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1. Data from CEP-28122, a Highly Potent and Selective Orally Active Inhibitor of Anaplastic Lymphoma Kinase with Antitumor Activity in Experimental Models of Human Cancers

Author

Cheng, Mangeng, primary, Quail, Matthew R., primary, Gingrich, Diane E., primary, Ott, Gregory R., primary, Lu, Lihui, primary, Wan, Weihua, primary, Albom, Mark S., primary, Angeles, Thelma S., primary, Aimone, Lisa D., primary, Cristofani, Flavio, primary, Machiorlatti, Rodolfo, primary, Abele, Cristina, primary, Ator, Mark A., primary, Dorsey, Bruce D., primary, Inghirami, Giorgio, primary, and Ruggeri, Bruce A., primary

Published
2023
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2. Supplementary Figure 3 from CEP-28122, a Highly Potent and Selective Orally Active Inhibitor of Anaplastic Lymphoma Kinase with Antitumor Activity in Experimental Models of Human Cancers

Author

Cheng, Mangeng, primary, Quail, Matthew R., primary, Gingrich, Diane E., primary, Ott, Gregory R., primary, Lu, Lihui, primary, Wan, Weihua, primary, Albom, Mark S., primary, Angeles, Thelma S., primary, Aimone, Lisa D., primary, Cristofani, Flavio, primary, Machiorlatti, Rodolfo, primary, Abele, Cristina, primary, Ator, Mark A., primary, Dorsey, Bruce D., primary, Inghirami, Giorgio, primary, and Ruggeri, Bruce A., primary

Published
2023
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3. Supplementary Table 1, Figures 1-2 from CEP-28122, a Highly Potent and Selective Orally Active Inhibitor of Anaplastic Lymphoma Kinase with Antitumor Activity in Experimental Models of Human Cancers

Author

Cheng, Mangeng, primary, Quail, Matthew R., primary, Gingrich, Diane E., primary, Ott, Gregory R., primary, Lu, Lihui, primary, Wan, Weihua, primary, Albom, Mark S., primary, Angeles, Thelma S., primary, Aimone, Lisa D., primary, Cristofani, Flavio, primary, Machiorlatti, Rodolfo, primary, Abele, Cristina, primary, Ator, Mark A., primary, Dorsey, Bruce D., primary, Inghirami, Giorgio, primary, and Ruggeri, Bruce A., primary

Published
2023
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5. Discovery of Clinical Candidate CEP-37440, a Selective Inhibitor of Focal Adhesion Kinase (FAK) and Anaplastic Lymphoma Kinase (ALK)

Author

Ott, Gregory R., primary, Cheng, Mangeng, additional, Learn, Keith S., additional, Wagner, Jason, additional, Gingrich, Diane E., additional, Lisko, Joseph G., additional, Curry, Matthew, additional, Mesaros, Eugen F., additional, Ghose, Arup K., additional, Quail, Matthew R., additional, Wan, Weihua, additional, Lu, Lihui, additional, Dobrzanski, Pawel, additional, Albom, Mark S., additional, Angeles, Thelma S., additional, Wells-Knecht, Kevin, additional, Huang, Zeqi, additional, Aimone, Lisa D., additional, Bruckheimer, Elizabeth, additional, Anderson, Nathan, additional, Friedman, Jay, additional, Fernandez, Sandra V., additional, Ator, Mark A., additional, Ruggeri, Bruce A., additional, and Dorsey, Bruce D., additional

Published
2016
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6. Optimization of a novel kinase inhibitor scaffold for the dual inhibition of JAK2 and FAK kinases

Author

Zificsak, Craig A., Gingrich, Diane E., Breslin, Henry J., Dunn, Derek D., Milkiewicz, Karen L., Theroff, Jay P., Thieu, Tho V., Underiner, Ted L., Weinberg, Linda R., Aimone, Lisa D., Albom, Mark S., Mason, Jennifer L., Saville, Lisa, Husten, Jean, Angeles, Thelma S., Finn, James P., Jan, Mahfuza, O’Kane, Teresa M., Dobrzanski, Pawel, and Dorsey, Bruce D.

