Directed Differentiation of Bone Marrow Derived Mesenchymal Stem Cells Into Bladder Urothelium

Govindaraj Anumanthan; John H. Makari; Lindsey Honea; John C. Thomas; Marcia L. Wills; Neil A. Bhowmick; Mark C. Adams; Simon W. Hayward; Robert J. Matusik; John W. Brock; John C. Pope IV

doi:10.1016/j.juro.2008.04.076

Directed Differentiation of Bone Marrow Derived Mesenchymal Stem Cells Into Bladder Urothelium

Govindaraj Anumanthan, John H. Makari, Lindsey Honea, John C. Thomas, Marcia L. Wills, Neil A. Bhowmick, Mark C. Adams, Simon W. Hayward, Robert J. Matusik, John W. Brock, John C. Pope IV

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

69 Scopus citations

Abstract

Purpose: We have previously reported that embryonic rat bladder mesenchyma has the appropriate inductive signals to direct pluripotent mouse embryonic stem cells toward endodermal derived urothelium and develop mature bladder tissue. We determined whether nonembryonic stem cells, specifically bone marrow derived mesenchymal stem cells, could serve as a source of pluripotent or multipotent progenitor cells. Materials and Methods: Epithelium was separated from the mesenchymal shells of embryonic day 14 rat bladders. Mesenchymal stem cells were isolated from mouse femoral and tibial bone marrow. Heterospecific recombinant xenografts were created by combining the embryonic rat bladder mesenchyma shells with mesenchymal stem cells and grafting them into the renal subcapsular space of athymic nude mice. Grafts were harvested at time points of up to 42 days and stained for urothelial and stromal differentiation. Results: Histological examination of xenografts comprising mouse mesenchymal stem cells and rat embryonic rat bladder mesenchyma yielded mature bladder structures showing normal microscopic architecture as well as proteins confirming functional characteristics. Specifically the induced urothelium expressed uroplakin, a highly selective marker of urothelial differentiation. These differentiated bladder structures demonstrated appropriate α-smooth muscle actin staining. Finally, Hoechst staining of the xenografts revealed nuclear architecture consistent with a mouse mesenchymal stem cell origin of the urothelium, supporting differentiated development of these cells. Conclusions: In the appropriate signaling environment bone marrow derived mesenchymal stem cells can undergo directed differentiation toward endodermal derived urothelium and develop into mature bladder tissue in a tissue recombination model. This model serves as an important tool for the study of bladder development with long-term application toward cell replacement therapies in the future.

Original language	English (US)
Pages (from-to)	1778-1783
Number of pages	6
Journal	Journal of Urology
Volume	180
Issue number	4 SUPPL.
DOIs	https://doi.org/10.1016/j.juro.2008.04.076
State	Published - Oct 2008
Externally published	Yes

Keywords

bone marrow
mesoderm
stem cells
urinary bladder
urothelium

ASJC Scopus subject areas

Urology

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10.1016/j.juro.2008.04.076

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@article{42b5c473cd724c5c91ef85adbadc6ed6,

title = "Directed Differentiation of Bone Marrow Derived Mesenchymal Stem Cells Into Bladder Urothelium",

abstract = "Purpose: We have previously reported that embryonic rat bladder mesenchyma has the appropriate inductive signals to direct pluripotent mouse embryonic stem cells toward endodermal derived urothelium and develop mature bladder tissue. We determined whether nonembryonic stem cells, specifically bone marrow derived mesenchymal stem cells, could serve as a source of pluripotent or multipotent progenitor cells. Materials and Methods: Epithelium was separated from the mesenchymal shells of embryonic day 14 rat bladders. Mesenchymal stem cells were isolated from mouse femoral and tibial bone marrow. Heterospecific recombinant xenografts were created by combining the embryonic rat bladder mesenchyma shells with mesenchymal stem cells and grafting them into the renal subcapsular space of athymic nude mice. Grafts were harvested at time points of up to 42 days and stained for urothelial and stromal differentiation. Results: Histological examination of xenografts comprising mouse mesenchymal stem cells and rat embryonic rat bladder mesenchyma yielded mature bladder structures showing normal microscopic architecture as well as proteins confirming functional characteristics. Specifically the induced urothelium expressed uroplakin, a highly selective marker of urothelial differentiation. These differentiated bladder structures demonstrated appropriate α-smooth muscle actin staining. Finally, Hoechst staining of the xenografts revealed nuclear architecture consistent with a mouse mesenchymal stem cell origin of the urothelium, supporting differentiated development of these cells. Conclusions: In the appropriate signaling environment bone marrow derived mesenchymal stem cells can undergo directed differentiation toward endodermal derived urothelium and develop into mature bladder tissue in a tissue recombination model. This model serves as an important tool for the study of bladder development with long-term application toward cell replacement therapies in the future.",

keywords = "bone marrow, mesoderm, stem cells, urinary bladder, urothelium",

author = "Govindaraj Anumanthan and Makari, {John H.} and Lindsey Honea and Thomas, {John C.} and Wills, {Marcia L.} and Bhowmick, {Neil A.} and Adams, {Mark C.} and Hayward, {Simon W.} and Matusik, {Robert J.} and Brock, {John W.} and {Pope IV}, {John C.}",

note = "Funding Information: Supported by National Institutes of Health Grant R01-DK057483 (JCP) and a Society of Pediatric Urology grant (JHM). ",

year = "2008",

month = oct,

doi = "10.1016/j.juro.2008.04.076",

language = "English (US)",

volume = "180",

pages = "1778--1783",

journal = "Journal of Urology",

issn = "0022-5347",

publisher = "Wolters Kluwer Health",

number = "4 SUPPL.",

}

TY - JOUR

T1 - Directed Differentiation of Bone Marrow Derived Mesenchymal Stem Cells Into Bladder Urothelium

AU - Anumanthan, Govindaraj

AU - Makari, John H.

