High ubiquitous hCD55 and hCD39 co-expression in live transgenic alpha1,3-Gal Knock-out piglet

Andrea Perota; Irina Lagutina; Silvia Colleoni; Roberto Duchi; Giovanna Lazzari; Emanuele Cozzi; Fiorella Calabrese; Mathias Chatelais; Beatrice Charreau; Franco Lucchini; Cesare Galli

doi:10.1111/j.1399-3089.2011.00661.x

High ubiquitous hCD55 and hCD39 co-expression in live transgenic alpha1,3-Gal Knock-out piglet

Andrea Perota, Irina Lagutina, Silvia Colleoni, Roberto Duchi, Giovanna Lazzari, Emanuele Cozzi, Fiorella Calabrese, Mathias Chatelais, Beatrice Charreau, Franco Lucchini, Cesare Galli

Risultato della ricerca: Contributo in rivista › Contributo a convegno › peer review

Abstract

in xenotransplantation studies (pig to non-human primates) it was demonstrated that alpha-1,3 galactosyltransferase gene deletion (gal-ko) protected transplanted organs from hyperacute rejection. However the vascular acute rejection (avr) has to be solved through genetic engineering of donors inserting different human transgenes involved into prevention of complement activation (hCd55), coagulation and inﬂammation (hCd39) pathways. we created two different ubiquitous expression vectors for hCd55 (53mdH) and hCd39 (2JC9) exploiting the pCaggs promoter. primary ﬁbroblasts (1x10 6 ) from gal-ko pig were co-transfected with 5 micrograms of 53mdH+2JC9 (1:3) using nucleofector technology. after 24 hours, selection medium (Hygromicine = 175 ug/ml) was added to transfected cells and maintained for 15 days. sixty well growing resistant clones were picked up and analyzed for transgenes expression using western blot (wb) and immunocytochemistry (iCC). about 28% of colonies (n=17) showed high and uniform expression of both transgenes. four colonies were used as cell donors for sCnt and 265 cloned compacted morula and blastocysts d6 were transferred into 3 synchronized recipient sows. all sows became pregnant, 2 aborted at 30 th day, but one went to term (33%) and delivered one alive piglet and mummiﬁed fetus. the piglet died for e.coli infection at the age of 1 month. expression hCd39 was detected in every tissue (kidney, pancreas, brain, muscle, heart, liver, spleen, lung, umbilical cord) and primary cells (ﬁbroblasts and porcine aortic endothelial cells) analyzed with wb and iCC whereas hCd55 was not detected only in brain sample. we obtained a gal-ko piglet with ubiquitous high hCd39+hCd55 expression using the pCaggs promoter and he survived for one month without any apparent disorder. more pregnancies are ongoing with the same cell clones. the function of these two transgenes combination will be tested by xenotransplantation to primates as soon as more animals will be available

Lingua originale	English
pagine (da-a)	297-297
Numero di pagine	1
Rivista	Xenotransplantation
Volume	18
DOI	https://doi.org/10.1111/j.1399-3089.2011.00661.x
Stato di pubblicazione	Pubblicato - 2011
Evento	Joint Congress of the Cell Transplant Society (CTS) and the International Xenotranplantation Association (IXA - Miami Durata: 23 ott 2011 → 26 ott 2011

Keywords

CD39
CD55
transgenic pig
xenotransplantation

Accesso al documento

10.1111/j.1399-3089.2011.00661.x

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title = "High ubiquitous hCD55 and hCD39 co-expression in live transgenic alpha1,3-Gal Knock-out piglet",

abstract = "in xenotransplantation studies (pig to non-human primates) it was demonstrated that alpha-1,3 galactosyltransferase gene deletion (gal-ko) protected transplanted organs from hyperacute rejection. However the vascular acute rejection (avr) has to be solved through genetic engineering of donors inserting different human transgenes involved into prevention of complement activation (hCd55), coagulation and inﬂammation (hCd39) pathways. we created two different ubiquitous expression vectors for hCd55 (53mdH) and hCd39 (2JC9) exploiting the pCaggs promoter. primary ﬁbroblasts (1x10 6 ) from gal-ko pig were co-transfected with 5 micrograms of 53mdH+2JC9 (1:3) using nucleofector technology. after 24 hours, selection medium (Hygromicine = 175 ug/ml) was added to transfected cells and maintained for 15 days. sixty well growing resistant clones were picked up and analyzed for transgenes expression using western blot (wb) and immunocytochemistry (iCC). about 28% of colonies (n=17) showed high and uniform expression of both transgenes. four colonies were used as cell donors for sCnt and 265 cloned compacted morula and blastocysts d6 were transferred into 3 synchronized recipient sows. all sows became pregnant, 2 aborted at 30 th day, but one went to term (33%) and delivered one alive piglet and mummiﬁed fetus. the piglet died for e.coli infection at the age of 1 month. expression hCd39 was detected in every tissue (kidney, pancreas, brain, muscle, heart, liver, spleen, lung, umbilical cord) and primary cells (ﬁbroblasts and porcine aortic endothelial cells) analyzed with wb and iCC whereas hCd55 was not detected only in brain sample. we obtained a gal-ko piglet with ubiquitous high hCd39+hCd55 expression using the pCaggs promoter and he survived for one month without any apparent disorder. more pregnancies are ongoing with the same cell clones. the function of these two transgenes combination will be tested by xenotransplantation to primates as soon as more animals will be available",

keywords = "CD39, CD55, transgenic pig, xenotransplantation, CD39, CD55, transgenic pig, xenotransplantation",

author = "Andrea Perota and Irina Lagutina and Silvia Colleoni and Roberto Duchi and Giovanna Lazzari and Emanuele Cozzi and Fiorella Calabrese and Mathias Chatelais and Beatrice Charreau and Franco Lucchini and Cesare Galli",

year = "2011",

doi = "10.1111/j.1399-3089.2011.00661.x",

language = "English",

volume = "18",

pages = "297--297",

journal = "Xenotransplantation",

issn = "0908-665X",

publisher = "Wiley-Blackwell Publishing Ltd",

note = "Joint Congress of the Cell Transplant Society (CTS) and the International Xenotranplantation Association (IXA ; Conference date: 23-10-2011 Through 26-10-2011",