Published
2012
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8. A novel preparation of scalemic N-methyl-alfa-amino acids

Author

Dorow, R.L. and Gingrich, Diane E.

Subjects
Amino acids -- Synthesis, Biological sciences, Chemistry
Abstract

Alfa-azido acids can act as a starting material for the preparation of a wide range of scalemic N-methyl-alfa-amino compounds, namely phenyl- and tert-butylglycine. They are prepared by the reductive alkylation method. The esters produced by this reaction show a cleavage in their structures, and acids, amides and ethers are stable with respect to the reaction conditions. The change of borane group by the carbonyl group facilitates the reaction so that the haloboranes can react with azido acid derivatives.

Published
1995

9. A Selective, Orally Bioavailable 1,2,4-Triazolo[1,5-a]pyridine-Based Inhibitor of Janus Kinase 2 for Use in Anticancer Therapy: Discovery of CEP-33779

Author

Dugan, Benjamin J., primary, Gingrich, Diane E., additional, Mesaros, Eugen F., additional, Milkiewicz, Karen L., additional, Curry, Matthew A., additional, Zulli, Allison L., additional, Dobrzanski, Pawel, additional, Serdikoff, Cynthia, additional, Jan, Mahfuza, additional, Angeles, Thelma S., additional, Albom, Mark S., additional, Mason, Jennifer L., additional, Aimone, Lisa D., additional, Meyer, Sheryl L., additional, Huang, Zeqi, additional, Wells-Knecht, Kevin J., additional, Ator, Mark A., additional, Ruggeri, Bruce A., additional, and Dorsey, Bruce D., additional

Published
2012
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10. Discovery of an Orally Efficacious Inhibitor of Anaplastic Lymphoma Kinase

Author

Gingrich, Diane E., primary, Lisko, Joseph G., additional, Curry, Matthew A., additional, Cheng, Mangeng, additional, Quail, Matthew, additional, Lu, Lihui, additional, Wan, Weihua, additional, Albom, Mark S., additional, Angeles, Thelma S., additional, Aimone, Lisa D., additional, Haltiwanger, R. Curtis, additional, Wells-Knecht, Kevin, additional, Ott, Gregory R., additional, Ghose, Arup K., additional, Ator, Mark A., additional, Ruggeri, Bruce, additional, and Dorsey, Bruce D., additional

Published
2012
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11. CEP-28122, a Highly Potent and Selective Orally Active Inhibitor of Anaplastic Lymphoma Kinase with Antitumor Activity in Experimental Models of Human Cancers

Author

Cheng, Mangeng, primary, Quail, Matthew R., additional, Gingrich, Diane E., additional, Ott, Gregory R., additional, Lu, Lihui, additional, Wan, Weihua, additional, Albom, Mark S., additional, Angeles, Thelma S., additional, Aimone, Lisa D., additional, Cristofani, Flavio, additional, Machiorlatti, Rodolfo, additional, Abele, Cristina, additional, Ator, Mark A., additional, Dorsey, Bruce D., additional, Inghirami, Giorgio, additional, and Ruggeri, Bruce A., additional

Published
2012
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13. 2,7-Disubstituted-Pyrrolotriazine Kinase Inhibitors with an Unusually High Degree of Reactive Metabolite Formation

Author

Wells-Knecht, Kevin J., primary, Ott, Gregory R., additional, Cheng, Mangeng, additional, Wells, Gregory J., additional, Breslin, Henry J., additional, Gingrich, Diane E., additional, Weinberg, Linda, additional, Mesaros, Eugen F., additional, Huang, Zeqi, additional, Yazdanian, Mehran, additional, Ator, Mark A., additional, Aimone, Lisa D., additional, Zeigler, Kelli, additional, and Dorsey, Bruce D., additional

