Natural Product Libraries to Accelerate the High Throughput Discovery of Therapeutic Leads

Tyler Johnson; Johann Sohn; Wayne D Inman; Samarkand A. Estee; Steven T. Loveridge; Helene C. Vervoort; Karen Tenney; Junke Liu; Kenny Kean-Hooi Ang; Joseline Ratnam; Walter M. Bray; Nadine C Gassner; Young Y. Shen; R. Scott Lokey; James H McKerrow; Kyria Boundy-Mills; Arif Nukanto; Atit Kanti; Heddy Julistiono; Leonardus B.S. Kardono; Leonard F. Bjeldanes; Phillip Crews

doi:10.1021/np200673b

Natural Product Libraries to Accelerate the High Throughput Discovery of Therapeutic Leads

Tyler Johnson, Johann Sohn, Wayne D Inman, Samarkand A. Estee, Steven T. Loveridge, Helene C. Vervoort, Karen Tenney, Junke Liu, Kenny Kean-Hooi Ang, Joseline Ratnam, Walter M. Bray, Nadine C Gassner, Young Y. Shen, R. Scott Lokey, James H McKerrow, Kyria Boundy-Mills, Arif Nukanto, Atit Kanti, Heddy Julistiono, Leonardus B.S. KardonoLeonard F. Bjeldanes, Phillip Crews

Research output: Contribution to journal › Article › peer-review

Abstract

A high-throughput (HT) paradigm generating LC-MS-UV-ELSD-based natural product libraries to discover compounds with new bioactivities and or molecular structures is presented. To validate this methodology, an extract of the Indo-Pacific marine sponge Cacospongia mycofijiensis was evaluated using assays involving cytoskeletal profiling, tumor cell lines, and parasites. Twelve known compounds were identified including latrunculins (1–4, 10), fijianolides (5, 8, 9), mycothiazole (11), aignopsanes (6, 7), and sacrotride A (13). Compounds 1–5 and 8–11 exhibited bioactivity not previously reported against the parasite T. brucei, while 11 showed selectivity for lymphoma (U937) tumor cell lines. Four new compounds were also discovered including aignopsanoic acid B (13), apolatrunculin T (14), 20-methoxy-fijianolide A (15), and aignopsane ketal (16). Compounds 13 and 16 represent important derivatives of the aignopsane class, 14 exhibited inhibition of T. brucei without disrupting microfilament assembly, and 15 demonstrated modest microtubule-stabilizing effects. The use of removable well plate libraries to avoid false positives from extracts enriched with only one or two major metabolites is also discussed. Overall, these results highlight the advantages of applying modern methods in natural products-based research to accelerate the HT discovery of therapeutic leads and/or new molecular structures using LC-MS-UV-ELSD-based libraries.

Original language	American English
Pages (from-to)	2545-2555
Number of pages	11
Journal	Journal of Natural Products
Volume	74
Issue number	12
DOIs	https://doi.org/10.1021/np200673b
State	Published - Nov 30 2011
Externally published	Yes

Keywords

Cells
Drug Discovery
Ions
Pharmaceuticals
Screening Assays

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10.1021/np200673b

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Cite this

Johnson, T., Sohn, J., Inman, W. D., Estee, S. A., Loveridge, S. T., Vervoort, H. C., Tenney, K., Liu, J., Ang, K. K.-H., Ratnam, J., Bray, W. M., Gassner, N. C., Shen, Y. Y., Lokey, R. S., McKerrow, J. H., Boundy-Mills, K., Nukanto, A., Kanti, A., Julistiono, H., ... Crews, P. (2011). Natural Product Libraries to Accelerate the High Throughput Discovery of Therapeutic Leads. Journal of Natural Products, 74(12), 2545-2555. https://doi.org/10.1021/np200673b

Johnson, T, Sohn, J, Inman, WD, Estee, SA, Loveridge, ST, Vervoort, HC, Tenney, K, Liu, J, Ang, KK-H, Ratnam, J, Bray, WM, Gassner, NC, Shen, YY, Lokey, RS, McKerrow, JH, Boundy-Mills, K, Nukanto, A, Kanti, A, Julistiono, H, Kardono, LBS, Bjeldanes, LF & Crews, P 2011, 'Natural Product Libraries to Accelerate the High Throughput Discovery of Therapeutic Leads', Journal of Natural Products, vol. 74, no. 12, pp. 2545-2555. https://doi.org/10.1021/np200673b

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abstract = "A high-throughput (HT) paradigm generating LC-MS-UV-ELSD-based natural product libraries to discover compounds with new bioactivities and or molecular structures is presented. To validate this methodology, an extract of the Indo-Pacific marine sponge Cacospongia mycofijiensis was evaluated using assays involving cytoskeletal profiling, tumor cell lines, and parasites. Twelve known compounds were identified including latrunculins (1–4, 10), fijianolides (5, 8, 9), mycothiazole (11), aignopsanes (6, 7), and sacrotride A (13). Compounds 1–5 and 8–11 exhibited bioactivity not previously reported against the parasite T. brucei, while 11 showed selectivity for lymphoma (U937) tumor cell lines. Four new compounds were also discovered including aignopsanoic acid B (13), apolatrunculin T (14), 20-methoxy-fijianolide A (15), and aignopsane ketal (16). Compounds 13 and 16 represent important derivatives of the aignopsane class, 14 exhibited inhibition of T. brucei without disrupting microfilament assembly, and 15 demonstrated modest microtubule-stabilizing effects. The use of removable well plate libraries to avoid false positives from extracts enriched with only one or two major metabolites is also discussed. Overall, these results highlight the advantages of applying modern methods in natural products-based research to accelerate the HT discovery of therapeutic leads and/or new molecular structures using LC-MS-UV-ELSD-based libraries.",

