark

Subjects
POLYNOMIALS, INTEGERS, CATALAN numbers, BINOMIAL coefficients, GENERATING functions
Abstract

We discuss the integer sequence transform a 1→ b, where bn is the number of real roots of the polynomial a0 + a1x + a2x2 + · · · + anxn. It is shown that several sequences a give the trivial sequence b = (0, 1, 0, 1, 0, 1,...), i.e., bn = n mod 2, among them the Catalan numbers, central binomial coefficients, n! and for a fixed k. We also look at some sequences a for which b is more interesting such as an = (n + 1)k for k ≥ 3. Further, general procedures are given for constructing real sequences an for which bn is either always maximal or minimal. [ABSTRACT FROM AUTHOR]

Published
2023
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19. TU5.8 Audit on Adherence to NICE Guidelines for VTE Prophylaxis in Patients Undergoing Surgery for Appendicitis

Author

Sreekar Devarakonda, Paul Shuttleworth, and Edwin Clark

Subjects
Surgery
Abstract

Background and Aims According to the Nice Guidelines (NG89), for any person (over 16 years) undergoing abdominal surgery, pharmacological VTE prophylaxis must be added for a minimum of 7 days (if the risk of VTE outweighs the risk of bleeding). Also, mechanical VTE prophylaxis must commence on admission. We wanted to audit our adherence to these guidelines in the patients undergoing surgery for appendicitis. Methods A review of the electronic pharmacy records of the patients (over 16 years) who underwent surgery for appendicitis (proven with a CT scan or diagnosed intra-operatively) was performed from October to December 2021. We used the Department of Health VTE risk assessment form, and only the patients whose risk of VTE outweighed the bleeding risk were included. Results Of the 23 patients, 22 (95.6%) underwent laparoscopic appendicectomy and, open appendicectomy was done in 1 (4.4%) patient. 11 (47.8%) patients were females, and 12 (52.2%) were males. The mean age was 38.3 (±16) years, and the mean duration of hospital stay was 2.8 (±1.6) days. VTE risk assessment form was completed only for 12 (52.2%) patients. During the hospital stay, 15 of 23 (65.2%) patients received TEDS, and 18 (78.2%) patients received Enoxaparin. 4 (17.4%) patients did not receive any form of VTE prophylaxis. None of these patients was prescribed seven days of pharmacological prophylaxis. Conclusions VTE prophylaxis prescription in patients with short hospital stays is often missed. We must explore the necessary interventions to ensure that patients are given seven days of VTE prophylaxis and regularly audit this practice.

Published
2022

20. Discovery of Mcl-1-specific inhibitor AZD5991 and preclinical activity in multiple myeloma and acute myeloid leukemia

Author

Nancy Su, Brian Aquila, Gareth P. Gregory, Stephen Fawell, J. Adam Hendricks, Ammar Adam, Lawrence H. Boise, Jeffrey W. Johannes, Kevin J. Embrey, Edwin Clark, Philip B. Rawlins, Justin Cidado, Francis D. Gibbons, Ricky W. Johnstone, Qing Ye, Elisabetta Chiarparin, Steven L. Kazmirski, Michelle Lamb, J. Paul Secrist, Wenzhan Yang, Alexander Hird, Daniel W. Robbins, Adriana E. Tron, Alwin Schuller, Martin J. Packer, David J. Hargreaves, Xiaolan Zheng, Matthew A. Belmonte, Eric Gangl, Ajay K. Nooka, Shannon M. Matulis, Jason Grant Kettle, Bo Peng, and David Matthew Wilson

Subjects
0301 basic medicine, Myeloid, General Physics and Astronomy, Apoptosis, Mice, SCID, medicine.disease_cause, Crystallography, X-Ray, Bortezomib, chemistry.chemical_compound, Mice, 0302 clinical medicine, immune system diseases, hemic and lymphatic diseases, lcsh:Science, Multiple myeloma, Sulfonamides, Multidisciplinary, Myeloid leukemia, Leukemia, Leukemia, Myeloid, Acute, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Multiple Myeloma, medicine.drug, Science, Antineoplastic Agents, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Rats, Nude, Cell Line, Tumor, medicine, Animals, Humans, neoplasms, Venetoclax, business.industry, General Chemistry, medicine.disease, Bridged Bicyclo Compounds, Heterocyclic, Xenograft Model Antitumor Assays, Rats, Mice, Inbred C57BL, 030104 developmental biology, chemistry, Cancer cell, Cancer research, Myeloid Cell Leukemia Sequence 1 Protein, lcsh:Q, Carcinogenesis, business
Abstract