AU - Honea, Lindsey

AU - Thomas, John C.

AU - Wills, Marcia L.

AU - Bhowmick, Neil A.

AU - Adams, Mark C.

AU - Hayward, Simon W.

AU - Matusik, Robert J.

AU - Brock, John W.

AU - Pope IV, John C.

N1 - Funding Information: Supported by National Institutes of Health Grant R01-DK057483 (JCP) and a Society of Pediatric Urology grant (JHM).

PY - 2008/10

Y1 - 2008/10

N2 - Purpose: We have previously reported that embryonic rat bladder mesenchyma has the appropriate inductive signals to direct pluripotent mouse embryonic stem cells toward endodermal derived urothelium and develop mature bladder tissue. We determined whether nonembryonic stem cells, specifically bone marrow derived mesenchymal stem cells, could serve as a source of pluripotent or multipotent progenitor cells. Materials and Methods: Epithelium was separated from the mesenchymal shells of embryonic day 14 rat bladders. Mesenchymal stem cells were isolated from mouse femoral and tibial bone marrow. Heterospecific recombinant xenografts were created by combining the embryonic rat bladder mesenchyma shells with mesenchymal stem cells and grafting them into the renal subcapsular space of athymic nude mice. Grafts were harvested at time points of up to 42 days and stained for urothelial and stromal differentiation. Results: Histological examination of xenografts comprising mouse mesenchymal stem cells and rat embryonic rat bladder mesenchyma yielded mature bladder structures showing normal microscopic architecture as well as proteins confirming functional characteristics. Specifically the induced urothelium expressed uroplakin, a highly selective marker of urothelial differentiation. These differentiated bladder structures demonstrated appropriate α-smooth muscle actin staining. Finally, Hoechst staining of the xenografts revealed nuclear architecture consistent with a mouse mesenchymal stem cell origin of the urothelium, supporting differentiated development of these cells. Conclusions: In the appropriate signaling environment bone marrow derived mesenchymal stem cells can undergo directed differentiation toward endodermal derived urothelium and develop into mature bladder tissue in a tissue recombination model. This model serves as an important tool for the study of bladder development with long-term application toward cell replacement therapies in the future.

AB - Purpose: We have previously reported that embryonic rat bladder mesenchyma has the appropriate inductive signals to direct pluripotent mouse embryonic stem cells toward endodermal derived urothelium and develop mature bladder tissue. We determined whether nonembryonic stem cells, specifically bone marrow derived mesenchymal stem cells, could serve as a source of pluripotent or multipotent progenitor cells. Materials and Methods: Epithelium was separated from the mesenchymal shells of embryonic day 14 rat bladders. Mesenchymal stem cells were isolated from mouse femoral and tibial bone marrow. Heterospecific recombinant xenografts were created by combining the embryonic rat bladder mesenchyma shells with mesenchymal stem cells and grafting them into the renal subcapsular space of athymic nude mice. Grafts were harvested at time points of up to 42 days and stained for urothelial and stromal differentiation. Results: Histological examination of xenografts comprising mouse mesenchymal stem cells and rat embryonic rat bladder mesenchyma yielded mature bladder structures showing normal microscopic architecture as well as proteins confirming functional characteristics. Specifically the induced urothelium expressed uroplakin, a highly selective marker of urothelial differentiation. These differentiated bladder structures demonstrated appropriate α-smooth muscle actin staining. Finally, Hoechst staining of the xenografts revealed nuclear architecture consistent with a mouse mesenchymal stem cell origin of the urothelium, supporting differentiated development of these cells. Conclusions: In the appropriate signaling environment bone marrow derived mesenchymal stem cells can undergo directed differentiation toward endodermal derived urothelium and develop into mature bladder tissue in a tissue recombination model. This model serves as an important tool for the study of bladder development with long-term application toward cell replacement therapies in the future.

KW - bone marrow

KW - mesoderm

KW - stem cells

KW - urinary bladder

KW - urothelium

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DO - 10.1016/j.juro.2008.04.076

M3 - Article

C2 - 18721942

AN - SCOPUS:51049090361

SN - 0022-5347

VL - 180

SP - 1778

EP - 1783

JO - Journal of Urology

JF - Journal of Urology

IS - 4 SUPPL.

ER -

Directed Differentiation of Bone Marrow Derived Mesenchymal Stem Cells Into Bladder Urothelium

Abstract

Keywords

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