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author = "Tyler Johnson and Johann Sohn and Inman, \{Wayne D\} and Estee, \{Samarkand A.\} and Loveridge, \{Steven T.\} and Vervoort, \{Helene C.\} and Karen Tenney and Junke Liu and Ang, \{Kenny Kean-Hooi\} and Joseline Ratnam and Bray, \{Walter M.\} and Gassner, \{Nadine C\} and Shen, \{Young Y.\} and Lokey, \{R. Scott\} and McKerrow, \{James H\} and Kyria Boundy-Mills and Arif Nukanto and Atit Kanti and Heddy Julistiono and Kardono, \{Leonardus B.S.\} and Bjeldanes, \{Leonard F.\} and Phillip Crews",

year = "2011",

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doi = "10.1021/np200673b",

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T1 - Natural Product Libraries to Accelerate the High Throughput Discovery of Therapeutic Leads

AU - Johnson, Tyler

AU - Sohn, Johann

AU - Inman, Wayne D

AU - Estee, Samarkand A.

AU - Loveridge, Steven T.

AU - Vervoort, Helene C.

AU - Tenney, Karen

AU - Liu, Junke

AU - Ang, Kenny Kean-Hooi

AU - Ratnam, Joseline

AU - Bray, Walter M.

AU - Gassner, Nadine C

AU - Shen, Young Y.

AU - Lokey, R. Scott

AU - McKerrow, James H

AU - Boundy-Mills, Kyria

AU - Nukanto, Arif

AU - Kanti, Atit

AU - Julistiono, Heddy

AU - Kardono, Leonardus B.S.

AU - Bjeldanes, Leonard F.

AU - Crews, Phillip

PY - 2011/11/30

Y1 - 2011/11/30

N2 - A high-throughput (HT) paradigm generating LC-MS-UV-ELSD-based natural product libraries to discover compounds with new bioactivities and or molecular structures is presented. To validate this methodology, an extract of the Indo-Pacific marine sponge Cacospongia mycofijiensis was evaluated using assays involving cytoskeletal profiling, tumor cell lines, and parasites. Twelve known compounds were identified including latrunculins (1–4, 10), fijianolides (5, 8, 9), mycothiazole (11), aignopsanes (6, 7), and sacrotride A (13). Compounds 1–5 and 8–11 exhibited bioactivity not previously reported against the parasite T. brucei, while 11 showed selectivity for lymphoma (U937) tumor cell lines. Four new compounds were also discovered including aignopsanoic acid B (13), apolatrunculin T (14), 20-methoxy-fijianolide A (15), and aignopsane ketal (16). Compounds 13 and 16 represent important derivatives of the aignopsane class, 14 exhibited inhibition of T. brucei without disrupting microfilament assembly, and 15 demonstrated modest microtubule-stabilizing effects. The use of removable well plate libraries to avoid false positives from extracts enriched with only one or two major metabolites is also discussed. Overall, these results highlight the advantages of applying modern methods in natural products-based research to accelerate the HT discovery of therapeutic leads and/or new molecular structures using LC-MS-UV-ELSD-based libraries.

AB - A high-throughput (HT) paradigm generating LC-MS-UV-ELSD-based natural product libraries to discover compounds with new bioactivities and or molecular structures is presented. To validate this methodology, an extract of the Indo-Pacific marine sponge Cacospongia mycofijiensis was evaluated using assays involving cytoskeletal profiling, tumor cell lines, and parasites. Twelve known compounds were identified including latrunculins (1–4, 10), fijianolides (5, 8, 9), mycothiazole (11), aignopsanes (6, 7), and sacrotride A (13). Compounds 1–5 and 8–11 exhibited bioactivity not previously reported against the parasite T. brucei, while 11 showed selectivity for lymphoma (U937) tumor cell lines. Four new compounds were also discovered including aignopsanoic acid B (13), apolatrunculin T (14), 20-methoxy-fijianolide A (15), and aignopsane ketal (16). Compounds 13 and 16 represent important derivatives of the aignopsane class, 14 exhibited inhibition of T. brucei without disrupting microfilament assembly, and 15 demonstrated modest microtubule-stabilizing effects. The use of removable well plate libraries to avoid false positives from extracts enriched with only one or two major metabolites is also discussed. Overall, these results highlight the advantages of applying modern methods in natural products-based research to accelerate the HT discovery of therapeutic leads and/or new molecular structures using LC-MS-UV-ELSD-based libraries.

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KW - Drug Discovery

KW - Ions

KW - Pharmaceuticals

KW - Screening Assays

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DO - 10.1021/np200673b

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