Mcl-1 is a member of the Bcl-2 family of proteins that promotes cell survival by preventing induction of apoptosis in many cancers. High expression of Mcl-1 causes tumorigenesis and resistance to anticancer therapies highlighting the potential of Mcl-1 inhibitors as anticancer drugs. Here, we describe AZD5991, a rationally designed macrocyclic molecule with high selectivity and affinity for Mcl-1 currently in clinical development. Our studies demonstrate that AZD5991 binds directly to Mcl-1 and induces rapid apoptosis in cancer cells, most notably myeloma and acute myeloid leukemia, by activating the Bak-dependent mitochondrial apoptotic pathway. AZD5991 shows potent antitumor activity in vivo with complete tumor regression in several models of multiple myeloma and acute myeloid leukemia after a single tolerated dose as monotherapy or in combination with bortezomib or venetoclax. Based on these promising data, a Phase I clinical trial has been launched for evaluation of AZD5991 in patients with hematological malignancies (NCT03218683)., High expression of Mcl-1 promotes tumorigenesis and resistance to anticancer therapies. Here they report a macrocyclic molecule with high selectivity and affinity for Mcl-1 that exhibits potent anti-tumor effects as single agent and in combination with bortezomib or venetoclax in preclinical models of multiple myeloma and acute myeloid leukemia.

Published
2018

21. Algebraic properties of quandle extensions and values of cocycle knot invariants

Author

W. Edwin Clark and Masahico Saito

Subjects
Algebraic properties, Pure mathematics, Algebra and Number Theory, 010102 general mathematics, Abelian extension, 0102 computer and information sciences, 01 natural sciences, Mathematics::Algebraic Topology, Mathematics::Geometric Topology, Article, Knot (unit), 010201 computation theory & mathematics, Mathematics::Quantum Algebra, 0101 mathematics, Algebraic number, Invariant (mathematics), Mathematics
Abstract

Quandle 2-cocycles define invariants of classical and virtual knots, and extensions of quandles. We show that the quandle 2-cocycle invariant with respect to a non-trivial [Formula: see text]-cocycle is constant, or takes some other restricted form, for classical knots when the corresponding extensions satisfy certain algebraic conditions. In particular, if an abelian extension is a conjugation quandle, then the corresponding cocycle invariant is constant. Specific examples are presented from the list of connected quandles of order less than 48. Relations among various quandle epimorphisms involved are also examined.

Published
2021

22. q-Analogue of a binomial coefficient congruence

Author

W. Edwin Clark

Subjects
binomial coefficient, partition, congruence, cyclotomic polynomial, q-analogue., Mathematics, QA1-939
Abstract

We establish a q-analogue of the congruence (papb)≡(ab) (modp2) where p is a prime and a and b are positive integers.

Published
1995
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23. Glad greetings from New England

Author

William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, U.S. Department of Agriculture, National Agricultural Library, William Edwin Clark (Firm), Clark, William Edwin, and Henry G. Gilbert Nursery and Seed Trade Catalog Collection

Subjects
Bulbs (Plants), Gladiolus, Massachusetts, Nursery stock, Prices, Roots, Sharon, Varieties
Published
1941

24. Glad greetings from New England

Author

William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, U.S. Department of Agriculture, National Agricultural Library, William Edwin Clark (Firm), Clark, William Edwin, and Henry G. Gilbert Nursery and Seed Trade Catalog Collection

Subjects
Bulbs (Plants), Gladiolus, Massachusetts, Nursery stock, Prices, Roots, Sharon, Varieties
Published
1940