Published
2011
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14. Depletion of Autoreactive Plasma Cells and Treatment of Lupus Nephritis in Mice Using CEP-33779, a Novel, Orally Active, Selective Inhibitor of JAK2

Author

Lu, Lily D., primary, Stump, Kristine L., additional, Wallace, Nate H., additional, Dobrzanski, Pawel, additional, Serdikoff, Cynthia, additional, Gingrich, Diane E., additional, Dugan, Benjamin J., additional, Angeles, Thelma S., additional, Albom, Mark S., additional, Mason, Jennifer L., additional, Ator, Mark A., additional, Dorsey, Bruce D., additional, Ruggeri, Bruce A., additional, and Seavey, Matthew M., additional

Published
2011
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15. 2,7-Disubstituted-pyrrolo[2,1-f][1,2,4]triazines: New Variant of an Old Template and Application to the Discovery of Anaplastic Lymphoma Kinase (ALK) Inhibitors with in Vivo Antitumor Activity

Author

Ott, Gregory R., primary, Wells, Gregory J., additional, Thieu, Tho V., additional, Quail, Matthew R., additional, Lisko, Joseph G., additional, Mesaros, Eugen F., additional, Gingrich, Diane E., additional, Ghose, Arup K., additional, Wan, Weihua, additional, Lu, Lihui, additional, Cheng, Mangeng, additional, Albom, Mark S., additional, Angeles, Thelma S., additional, Huang, Zeqi, additional, Aimone, Lisa D., additional, Ator, Mark A., additional, Ruggeri, Bruce A., additional, and Dorsey, Bruce D., additional

Published
2011
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16. Abstract 3574: Identification and preclinical characterization of CEP-28122, a highly potent and selective orally active inhibitor of anaplastic lymphoma kinase, in lymphoma and non-small cell lung cancer models

Author

Cheng, Mangeng, primary, Quail, Matthew R., additional, Gingrich, Diane E., additional, Ott, Gregory R., additional, Lu, Lihui, additional, Wan, Weihua, additional, Albom, Mark S., additional, Angeles, Thelma S., additional, Aimone, Lisa D., additional, Cristofani, Flavio, additional, Machiorlatti, Rodolfo, additional, Abele, Cristina, additional, Ator, Mark A., additional, Dorsey, Bruce D., additional, Inghirami, Giorgio, additional, and Ruggeri, Bruce A., additional

Published
2011
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17. A highly selective, orally active inhibitor of Janus kinase 2, CEP-33779, ablates disease in two mouse models of rheumatoid arthritis

Author

Stump, Kristine L, primary, Lu, Lily D, additional, Dobrzanski, Pawel, additional, Serdikoff, Cynthia, additional, Gingrich, Diane E, additional, Dugan, Ben J, additional, Angeles, Thelma S, additional, Albom, Mark S, additional, Ator, Mark A, additional, Dorsey, Bruce D, additional, Ruggeri, Bruce A, additional, and Seavey, Matthew M, additional

Published
2011
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21. A New Class of Potent Vascular Endothelial Growth Factor Receptor Tyrosine Kinase Inhibitors: Structure−Activity Relationships for a Series of 9-Alkoxymethyl-12-(3-hydroxypropyl)indeno[2,1-a]pyrrolo[3,4-c]carbazole-5-ones and the Identification of CEP-5214 and Its Dimethylglycine Ester Prodrug Clinical Candidate CEP-7055

Author

Gingrich, Diane E., primary, Reddy, Dandu R., additional, Iqbal, Mohamed A., additional, Singh, Jasbir, additional, Aimone, Lisa D., additional, Angeles, Thelma S., additional, Albom, Mark, additional, Yang, Shi, additional, Ator, Mark A., additional, Meyer, Sheryl L., additional, Robinson, Candy, additional, Ruggeri, Bruce A., additional, Dionne, Craig A., additional, Vaught, Jeffry L., additional, Mallamo, John P., additional, and Hudkins, Robert L., additional

Published
2003
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28. A Selective, Orally Bioavailable1,2,4-Triazolo[1,5-a]pyridine-Based Inhibitor ofJanus Kinase 2 for Use inAnticancer Therapy: Discovery of CEP-33779.

