Hepatic targeting and biodistribution of human fetal liver stem/progenitor cells and adult hepatocytes in mice.

Daniel Benten; Kang Cheng; Kuldeep Bhargava; Mari Inada; Brigid Joseph; Christopher Palestro; Sanjeev Gupta

Hepatic targeting and biodistribution of human fetal liver stem/progenitor cells and adult hepatocytes in mice.

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Hepatic targeting and biodistribution of human fetal liver stem/progenitor cells and adult hepatocytes in mice. / Benten, Daniel; Cheng, Kang; Bhargava, Kuldeep; Inada, Mari; Joseph, Brigid; Palestro, Christopher; Gupta, Sanjeev.

in: HEPATOLOGY, Jahrgang 50, Nr. 4, 4, 2009, S. 1194-1203.

Publikationen: SCORING: Beitrag in Fachzeitschrift/Zeitung › SCORING: Zeitschriftenaufsatz › Forschung › Begutachtung

Harvard

Benten, D, Cheng, K, Bhargava, K, Inada, M, Joseph, B, Palestro, C & Gupta, S 2009, 'Hepatic targeting and biodistribution of human fetal liver stem/progenitor cells and adult hepatocytes in mice.', HEPATOLOGY, Jg. 50, Nr. 4, 4, S. 1194-1203. <http://www.ncbi.nlm.nih.gov/pubmed/19637284?dopt=Citation>

APA

Benten, D., Cheng, K., Bhargava, K., Inada, M., Joseph, B., Palestro, C., & Gupta, S. (2009). Hepatic targeting and biodistribution of human fetal liver stem/progenitor cells and adult hepatocytes in mice. HEPATOLOGY, 50(4), 1194-1203. [4]. http://www.ncbi.nlm.nih.gov/pubmed/19637284?dopt=Citation

Vancouver

Benten D, Cheng K, Bhargava K, Inada M, Joseph B, Palestro C et al. Hepatic targeting and biodistribution of human fetal liver stem/progenitor cells and adult hepatocytes in mice. HEPATOLOGY. 2009;50(4):1194-1203. 4.

Bibtex

@article{058191fbc07540f29505add99e60ebcf,

title = "Hepatic targeting and biodistribution of human fetal liver stem/progenitor cells and adult hepatocytes in mice.",

abstract = "Tracking stem/progenitor cells through noninvasive imaging is a helpful means of assessing the targeting of transplanted cells to specific organs. We performed in vitro and in vivo studies wherein adult human hepatocytes and human fetal liver stem/progenitor cells were labeled with indium-111 ((111)In)-oxine and technetium-99m ((99m)Tc)-Ultratag or (99m)Tc-Ceretec. The labeling efficiency and viability of cells was analyzed in vitro, and organ biodistribution of cells was analyzed in vivo after transplantation in xenotolerant nonobese diabetic/severe combined immunodeficiency mice through intrasplenic or intraportal routes. We found that adult hepatocytes and fetal liver stem/progenitor cells incorporated (111)In but not (99m)Tc labels. After radiolabeling, cell viability was unchanged. Transplanted adult hepatocytes or fetal liver stem/progenitor cells were targeted to the liver more effectively by the intraportal rather than the intrasplenic route. Transplanted cells were retained in the liver after intraportal injection and in the liver and spleen after intrasplenic injection, without translocations into pulmonary or systemic circulations. Compared with fetal liver stem/progenitor cells, fewer adult hepatocytes were retained in the spleen after intrasplenic transplantation. The distribution of transplanted cells in organs was substantiated by genetic assays, including polymerase chain reaction amplification of DNA sequences from a primate-specific Charcot-Marie-Tooth element, and in situ hybridization for primate alphoid satellite sequences ubiquitous in all centromeres. CONCLUSION: (111)In labeling of human fetal liver stem/progenitor cells and adult hepatocytes was effective for noninvasive localization of transplanted cells. This should facilitate continued development of cell therapies through further animal and clinical studies.",

author = "Daniel Benten and Kang Cheng and Kuldeep Bhargava and Mari Inada and Brigid Joseph and Christopher Palestro and Sanjeev Gupta",

year = "2009",

language = "Deutsch",

volume = "50",

pages = "1194--1203",

journal = "HEPATOLOGY",

issn = "0270-9139",

publisher = "John Wiley and Sons Ltd",

number = "4",

}

RIS

TY - JOUR

T1 - Hepatic targeting and biodistribution of human fetal liver stem/progenitor cells and adult hepatocytes in mice.