25. Glad greetings from New England

Author

William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, U.S. Department of Agriculture, National Agricultural Library, William Edwin Clark (Firm), Clark, William Edwin, and Henry G. Gilbert Nursery and Seed Trade Catalog Collection

Subjects
Bulbs (Plants), Gladiolus, Massachusetts, Nursery stock, Prices, Roots, Sharon, Varieties
Published
1939

26. Glad greetings from New England /

Author

William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, U.S. Department of Agriculture, National Agricultural Library, William Edwin Clark (Firm), Clark, William Edwin, and Henry G. Gilbert Nursery and Seed Trade Catalog Collection

Subjects
Bulbs (Plants), Gladiolus, Massachusetts, Nursery stock, Prices, Roots, Sharon, Varieties
Published
1938

27. Glad greetings from New England /

Author

William Edwin Clark (Firm), Clark, William Edwin, Sunnymede Gardens, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, U.S. Department of Agriculture, National Agricultural Library, William Edwin Clark (Firm), Clark, William Edwin, Sunnymede Gardens, and Henry G. Gilbert Nursery and Seed Trade Catalog Collection

Subjects
Bulbs (Plants), Gladiolus, Massachusetts, Nursery stock, Prices, Roots, Sharon, Varieties
Published
1937

28. Glad greetings from New England /

Author

William Edwin Clark (Firm), Clark, William Edwin, Sunnymede Gardens, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, U.S. Department of Agriculture, National Agricultural Library, William Edwin Clark (Firm), Clark, William Edwin, Sunnymede Gardens, and Henry G. Gilbert Nursery and Seed Trade Catalog Collection

Subjects
Bulbs (Plants), Gladiolus, Massachusetts, Nursery stock, Prices, Roots, Sharon, Varieties
Published
1936

29. Glad greetings from New England /

Author

William Edwin Clark (Firm), Clark, William Edwin, Sunnymede Gardens, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, U.S. Department of Agriculture, National Agricultural Library, William Edwin Clark (Firm), Clark, William Edwin, Sunnymede Gardens, and Henry G. Gilbert Nursery and Seed Trade Catalog Collection

Subjects
Bulbs (Plants), Gladiolus, Massachusetts, Nursery stock, Prices, Roots, Sharon, Varieties
Published
1934

30. Glad greetings from New England /

Author

William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, Sunnymede Gardens, U.S. Department of Agriculture, National Agricultural Library, William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, and Sunnymede Gardens

Subjects
Bulbs (Plants), Gladiolus, Massachusetts, Nursery stock, Prices, Roots, Sharon, Varieties
Published
1933

31. 1932 / 1931 glad greetings from New England /

Author

William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, Sunnymede Gardens, U.S. Department of Agriculture, National Agricultural Library, William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, and Sunnymede Gardens

Subjects
Bulbs (Plants), Gladiolus, Massachusetts, Nurseries (Horticulture), Nursery stock, Prices, Roots, Sharon, Varieties
Published
1932

32. 1931 Glad greetings from New England /

Author

William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, Sunnymede Gardens, U.S. Department of Agriculture, National Agricultural Library, William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, and Sunnymede Gardens

Subjects
Bulbs (Plants), Gladiolus, Massachusetts, Nurseries (Horticulture), Nursery stock, Prices, Roots, Sharon, Varieties
Published
1931

33. 1931 Glad greetings from New England : wholesale list for 1931 /

Author

William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, Sunnymede Gardens, U.S. Department of Agriculture, National Agricultural Library, William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, and Sunnymede Gardens

Subjects
Bulbs (Plants), Gladiolus, Massachusetts, Nursery stock, Prices, Roots, Seeds, Sharon, Varieties, Wholesale trade
Published
1931

34. 1930 Glad greetings from New England /

Author

William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, Sunnymede Gardens, U.S. Department of Agriculture, National Agricultural Library, William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, and Sunnymede Gardens

Subjects
Bulbs (Plants), Gladiolus, Massachusetts, Nurseries (Horticulture), Nursery stock, Prices, Roots, Sharon, Varieties
Published
1930

