Identification of sennoside A as a novel inhibitor of the slingshot (SSH) family proteins related to cancer metastasis

Seon Young Lee; Wooil Kim; Young Geun Lee; Hyo Jin Kang; Sang Hyun Lee; Sun Young Park; Jeong Ki Min; Sang Rae Lee; Sang J. Chung

doi:10.1016/j.phrs.2017.03.003

Identification of sennoside A as a novel inhibitor of the slingshot (SSH) family proteins related to cancer metastasis

Seon Young Lee, Wooil Kim, Young Geun Lee, Hyo Jin Kang, Sang Hyun Lee, Sun Young Park, Jeong Ki Min, Sang Rae Lee, Sang J. Chung

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

48 Scopus citations

Abstract

Phospho-cofilin (p-cofilin), which has a phosphate group on Ser-3, is involved in actin polymerization. Its dephosphorylated form promotes filopodia formation and cell migration by enhancing actin depolymerization. Protein phosphatase slingshot homologs (SSHs), known as dual-specificity phosphatases, catalyze hydrolytic removal of the Ser-3 phosphate group from phospho-cofilin. Aberrant SSH activity results in cancer metastasis, implicating SSHs as potential therapeutic targets for cancer metastasis. In this study, we screened 658 natural products purified from traditional oriental medicinal plants to identify three potent SSH inhibitors with submicromolar or single-digit micromolar K_i values: gossypol, hypericin, and sennoside A. The three compounds were purified from cottonseed, Saint John's wort, and rhubarb, respectively. Sennoside A markedly increased cofilin phosphorylation in pancreatic cancer cells, leading to impaired actin dynamics in pancreatic cancer cells with or without EGF stimulation and reduced motility and invasiveness in vitro and in vivo. Collaboratively, these results demonstrate that sennoside A is a novel inhibitor of SSHs and suggest that it may be valuable in the development of pharmaceutical drugs for treating cancer metastasis.

Original language	English
Pages (from-to)	422-430
Number of pages	9
Journal	Pharmacological Research
Volume	119
DOIs	https://doi.org/10.1016/j.phrs.2017.03.003
State	Published - 1 May 2017
Externally published	Yes

Keywords

Cofilin
Dual-specificity phosphatase
Natural product
Pancreatic cancer metastasis
Slingshot homologs (SSHs)

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.phrs.2017.03.003

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@article{368ffba09d304d83b6bafc5fbdb6002c,

title = "Identification of sennoside A as a novel inhibitor of the slingshot (SSH) family proteins related to cancer metastasis",

abstract = "Phospho-cofilin (p-cofilin), which has a phosphate group on Ser-3, is involved in actin polymerization. Its dephosphorylated form promotes filopodia formation and cell migration by enhancing actin depolymerization. Protein phosphatase slingshot homologs (SSHs), known as dual-specificity phosphatases, catalyze hydrolytic removal of the Ser-3 phosphate group from phospho-cofilin. Aberrant SSH activity results in cancer metastasis, implicating SSHs as potential therapeutic targets for cancer metastasis. In this study, we screened 658 natural products purified from traditional oriental medicinal plants to identify three potent SSH inhibitors with submicromolar or single-digit micromolar Ki values: gossypol, hypericin, and sennoside A. The three compounds were purified from cottonseed, Saint John's wort, and rhubarb, respectively. Sennoside A markedly increased cofilin phosphorylation in pancreatic cancer cells, leading to impaired actin dynamics in pancreatic cancer cells with or without EGF stimulation and reduced motility and invasiveness in vitro and in vivo. Collaboratively, these results demonstrate that sennoside A is a novel inhibitor of SSHs and suggest that it may be valuable in the development of pharmaceutical drugs for treating cancer metastasis.",

keywords = "Cofilin, Dual-specificity phosphatase, Natural product, Pancreatic cancer metastasis, Slingshot homologs (SSHs)",

author = "Lee, \{Seon Young\} and Wooil Kim and Lee, \{Young Geun\} and Kang, \{Hyo Jin\} and Lee, \{Sang Hyun\} and Park, \{Sun Young\} and Min, \{Jeong Ki\} and Lee, \{Sang Rae\} and Chung, \{Sang J.\}",

note = "Publisher Copyright: {\textcopyright} 2017 Elsevier Ltd",

year = "2017",

month = may,

day = "1",

doi = "10.1016/j.phrs.2017.03.003",

language = "English",

volume = "119",

pages = "422--430",

journal = "Pharmacological Research",

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publisher = "Academic Press",