Author

Dugan, Benjamin J., Gingrich, Diane E., Mesaros, Eugen F., Milkiewicz, Karen L., Curry, Matthew A., Zulli, Allison L., Dobrzanski, Pawel, Serdikoff, Cynthia, Jan, Mahfuza, Angeles, Thelma S., Albom, Mark S., Mason, Jennifer L., Aimone, Lisa D., Meyer, Sheryl L., Huang, Zeqi, Wells-Knecht, Kevin J., Ator, Mark A., Ruggeri, Bruce A., and Dorsey, Bruce D.

Subjects
*DRUG bioavailability, *PYRIDINE, *KINASE inhibitors, *ANTINEOPLASTIC agents, *CANCER invasiveness, *TUMOR growth, *TYROSINE, *TARGETED drug delivery, *STRUCTURE-activity relationships, *IMMUNOSUPPRESSION
Abstract

Members of the JAK family of nonreceptor tyrosine kinasesplaya critical role in the growth and progression of many cancers andin inflammatory diseases. JAK2 has emerged as a leading therapeutictarget for oncology, providing a rationale for the development ofa selective JAK2 inhibitor. A program to optimize selective JAK2 inhibitorsto combat cancer while reducing the risk of immune suppression associatedwith JAK3 inhibition was undertaken. The structure–activityrelationships and biological evaluation of a novel series of compoundsbased on a 1,2,4-triazolo[1,5-a]pyridine scaffoldare reported. Parasubstitution on the aryl at theC8 position of the core was optimum for JAK2 potency (17). Substitution at the C2 nitrogen position was required for cellpotency (21). Interestingly, metasubstitutionof C2-NH-aryl moiety provided exceptional selectivity for JAK2 overJAK3 (23). These efforts led to the discovery of CEP-33779(29), a novel, selective, and orally bioavailable inhibitorof JAK2. [ABSTRACT FROM AUTHOR]

Published
2012
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29. Discovery of an OrallyEfficacious Inhibitor of Anaplastic Lymphoma Kinase.

Author

Gingrich, Diane E., Lisko, Joseph G., Curry, Matthew A., Cheng, Mangeng, Quail, Matthew, Lu, Lihui, Wan, Weihua, Albom, Mark S., Angeles, Thelma S., Aimone, Lisa D., Haltiwanger, R. Curtis, Wells-Knecht, Kevin, Ott, Gregory R., Ghose, Arup K., Ator, Mark A., Ruggeri, Bruce, and Dorsey, Bruce D.

Subjects
*PHARMACEUTICAL research, *CANCER treatment, *ANAPLASTIC lymphoma kinase, *ENZYME inhibitors, *TARGETED drug delivery, *ANTINEOPLASTIC agents, *LABORATORY rats
Abstract

Anaplastic lymphoma kinase (ALK) is a promising therapeutictarget for the treatment of cancer, supported by considerable favorablepreclinical and clinical activities over the past several years andculminating in the recent FDA approval of the ALK inhibitor crizotinib.Through a series of targeted modifications on an ALK inhibitor diaminopyrimidinescaffold, our research group has driven improvements in ALK potency,kinase selectivity, and overall pharmaceutical properties. Optimizationof this scaffold has led to the identification of a potent and efficaciousinhibitor of ALK, 25b. A striking feature of 25bover previously described ALK inhibitors is its >600-fold selectivityover insulin receptor (IR), a closely related kinase family member.Most importantly, 25bexhibited dose proportional escalationin rat compared to compound 3which suffered dose limitingabsorption preventing further advancement. Compound 25bexhibited significant in vivo antitumorefficacy when dosed orally in an ALK-positive ALCL tumor xenograftmodel in SCID mice, warranting further assessment in advanced preclinicalmodels. [ABSTRACT FROM AUTHOR]

