Systemic ASBT inactivation protects against liver damage in obstructive cholestasis in mice

Roni F. Kunst; Dirk R. de Waart; Frank Wolters; Suzanne Duijst; Esther W. Vogels; Isabelle Bolt; Joanne Verheij; Ulrich Beuers; Ronald P. J. Oude Elferink; Stan F. J. van de Graaf

doi:10.1016/j.jhepr.2022.100573

Systemic ASBT inactivation protects against liver damage in obstructive cholestasis in mice

Roni F. Kunst, Dirk R. de Waart, Frank Wolters, Suzanne Duijst, Esther W. Vogels, Isabelle Bolt, Joanne Verheij, Ulrich Beuers, Ronald P. J. Oude Elferink, Stan F. J. van de Graaf

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

16 Citations (Scopus)

Abstract

BACKGROUND & AIMS: Non-absorbable inhibitors of the apical sodium-dependent bile acid transporter (ASBT; also called ileal bile acid transporter [IBAT]) are recently approved or in clinical development for multiple cholestatic liver disorders and lead to a reduction in pruritus and (markers for) liver injury. Unfortunately, non-absorbable ASBT inhibitors (ASBTi) can induce diarrhoea or may be ineffective if cholestasis is extensive and largely precludes intestinal excretion of bile acids. Systemically acting ASBTi that divert bile salts towards renal excretion may alleviate these issues.

METHODS: Bile duct ligation (BDL) was performed in ASBT-deficient (ASBT knockout [KO]) mice as a model for chronic systemic ASBT inhibition in obstructive cholestasis. Co-infusion of radiolabelled taurocholate and inulin was used to quantify renal bile salt excretion after BDL. In a second (wild-type) mouse model, a combination of obeticholic acid (OCA) and intestine-restricted ASBT inhibition was used to lower the bile salt pool size before BDL.

RESULTS: After BDL, ASBT KO mice had reduced plasma bilirubin and alkaline phosphatase compared with wild-type mice with BDL and showed a marked reduction in liver necrotic areas at histopathological analysis, suggesting decreased BDL-induced liver damage. Furthermore, ASBT KO mice had reduced bile salt pool size, lower plasma taurine-conjugated polyhydroxylated bile salt, and increased urinary bile salt excretion. Pretreatment with OCA + ASBTi in wild-type mice reduced the pool size and greatly improved liver injury markers and liver histology.

CONCLUSIONS: A reduced bile salt pool at the onset of cholestasis effectively lowers cholestatic liver injury in mice. Systemic ASBT inhibition may be valuable as treatment for cholestatic liver disease by lowering the pool size and increasing renal bile salt output even under conditions of minimal faecal bile salt secretion.

LAY SUMMARY: Novel treatment approaches against cholestatic liver disease (resulting in reduced or blocked flow of bile) involve non-absorbable inhibitors of the bile acid transport protein ASBT, but these are not always effective and/or can cause unwanted side effects. In this study, we demonstrate that systemic inhibition/inactivation of ASBT protects mice against developing severe cholestatic liver injury after bile duct ligation, by reducing bile salt pool size and increasing renal bile salt excretion.

Original language	English
Article number	100573
Pages (from-to)	100573
Journal	JHEP Reports
Volume	4
Issue number	11
DOIs	https://doi.org/10.1016/j.jhepr.2022.100573 https://doi.org/10.1016/j.jhepr.2022.100573
Publication status	Published - 1 Nov 2022

Keywords

Alagille
Apical sodium-dependent bile acid transporter (ASBT)
BSEP
Bile salt pool size
Cholestasis
IBAT
NTCP
PFIC
Renal excretion

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Kunst, R. F., de Waart, D. R., Wolters, F., Duijst, S., Vogels, E. W., Bolt, I., Verheij, J., Beuers, U., Oude Elferink, R. P. J., & van de Graaf, S. F. J. (2022). Systemic ASBT inactivation protects against liver damage in obstructive cholestasis in mice. JHEP Reports, 4(11), 100573. Article 100573. https://doi.org/10.1016/j.jhepr.2022.100573, https://doi.org/10.1016/j.jhepr.2022.100573