35. Glad greetings from New England : [price list] /

Author

William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, Sunnymede Gardens, U.S. Department of Agriculture, National Agricultural Library, William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, and Sunnymede Gardens

Subjects
Bulbs (Plants), Gladiolus, Massachusetts, Nurseries (Horticulture), Nursery stock, Prices, Roots, Sharon, Varieties
Published
1929

36. Glad greetings from New England : wholesale gladiolus list, 1928-1929 /

Author

William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, Sunnymede Gardens, U.S. Department of Agriculture, National Agricultural Library, William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, and Sunnymede Gardens

Subjects
Bulbs (Plants), Gladiolus, Massachusetts, Nurseries (Horticulture), Nursery stock, Prices, Roots, Sharon, Varieties
Published
1928

37. Glad greetings from New England : wholesale gladiolus list, 1927-1928 /

Author

William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, Sunnymede Gardens, U.S. Department of Agriculture, National Agricultural Library, William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, and Sunnymede Gardens

Subjects
Bulbs (Plants), Gladiolus, Massachusetts, Nursery stock, Prices, Roots, Sharon, Varieties
Published
1927

38. Iris price list /

Author

Mrs. William Edwin Clark (Firm), Clark, William Edwin, Mrs, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, Sunnymede Gardens, U.S. Department of Agriculture, National Agricultural Library, Mrs. William Edwin Clark (Firm), Clark, William Edwin, Mrs, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, and Sunnymede Gardens

Subjects
Bulbs (Plants), Irises (Plants), Massachusetts, Nursery stock, Prices, Sharon, Varieties
Published
1926

39. Wholesale gladiolus list 1925-1926 ; Recent Gersdorff ratings of Fischer varieties ; Favorite gladioli /

Author

William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, Sunnymede Gardens, U.S. Department of Agriculture, National Agricultural Library, William Edwin Clark (Firm), Clark, William Edwin, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, and Sunnymede Gardens

Subjects
Bulbs (Plants), Gladiolus, Massachusetts, Nursery stock, Prices, Sharon, Varieties
Published
1925

40. Gladioli [catalog] /

Author

Sunnymede Gardens, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, Mrs. William Edwin Clark (Firm), U.S. Department of Agriculture, National Agricultural Library, Sunnymede Gardens, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, and Mrs. William Edwin Clark (Firm)

Subjects
Bulbs (Plants), Catalogs, Gladiolus, Massachusetts, Nursery stock, Roots, Sharon
Published
1924

41. Sunnymede Gardens [irises and gladioli catalog] /

Author

Sunnymede Gardens, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, Mrs. William Edwin Clark (Firm), U.S. Department of Agriculture, National Agricultural Library, Sunnymede Gardens, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, and Mrs. William Edwin Clark (Firm)

Subjects
Bulbs (Plants), Catalogs, Gladiolus, Irises (Plants), Massachusetts, Nursery stock, Roots, Sharon
Published
1924

42. Sunnymede Gardens [catalog] /

Author

Sunnymede Gardens, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, Mrs. William Edwin Clark (Firm), U.S. Department of Agriculture, National Agricultural Library, Sunnymede Gardens, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, and Mrs. William Edwin Clark (Firm)

Subjects
Bulbs (Plants), Catalogs, Flowers, Massachusetts, Nursery stock, Seeds, Sharon
Published
1923

43. Sunnymede Gardens [catalog] /

Author

Sunnymede Gardens, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, Mrs. William Edwin Clark (Firm), U.S. Department of Agriculture, National Agricultural Library, Sunnymede Gardens, Henry G. Gilbert Nursery and Seed Trade Catalog Collection, and Mrs. William Edwin Clark (Firm)

Subjects
Bulbs (Plants), Catalogs, Flowers, Massachusetts, Nursery stock, Seeds, Sharon
Published
1922

44. Biomarker-Based Phase II Trial of Savolitinib in Patients With Advanced Papillary Renal Cell Cancer

Author

Elizabeth R. Plimack, Daniel Y.C. Heng, Amir Handzel, Melanie M. Frigault, Toni K. Choueiri, Humphrey Gardner, Shethah Morgan, Hendrik Tobias Arkenau, Edwin Clark, Eric Jonasch, Laurence Albiges, Sumanta K. Pal, and Thomas Powles