Published
2012
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32. A new class of potent vascular endothelial growth factor receptor tyrosine kinase inhibitors: structure-activity relationships for a series of 9-alkoxymethyl-12-(3-hydroxypropyl)indeno[2,1-a]pyrrolo[3,4-c]carbazole-5-ones and the identification of CEP-5214 and its dimethylglycine ester prodrug clinical candidate CEP-7055.

Author

Gingrich DE, Reddy DR, Iqbal MA, Singh J, Aimone LD, Angeles TS, Albom M, Yang S, Ator MA, Meyer SL, Robinson C, Ruggeri BA, Dionne CA, Vaught JL, Mallamo JP, and Hudkins RL

Subjects
Angiogenesis Inhibitors chemistry, Angiogenesis Inhibitors pharmacology, Animals, Carbazoles chemistry, Carbazoles pharmacology, Cells, Cultured, Drug Screening Assays, Antitumor, Endothelium, Vascular cytology, Endothelium, Vascular enzymology, Enzyme-Linked Immunosorbent Assay, Female, Hemangiosarcoma drug therapy, Humans, In Vitro Techniques, Indenes chemical synthesis, Indenes chemistry, Indenes pharmacology, Liver drug effects, Liver metabolism, Male, Mice, Mice, Nude, Models, Molecular, Phosphorylation, Prodrugs chemistry, Prodrugs pharmacology, Pyrroles chemical synthesis, Pyrroles chemistry, Pyrroles pharmacology, Rats, Rats, Sprague-Dawley, Solubility, Structure-Activity Relationship, Angiogenesis Inhibitors chemical synthesis, Carbazoles chemical synthesis, Prodrugs chemical synthesis, Sarcosine analogs & derivatives, Sarcosine chemistry, Vascular Endothelial Growth Factor Receptor-2 antagonists & inhibitors
Abstract

A series of potent vascular endothelial growth factor R2 (VEGF-R2) tyrosine kinase inhibitors from a new indenopyrrolocarbazole template is reported. The structure-activity relationships for a series of 9-alkoxymethyl-12-(3-hydroxypropyl)indeno[2,1-a]pyrrolo[3,4-c]carbazole-5-ones revealed an optimal R9 substitution with ethoxymethyl 19 (VEGF-R2 IC(50) = 4 nM) and isopropoxymethyl 21 (VEGF-R2 IC(50) = 8 nM) being the most potent inhibitors in the series. The VEGF-R2 activity was reduced appreciably by increasing the size of the R9 alkoxy group or by alpha-methyl branching adjacent to the ring. The combined R9 alkoxymethyl and N12 hydroxypropyl substitutions were required for potent VEGF-R2 activity, and the corresponding thioether analogues were weaker than their ether counterparts. Compound 21 (R9 isopropoxymethyl, CEP-5214) was identified as a potent, low-nanomolar pan inhibitor of human VEGF-R tyrosine kinases, displaying IC(50) values of 16, 8, and 4 nM for VEGF-R1/FLT-1, VEGF-R2/KDR, and VEGF-R3/FLT-4, respectively, with cellular activity equivalent to the isolated enzyme activity. Compound 21 exhibited good selectivity against numerous tyrosine and serine/threonine kinases including PKC, Tie2, TrkA, CDK1, p38, JNK, and IRK. To increase water solubility and oral bioavailability, the N,N-dimethylglycine ester 40 was prepared. In pharmacokinetic studies in mice and rats, increased plasma levels of 21 were observed after oral administration of 40. Compound 21 demonstrated significant in vivo antitumor activity in numerous tumor models and was advanced into phase I clinical trials as the water-soluble N,N-dimethylglycine ester prodrug 40 (CEP-7055).

Published
2003
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