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title = "Systemic ASBT inactivation protects against liver damage in obstructive cholestasis in mice",

abstract = "BACKGROUND & AIMS: Non-absorbable inhibitors of the apical sodium-dependent bile acid transporter (ASBT; also called ileal bile acid transporter [IBAT]) are recently approved or in clinical development for multiple cholestatic liver disorders and lead to a reduction in pruritus and (markers for) liver injury. Unfortunately, non-absorbable ASBT inhibitors (ASBTi) can induce diarrhoea or may be ineffective if cholestasis is extensive and largely precludes intestinal excretion of bile acids. Systemically acting ASBTi that divert bile salts towards renal excretion may alleviate these issues.METHODS: Bile duct ligation (BDL) was performed in ASBT-deficient (ASBT knockout [KO]) mice as a model for chronic systemic ASBT inhibition in obstructive cholestasis. Co-infusion of radiolabelled taurocholate and inulin was used to quantify renal bile salt excretion after BDL. In a second (wild-type) mouse model, a combination of obeticholic acid (OCA) and intestine-restricted ASBT inhibition was used to lower the bile salt pool size before BDL.RESULTS: After BDL, ASBT KO mice had reduced plasma bilirubin and alkaline phosphatase compared with wild-type mice with BDL and showed a marked reduction in liver necrotic areas at histopathological analysis, suggesting decreased BDL-induced liver damage. Furthermore, ASBT KO mice had reduced bile salt pool size, lower plasma taurine-conjugated polyhydroxylated bile salt, and increased urinary bile salt excretion. Pretreatment with OCA + ASBTi in wild-type mice reduced the pool size and greatly improved liver injury markers and liver histology.CONCLUSIONS: A reduced bile salt pool at the onset of cholestasis effectively lowers cholestatic liver injury in mice. Systemic ASBT inhibition may be valuable as treatment for cholestatic liver disease by lowering the pool size and increasing renal bile salt output even under conditions of minimal faecal bile salt secretion.LAY SUMMARY: Novel treatment approaches against cholestatic liver disease (resulting in reduced or blocked flow of bile) involve non-absorbable inhibitors of the bile acid transport protein ASBT, but these are not always effective and/or can cause unwanted side effects. In this study, we demonstrate that systemic inhibition/inactivation of ASBT protects mice against developing severe cholestatic liver injury after bile duct ligation, by reducing bile salt pool size and increasing renal bile salt excretion.",

keywords = "Alagille, Apical sodium-dependent bile acid transporter (ASBT), BSEP, Bile salt pool size, Cholestasis, IBAT, NTCP, PFIC, Renal excretion",

author = "Kunst, {Roni F.} and {de Waart}, {Dirk R.} and Frank Wolters and Suzanne Duijst and Vogels, {Esther W.} and Isabelle Bolt and Joanne Verheij and Ulrich Beuers and {Oude Elferink}, {Ronald P. J.} and {van de Graaf}, {Stan F. J.}",

note = "Funding Information: This work was supported by grants from The Netherlands Organization for Scientific Research ( Vidi 91713319 and Vici 09150182010007 to SFJVDG) and the European Research Council (Starting grant 337479 to SFJVDG). Publisher Copyright: {\textcopyright} 2022 The Author(s)",

year = "2022",

month = nov,

day = "1",

doi = "10.1016/j.jhepr.2022.100573",

language = "English",

volume = "4",

pages = "100573",

journal = "JHEP Reports",

issn = "2589-5559",

publisher = "Elsevier",

number = "11",

}

Kunst, RF , de Waart, DR , Wolters, F , Duijst, S , Vogels, EW , Bolt, I , Verheij, J , Beuers, U , Oude Elferink, RPJ & van de Graaf, SFJ 2022, 'Systemic ASBT inactivation protects against liver damage in obstructive cholestasis in mice', JHEP Reports, vol. 4, no. 11, 100573, pp. 100573. https://doi.org/10.1016/j.jhepr.2022.100573, https://doi.org/10.1016/j.jhepr.2022.100573

TY - JOUR

T1 - Systemic ASBT inactivation protects against liver damage in obstructive cholestasis in mice

AU - Kunst, Roni F.

AU - de Waart, Dirk R.

AU - Wolters, Frank

AU - Duijst, Suzanne

AU - Vogels, Esther W.

AU - Bolt, Isabelle

AU - Verheij, Joanne

AU - Beuers, Ulrich

AU - Oude Elferink, Ronald P. J.

AU - van de Graaf, Stan F. J.

N1 - Funding Information: This work was supported by grants from The Netherlands Organization for Scientific Research ( Vidi 91713319 and Vici 09150182010007 to SFJVDG) and the European Research Council (Starting grant 337479 to SFJVDG). Publisher Copyright: © 2022 The Author(s)