Subjects
Adult, Male, 0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Pathology, C-Met, medicine.drug_class, Administration, Oral, Phases of clinical research, Kaplan-Meier Estimate, Disease-Free Survival, Tyrosine-kinase inhibitor, Young Adult, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Internal medicine, Biomarkers, Tumor, medicine, Carcinoma, Humans, Carcinoma, Renal Cell, Aged, Aged, 80 and over, Papillary renal cell carcinomas, Triazines, business.industry, Sunitinib, Middle Aged, Proto-Oncogene Proteins c-met, medicine.disease, Kidney Neoplasms, 030104 developmental biology, chemistry, Savolitinib, Pyrazines, 030220 oncology & carcinogenesis, Biomarker (medicine), Female, business, medicine.drug
Abstract

Purpose Patients with advanced papillary renal cell carcinoma (PRCC) have limited therapeutic options. PRCC may involve activation of the MET pathway, for example, through gene amplification or mutations. Savolitinib (AZD6094, HMPL-504, volitinib) is a highly selective MET tyrosine kinase inhibitor. We report results of a single-arm, multicenter, phase II study evaluating the safety and efficacy of savolitinib in patients with PRCC according to MET status. Patients and Methods Patients with histologically confirmed locally advanced or metastatic PRCC were enrolled and received savolitinib 600 mg orally once daily. MET-driven PRCC was defined as any of the following: chromosome 7 copy gain, focal MET or HGF gene amplification, or MET kinase domain mutations. Efficacy was assessed according to MET status. Safety, toxicity, and patient-reported health-related quality-of-life outcomes were assessed in all patients. Results Of 109 patients treated, PRCC was MET driven in 44 (40%) and MET independent in 46 (42%); MET status was unknown in 19 (17%). MET-driven PRCC was strongly associated with response; there were eight confirmed partial responders with MET-driven disease (18%), but none with MET-independent disease ( P = .002). Median progression-free survival for patients with MET-driven and MET-independent PRCC was 6.2 months (95% CI, 4.1 to 7.0 months) and 1.4 months (95% CI, 1.4 to 2.7 months), respectively (hazard ratio, 0.33; 95% CI, 0.20 to 0.52; log-rank P < .001). The most frequent adverse events associated with savolitinib were nausea, fatigue, vomiting, and peripheral edema. Conclusion These data show activity and tolerability of savolitinib in the subgroup of patients with MET-driven PRCC. Furthermore, molecular characterization of MET status was more predictive of response to savolitinib than a classification based on pathology. These findings justify investigating savolitinib in MET-driven PRCC.

Published
2017

45. Translational Modeling of Drug-Induced Myelosuppression and Effect of Pretreatment Myelosuppression for AZD5153, a Selective BRD4 Inhibitor

Author

Teresa Collins, Madhu Mondal, Maureen Hattersley, Jerome T. Mettetal, James W.T. Yates, and Edwin Clark

Subjects
0301 basic medicine, Drug, BRD4, Myeloid, business.industry, media_common.quotation_subject, Blood count, Myeloid leukemia, Pharmacology, medicine.disease, 03 medical and health sciences, Leukemia, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Modeling and Simulation, medicine, Pharmacology (medical), Platelet, Bone marrow, business, media_common
Abstract

In this work, we evaluate the potential risk of thrombocytopenia in man for a BRD4 inhibitor, AZD5153, based on the platelet count decreases from a Han Wistar rat study. The effects in rat were modeled and used to make clinical predictions for human populations with healthy baseline blood counts. At doses >10 mg, a dose-dependent effect on circulating platelets is expected, with similar predicted changes for both q.d. and b.i.d. dose schedules. These results suggest that at predicted efficacious doses, AZD5153 is likely to have some reductions in the clinical platelet counts, but within the normal range at projected efficacious doses. The model was then extended to incorporate preexisting myelosuppression where bone marrow function is inhibited by acute myeloid leukemia. Under these conditions, duration of platelet count recovery has the potential to be prolonged due to drug-induced myelosuppression.