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TY - JOUR

T1 - High ubiquitous hCD55 and hCD39 co-expression in live transgenic alpha1,3-Gal Knock-out piglet

AU - Perota, Andrea

AU - Lagutina, Irina

AU - Colleoni, Silvia

AU - Duchi, Roberto

AU - Lazzari, Giovanna

AU - Cozzi, Emanuele

AU - Calabrese, Fiorella

AU - Chatelais, Mathias

AU - Charreau, Beatrice

AU - Lucchini, Franco

AU - Galli, Cesare

PY - 2011

Y1 - 2011

N2 - in xenotransplantation studies (pig to non-human primates) it was demonstrated that alpha-1,3 galactosyltransferase gene deletion (gal-ko) protected transplanted organs from hyperacute rejection. However the vascular acute rejection (avr) has to be solved through genetic engineering of donors inserting different human transgenes involved into prevention of complement activation (hCd55), coagulation and inﬂammation (hCd39) pathways. we created two different ubiquitous expression vectors for hCd55 (53mdH) and hCd39 (2JC9) exploiting the pCaggs promoter. primary ﬁbroblasts (1x10 6 ) from gal-ko pig were co-transfected with 5 micrograms of 53mdH+2JC9 (1:3) using nucleofector technology. after 24 hours, selection medium (Hygromicine = 175 ug/ml) was added to transfected cells and maintained for 15 days. sixty well growing resistant clones were picked up and analyzed for transgenes expression using western blot (wb) and immunocytochemistry (iCC). about 28% of colonies (n=17) showed high and uniform expression of both transgenes. four colonies were used as cell donors for sCnt and 265 cloned compacted morula and blastocysts d6 were transferred into 3 synchronized recipient sows. all sows became pregnant, 2 aborted at 30 th day, but one went to term (33%) and delivered one alive piglet and mummiﬁed fetus. the piglet died for e.coli infection at the age of 1 month. expression hCd39 was detected in every tissue (kidney, pancreas, brain, muscle, heart, liver, spleen, lung, umbilical cord) and primary cells (ﬁbroblasts and porcine aortic endothelial cells) analyzed with wb and iCC whereas hCd55 was not detected only in brain sample. we obtained a gal-ko piglet with ubiquitous high hCd39+hCd55 expression using the pCaggs promoter and he survived for one month without any apparent disorder. more pregnancies are ongoing with the same cell clones. the function of these two transgenes combination will be tested by xenotransplantation to primates as soon as more animals will be available

AB - in xenotransplantation studies (pig to non-human primates) it was demonstrated that alpha-1,3 galactosyltransferase gene deletion (gal-ko) protected transplanted organs from hyperacute rejection. However the vascular acute rejection (avr) has to be solved through genetic engineering of donors inserting different human transgenes involved into prevention of complement activation (hCd55), coagulation and inﬂammation (hCd39) pathways. we created two different ubiquitous expression vectors for hCd55 (53mdH) and hCd39 (2JC9) exploiting the pCaggs promoter. primary ﬁbroblasts (1x10 6 ) from gal-ko pig were co-transfected with 5 micrograms of 53mdH+2JC9 (1:3) using nucleofector technology. after 24 hours, selection medium (Hygromicine = 175 ug/ml) was added to transfected cells and maintained for 15 days. sixty well growing resistant clones were picked up and analyzed for transgenes expression using western blot (wb) and immunocytochemistry (iCC). about 28% of colonies (n=17) showed high and uniform expression of both transgenes. four colonies were used as cell donors for sCnt and 265 cloned compacted morula and blastocysts d6 were transferred into 3 synchronized recipient sows. all sows became pregnant, 2 aborted at 30 th day, but one went to term (33%) and delivered one alive piglet and mummiﬁed fetus. the piglet died for e.coli infection at the age of 1 month. expression hCd39 was detected in every tissue (kidney, pancreas, brain, muscle, heart, liver, spleen, lung, umbilical cord) and primary cells (ﬁbroblasts and porcine aortic endothelial cells) analyzed with wb and iCC whereas hCd55 was not detected only in brain sample. we obtained a gal-ko piglet with ubiquitous high hCd39+hCd55 expression using the pCaggs promoter and he survived for one month without any apparent disorder. more pregnancies are ongoing with the same cell clones. the function of these two transgenes combination will be tested by xenotransplantation to primates as soon as more animals will be available

KW - CD39

KW - CD55

KW - transgenic pig

KW - xenotransplantation

KW - CD39

KW - CD55

KW - transgenic pig

KW - xenotransplantation

UR - http://hdl.handle.net/10807/23254

UR - http://onlinelibrary.wiley.com/doi/10.1111/j.1399-3089.2011.00661.x/pdf

U2 - 10.1111/j.1399-3089.2011.00661.x

DO - 10.1111/j.1399-3089.2011.00661.x

M3 - Conference article

SN - 0908-665X

VL - 18

SP - 297

EP - 297

JO - Xenotransplantation

JF - Xenotransplantation

T2 - Joint Congress of the Cell Transplant Society (CTS) and the International Xenotranplantation Association (IXA

Y2 - 23 October 2011 through 26 October 2011

ER -

High ubiquitous hCD55 and hCD39 co-expression in live transgenic alpha1,3-Gal Knock-out piglet

Abstract

Keywords

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