PY - 2022/11/1

Y1 - 2022/11/1

N2 - BACKGROUND & AIMS: Non-absorbable inhibitors of the apical sodium-dependent bile acid transporter (ASBT; also called ileal bile acid transporter [IBAT]) are recently approved or in clinical development for multiple cholestatic liver disorders and lead to a reduction in pruritus and (markers for) liver injury. Unfortunately, non-absorbable ASBT inhibitors (ASBTi) can induce diarrhoea or may be ineffective if cholestasis is extensive and largely precludes intestinal excretion of bile acids. Systemically acting ASBTi that divert bile salts towards renal excretion may alleviate these issues.METHODS: Bile duct ligation (BDL) was performed in ASBT-deficient (ASBT knockout [KO]) mice as a model for chronic systemic ASBT inhibition in obstructive cholestasis. Co-infusion of radiolabelled taurocholate and inulin was used to quantify renal bile salt excretion after BDL. In a second (wild-type) mouse model, a combination of obeticholic acid (OCA) and intestine-restricted ASBT inhibition was used to lower the bile salt pool size before BDL.RESULTS: After BDL, ASBT KO mice had reduced plasma bilirubin and alkaline phosphatase compared with wild-type mice with BDL and showed a marked reduction in liver necrotic areas at histopathological analysis, suggesting decreased BDL-induced liver damage. Furthermore, ASBT KO mice had reduced bile salt pool size, lower plasma taurine-conjugated polyhydroxylated bile salt, and increased urinary bile salt excretion. Pretreatment with OCA + ASBTi in wild-type mice reduced the pool size and greatly improved liver injury markers and liver histology.CONCLUSIONS: A reduced bile salt pool at the onset of cholestasis effectively lowers cholestatic liver injury in mice. Systemic ASBT inhibition may be valuable as treatment for cholestatic liver disease by lowering the pool size and increasing renal bile salt output even under conditions of minimal faecal bile salt secretion.LAY SUMMARY: Novel treatment approaches against cholestatic liver disease (resulting in reduced or blocked flow of bile) involve non-absorbable inhibitors of the bile acid transport protein ASBT, but these are not always effective and/or can cause unwanted side effects. In this study, we demonstrate that systemic inhibition/inactivation of ASBT protects mice against developing severe cholestatic liver injury after bile duct ligation, by reducing bile salt pool size and increasing renal bile salt excretion.

AB - BACKGROUND & AIMS: Non-absorbable inhibitors of the apical sodium-dependent bile acid transporter (ASBT; also called ileal bile acid transporter [IBAT]) are recently approved or in clinical development for multiple cholestatic liver disorders and lead to a reduction in pruritus and (markers for) liver injury. Unfortunately, non-absorbable ASBT inhibitors (ASBTi) can induce diarrhoea or may be ineffective if cholestasis is extensive and largely precludes intestinal excretion of bile acids. Systemically acting ASBTi that divert bile salts towards renal excretion may alleviate these issues.METHODS: Bile duct ligation (BDL) was performed in ASBT-deficient (ASBT knockout [KO]) mice as a model for chronic systemic ASBT inhibition in obstructive cholestasis. Co-infusion of radiolabelled taurocholate and inulin was used to quantify renal bile salt excretion after BDL. In a second (wild-type) mouse model, a combination of obeticholic acid (OCA) and intestine-restricted ASBT inhibition was used to lower the bile salt pool size before BDL.RESULTS: After BDL, ASBT KO mice had reduced plasma bilirubin and alkaline phosphatase compared with wild-type mice with BDL and showed a marked reduction in liver necrotic areas at histopathological analysis, suggesting decreased BDL-induced liver damage. Furthermore, ASBT KO mice had reduced bile salt pool size, lower plasma taurine-conjugated polyhydroxylated bile salt, and increased urinary bile salt excretion. Pretreatment with OCA + ASBTi in wild-type mice reduced the pool size and greatly improved liver injury markers and liver histology.CONCLUSIONS: A reduced bile salt pool at the onset of cholestasis effectively lowers cholestatic liver injury in mice. Systemic ASBT inhibition may be valuable as treatment for cholestatic liver disease by lowering the pool size and increasing renal bile salt output even under conditions of minimal faecal bile salt secretion.LAY SUMMARY: Novel treatment approaches against cholestatic liver disease (resulting in reduced or blocked flow of bile) involve non-absorbable inhibitors of the bile acid transport protein ASBT, but these are not always effective and/or can cause unwanted side effects. In this study, we demonstrate that systemic inhibition/inactivation of ASBT protects mice against developing severe cholestatic liver injury after bile duct ligation, by reducing bile salt pool size and increasing renal bile salt excretion.

KW - Alagille

KW - Apical sodium-dependent bile acid transporter (ASBT)

KW - BSEP

KW - Bile salt pool size

KW - Cholestasis

KW - IBAT

KW - NTCP

KW - PFIC

KW - Renal excretion

UR - http://www.scopus.com/inward/record.url?scp=85138583747&partnerID=8YFLogxK

U2 - 10.1016/j.jhepr.2022.100573

DO - 10.1016/j.jhepr.2022.100573

M3 - Article

C2 - 36160754

SN - 2589-5559

VL - 4

SP - 100573

JO - JHEP Reports

JF - JHEP Reports

IS - 11

M1 - 100573

ER -

Systemic ASBT inactivation protects against liver damage in obstructive cholestasis in mice

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