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TY - JOUR

T1 - Identification of sennoside A as a novel inhibitor of the slingshot (SSH) family proteins related to cancer metastasis

AU - Lee, Seon Young

AU - Kim, Wooil

AU - Lee, Young Geun

AU - Kang, Hyo Jin

AU - Lee, Sang Hyun

AU - Park, Sun Young

AU - Min, Jeong Ki

AU - Lee, Sang Rae

AU - Chung, Sang J.

PY - 2017/5/1

Y1 - 2017/5/1

N2 - Phospho-cofilin (p-cofilin), which has a phosphate group on Ser-3, is involved in actin polymerization. Its dephosphorylated form promotes filopodia formation and cell migration by enhancing actin depolymerization. Protein phosphatase slingshot homologs (SSHs), known as dual-specificity phosphatases, catalyze hydrolytic removal of the Ser-3 phosphate group from phospho-cofilin. Aberrant SSH activity results in cancer metastasis, implicating SSHs as potential therapeutic targets for cancer metastasis. In this study, we screened 658 natural products purified from traditional oriental medicinal plants to identify three potent SSH inhibitors with submicromolar or single-digit micromolar Ki values: gossypol, hypericin, and sennoside A. The three compounds were purified from cottonseed, Saint John's wort, and rhubarb, respectively. Sennoside A markedly increased cofilin phosphorylation in pancreatic cancer cells, leading to impaired actin dynamics in pancreatic cancer cells with or without EGF stimulation and reduced motility and invasiveness in vitro and in vivo. Collaboratively, these results demonstrate that sennoside A is a novel inhibitor of SSHs and suggest that it may be valuable in the development of pharmaceutical drugs for treating cancer metastasis.

AB - Phospho-cofilin (p-cofilin), which has a phosphate group on Ser-3, is involved in actin polymerization. Its dephosphorylated form promotes filopodia formation and cell migration by enhancing actin depolymerization. Protein phosphatase slingshot homologs (SSHs), known as dual-specificity phosphatases, catalyze hydrolytic removal of the Ser-3 phosphate group from phospho-cofilin. Aberrant SSH activity results in cancer metastasis, implicating SSHs as potential therapeutic targets for cancer metastasis. In this study, we screened 658 natural products purified from traditional oriental medicinal plants to identify three potent SSH inhibitors with submicromolar or single-digit micromolar Ki values: gossypol, hypericin, and sennoside A. The three compounds were purified from cottonseed, Saint John's wort, and rhubarb, respectively. Sennoside A markedly increased cofilin phosphorylation in pancreatic cancer cells, leading to impaired actin dynamics in pancreatic cancer cells with or without EGF stimulation and reduced motility and invasiveness in vitro and in vivo. Collaboratively, these results demonstrate that sennoside A is a novel inhibitor of SSHs and suggest that it may be valuable in the development of pharmaceutical drugs for treating cancer metastasis.

KW - Cofilin

KW - Dual-specificity phosphatase

KW - Natural product

KW - Pancreatic cancer metastasis

KW - Slingshot homologs (SSHs)

UR - https://www.scopus.com/pages/publications/85015396150

U2 - 10.1016/j.phrs.2017.03.003

DO - 10.1016/j.phrs.2017.03.003

M3 - Article

C2 - 28274853

AN - SCOPUS:85015396150

SN - 1043-6618

VL - 119

SP - 422

EP - 430

JO - Pharmacological Research

JF - Pharmacological Research

ER -

Identification of sennoside A as a novel inhibitor of the slingshot (SSH) family proteins related to cancer metastasis

Abstract

Keywords

UN SDGs

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