Published
2017

46. Algebraic and Computational Aspects of Quandle 2-Cocycle Invariant

Author

W. Edwin Clark and Masahico Saito

Subjects
Algebraic properties, Pure mathematics, Knot (unit), Mathematics::K-Theory and Homology, Mathematics::Quantum Algebra, Algebraic number, Homology (mathematics), Invariant (mathematics), Mathematics::Algebraic Topology, Mathematics::Geometric Topology, Mathematics
Abstract

Quandle homology theories have been developed and cocycles have been used to construct invariants in state-sum form for knots using colorings of knot diagrams by quandles. Quandle 2-cocycles can be also used to define extensions as in the case of groups. There are relations among algebraic properties of quandles, their homology theories, and cocycle invariants; certain algebraic properties of quandles affect the values of the cocycle invariants, and identities satisfied by quandles induce subcomplexes of homology theory. Recent developments in these matters, as well as computational aspects of the invariant, are reviewed. Problems and conjectures pertinent to the subject are also listed.

Published
2019

47. Potent and selective bivalent inhibitors of BET bromodomains

Author

Dmitri I. Svergun, Huawei Chen, Romel Bobby, Natalie Stratton, Danette L. Daniels, Scott Boiko, Rowena Callis, Yi Yao, Graeme R. Robb, Alfred A. Rabow, Mark S. B. McAlister, Graeme Walker, Joe Patel, Matthew B. Robers, Derek Ogg, Sakina Saif, Liz Flavell, Philip Petteruti, Austin Dulak, Ian L. Dale, Jacqui Méndez, Thomas A. Jowitt, Michael J. Waring, David Matthew Wilson, David Whittaker, Wenxian Wang, Edwin Clark, Alexey Kikhney, Geoff Holdgate, and Rob H. Bradbury

Subjects
0301 basic medicine, BRD4, Chemistry, Stereochemistry, Ligand, Protein subunit, Cell Biology, Bivalent (genetics), Bromodomain, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Biochemistry, 030220 oncology & carcinogenesis, Molecular Biology
Abstract

Proteins of the bromodomain and extraterminal (BET) family, in particular bromodomain-containing protein 4 (BRD4), are of great interest as biological targets. BET proteins contain two separate bromodomains, and existing inhibitors bind to them monovalently. Here we describe the discovery and characterization of probe compound biBET, capable of engaging both bromodomains simultaneously in a bivalent, in cis binding mode. The evidence provided here was obtained in a variety of biophysical and cellular experiments. The bivalent binding results in very high cellular potency for BRD4 binding and pharmacological responses such as disruption of BRD4-mediator complex subunit 1 foci with an EC50 of 100 pM. These compounds will be of considerable utility as BET/BRD4 chemical probes. This work illustrates a novel concept in ligand design-simultaneous targeting of two separate domains with a drug-like small molecule-providing precedent for a potentially more effective paradigm for developing ligands for other multi-domain proteins.

Published
2016

48. Optimization of a Series of Bivalent Triazolopyridazine Based Bromodomain and Extraterminal Inhibitors: The Discovery of (3R)-4-[2-[4-[1-(3-Methoxy-[1,2,4]triazolo[4,3-b]pyridazin-6-yl)-4-piperidyl]phenoxy]ethyl]-1,3-dimethyl-piperazin-2-one (AZD5153)

Author

Joe Patel, Mark A. Graham, Maureen Hattersley, Stephen Stokes, David Whittaker, Carr Gregory Richard, David Whalley, Edwin Clark, Craig A. Roberts, Gail L. Wrigley, Alfred A. Rabow, Graeme Walker, Christopher R. Jones, Natalie Stratton, Michael J. Waring, Rowena Callis, Lyman Feron, Robert Hugh Bradbury, Steve C. Glossop, Huawei Chen, Lara Ward, Anil Patel, Gilles Ouvry, and Scott G. Lamont