AU - Benten, Daniel

AU - Cheng, Kang

AU - Bhargava, Kuldeep

AU - Inada, Mari

AU - Joseph, Brigid

AU - Palestro, Christopher

AU - Gupta, Sanjeev

PY - 2009

Y1 - 2009

N2 - Tracking stem/progenitor cells through noninvasive imaging is a helpful means of assessing the targeting of transplanted cells to specific organs. We performed in vitro and in vivo studies wherein adult human hepatocytes and human fetal liver stem/progenitor cells were labeled with indium-111 ((111)In)-oxine and technetium-99m ((99m)Tc)-Ultratag or (99m)Tc-Ceretec. The labeling efficiency and viability of cells was analyzed in vitro, and organ biodistribution of cells was analyzed in vivo after transplantation in xenotolerant nonobese diabetic/severe combined immunodeficiency mice through intrasplenic or intraportal routes. We found that adult hepatocytes and fetal liver stem/progenitor cells incorporated (111)In but not (99m)Tc labels. After radiolabeling, cell viability was unchanged. Transplanted adult hepatocytes or fetal liver stem/progenitor cells were targeted to the liver more effectively by the intraportal rather than the intrasplenic route. Transplanted cells were retained in the liver after intraportal injection and in the liver and spleen after intrasplenic injection, without translocations into pulmonary or systemic circulations. Compared with fetal liver stem/progenitor cells, fewer adult hepatocytes were retained in the spleen after intrasplenic transplantation. The distribution of transplanted cells in organs was substantiated by genetic assays, including polymerase chain reaction amplification of DNA sequences from a primate-specific Charcot-Marie-Tooth element, and in situ hybridization for primate alphoid satellite sequences ubiquitous in all centromeres. CONCLUSION: (111)In labeling of human fetal liver stem/progenitor cells and adult hepatocytes was effective for noninvasive localization of transplanted cells. This should facilitate continued development of cell therapies through further animal and clinical studies.

AB - Tracking stem/progenitor cells through noninvasive imaging is a helpful means of assessing the targeting of transplanted cells to specific organs. We performed in vitro and in vivo studies wherein adult human hepatocytes and human fetal liver stem/progenitor cells were labeled with indium-111 ((111)In)-oxine and technetium-99m ((99m)Tc)-Ultratag or (99m)Tc-Ceretec. The labeling efficiency and viability of cells was analyzed in vitro, and organ biodistribution of cells was analyzed in vivo after transplantation in xenotolerant nonobese diabetic/severe combined immunodeficiency mice through intrasplenic or intraportal routes. We found that adult hepatocytes and fetal liver stem/progenitor cells incorporated (111)In but not (99m)Tc labels. After radiolabeling, cell viability was unchanged. Transplanted adult hepatocytes or fetal liver stem/progenitor cells were targeted to the liver more effectively by the intraportal rather than the intrasplenic route. Transplanted cells were retained in the liver after intraportal injection and in the liver and spleen after intrasplenic injection, without translocations into pulmonary or systemic circulations. Compared with fetal liver stem/progenitor cells, fewer adult hepatocytes were retained in the spleen after intrasplenic transplantation. The distribution of transplanted cells in organs was substantiated by genetic assays, including polymerase chain reaction amplification of DNA sequences from a primate-specific Charcot-Marie-Tooth element, and in situ hybridization for primate alphoid satellite sequences ubiquitous in all centromeres. CONCLUSION: (111)In labeling of human fetal liver stem/progenitor cells and adult hepatocytes was effective for noninvasive localization of transplanted cells. This should facilitate continued development of cell therapies through further animal and clinical studies.

M3 - SCORING: Zeitschriftenaufsatz

VL - 50

SP - 1194

EP - 1203

JO - HEPATOLOGY

JF - HEPATOLOGY

SN - 0270-9139

IS - 4

M1 - 4

ER -