Subjects
0301 basic medicine, Chemistry, Stereochemistry, Stereoisomerism, Combinatorial chemistry, Bivalent (genetics), In vitro, Bromodomain, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, In vivo, 030220 oncology & carcinogenesis, Drug Discovery, Molecular Medicine, Structure–activity relationship, Potency, Tumor growth inhibition
Abstract

Here we report the discovery and optimization of a series of bivalent bromodomain and extraterminal inhibitors. Starting with the observation of BRD4 activity of compounds from a previous program, the compounds were optimized for BRD4 potency and physical properties. The optimized compound from this campaign exhibited excellent pharmacokinetic profile and exhibited high potency in vitro and in vivo effecting c-Myc downregulation and tumor growth inhibition in xenograft studies. This compound was selected as the development candidate, AZD5153. The series showed enhanced potency as a result of bivalent binding and a clear correlation between BRD4 activity and cellular potency.

Published
2016

50. BRD4 amplification facilitates an oncogenic gene expression program in high-grade serous ovarian cancer and confers sensitivity to BET inhibitors

Author

Kelly Jacques, Michael Zinda, Gordon B. Mills, Lillian Castriotta, Farzin Gharahdaghi, Edwin Clark, Stephen Fawell, Wei Zhao, Garrett W. Rhyasen, Austin Dulak, Huawei Chen, Jingwen Zhang, Yi Yao, Paul Lyne, and Maureen Hattersley

Subjects
0301 basic medicine, Carcinogenesis, Cancer Treatment, Gene Expression, lcsh:Medicine, Cell Cycle Proteins, medicine.disease_cause, Piperazines, Mice, 0302 clinical medicine, Medicine and Health Sciences, E2F1, lcsh:Science, Ovarian Neoplasms, Regulation of gene expression, Multidisciplinary, Chromosome Biology, Nuclear Proteins, Chromatin, Ovarian Cancer, Precipitation Techniques, 3. Good health, Gene Expression Regulation, Neoplastic, Pyridazines, Oncology, 030220 oncology & carcinogenesis, Female, Epigenetics, Algorithms, Signal Transduction, Research Article, BRD4, Neuregulin-1, Immunoblotting, Molecular Probe Techniques, Antineoplastic Agents, Biology, Research and Analysis Methods, Heterocyclic Compounds, 2-Ring, BET inhibitor, 03 medical and health sciences, Cell Line, Tumor, Genetics, medicine, Animals, Humans, Immunoprecipitation, Molecular Biology Techniques, Molecular Biology, Cell Proliferation, Gene Expression Profiling, lcsh:R, Gene Amplification, Proteins, Cancers and Neoplasms, Biology and Life Sciences, Cell Biology, medicine.disease, Xenograft Model Antitumor Assays, Cystadenocarcinoma, Serous, Gene expression profiling, 030104 developmental biology, Cancer research, Pyrazoles, lcsh:Q, Ovarian cancer, Gynecological Tumors, Neoplasm Transplantation, Transcription Factors
Abstract

BRD4 is a transcriptional co-activator functioning to recruit regulatory complexes to acetylated chromatin. A subset of High-grade Serous Ovarian Cancer (HGSOC) patients are typified by focal, recurrent BRD4 gene amplifications. Despite previously described cancer dependencies, it is unclear whether BRD4 amplification events are oncogenic in HGSOC. We find that physiologically relevant levels of expression of BRD4 isoforms in non-transformed ovarian cells result in cellular transformation. Transcriptional profiling of BRD4-transformed ovarian cells, and BRD4-amplified HGSOC patient samples revealed shared expression patterns, including enriched MYC, and E2F1 gene signatures. Furthermore, we demonstrate that a novel BET inhibitor, AZD5153, is highly active in BRD4-amplified patient derived xenografts and uncover Neuregulin-1 as a novel BRD4 effector. Experiments involving Neuregulin-1 inhibition and exogenous addition, demonstrate Neuregulin-1 as necessary and sufficient for BRD4-mediated transformation. This study demonstrates the oncogenic potential of BRD4 amplification in cancer and establishes BRD4-amplified HGSOC as a potential patient population that could benefit from BET inhibitors.

Published
2018

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