ISSN 1866-8836
Клеточная терапия и трансплантация
Change template to: announce
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Balashov, Pavel E. Trakhtman, Elena V. Skorobogatova, Yulia V. Skvortsova, Zarema M. Dyshlevaja, Irina P. Shipitsina, Alexey A. Maschan, Alexander G. Rumyantsev</p>" ["TYPE"]=> string(4) "HTML" } ["DESCRIPTION"]=> string(0) "" ["VALUE_ENUM"]=> NULL ["VALUE_XML_ID"]=> NULL ["VALUE_SORT"]=> NULL ["~VALUE"]=> array(2) { ["TEXT"]=> string(177) "

Dmitry N. Balashov, Pavel E. Trakhtman, Elena V. Skorobogatova, Yulia V. Skvortsova, Zarema M. Dyshlevaja, Irina P. Shipitsina, Alexey A. Maschan, Alexander G. Rumyantsev

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Federal Research and Clinical Centre of Pediatric Hematology, Oncology and Immunology, Moscow, Russia

Correspondence
Dmitry N. Balashov, Federal Research and Clinical Centre of Pediatric Hematology, Oncology and Immunology, 117/2, Leninsky prosp, Moscow, Russia, 105062
Phone: +7(495) 9369023, Fax +7(495)9369120
E-mail: bala8@yandex.ru

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HSCT is the standard, and an effective method of therapy of SCID patients. Unfortunately, the poor somatic status of children and/or infectious complications are often grounds for the modification of the existing standard approach to HSCT in SCID. In some cases, decreasing the intensity of conditioning regimens seems to be the cause of mixed chimerism, delayed immunological reconstitution, long-term (or life-long) demand for IVIG transfusions, and an increase in morbidity and mortality after HSCT. Currently there are many publications about gene therapy. It’s a new and promising approach to the treatment of SCID patients. Perhaps it will be a good alternative for the standard HSCT method in the future.

Between 1997 and 2009, twelve patients (1 female and 11 males) with a median age of 6 months (range 2–12 months) received standard HSCT for SCID at the Federal Research and Clinical Centre of Pediatric Hematology, Oncology and Immunology. In 7 patients we found genetic mutations, and confirmed X1-SCID (n=5), ADA-deficient-SCID (n=1), and Omenn's syndrome (n=1). In other cases we did not discover any genetic mutations, but patients showed clinical signs and immunological phenotypes that match SCID. One patient was transplanted from an HLA-compatible sibling donor, other cases were treated with haploidentical HSCT from their parents. At present, the median follow-up is 76 months (range 3–164 months); 7 children are alive and have full donor chimerism, and five of them demonstrate full immunological reconstitution. 

Currently, gene therapy is not available for most patients, but HSCT is an effective method of treatment for SCID patients.

Keywords

SCID, transplantation, conditioning, gene therapy, children

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Balashov, Pavel E. Trakhtman, Elena V. Skorobogatova, Yulia V. Skvortsova, Zarema M. Dyshlevaja, Irina P. Shipitsina, Alexey A. Maschan, Alexander G. Rumyantsev</p>" ["TYPE"]=> string(4) "HTML" } ["DESCRIPTION"]=> string(0) "" ["VALUE_ENUM"]=> NULL ["VALUE_XML_ID"]=> NULL ["VALUE_SORT"]=> NULL ["~VALUE"]=> array(2) { ["TEXT"]=> string(177) "

Dmitry N. Balashov, Pavel E. Trakhtman, Elena V. Skorobogatova, Yulia V. Skvortsova, Zarema M. Dyshlevaja, Irina P. Shipitsina, Alexey A. Maschan, Alexander G. Rumyantsev

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Dmitry N. Balashov, Pavel E. Trakhtman, Elena V. Skorobogatova, Yulia V. Skvortsova, Zarema M. Dyshlevaja, Irina P. Shipitsina, Alexey A. Maschan, Alexander G. Rumyantsev

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HSCT is the standard, and an effective method of therapy of SCID patients. Unfortunately, the poor somatic status of children and/or infectious complications are often grounds for the modification of the existing standard approach to HSCT in SCID. In some cases, decreasing the intensity of conditioning regimens seems to be the cause of mixed chimerism, delayed immunological reconstitution, long-term (or life-long) demand for IVIG transfusions, and an increase in morbidity and mortality after HSCT. Currently there are many publications about gene therapy. It’s a new and promising approach to the treatment of SCID patients. Perhaps it will be a good alternative for the standard HSCT method in the future.

Between 1997 and 2009, twelve patients (1 female and 11 males) with a median age of 6 months (range 2–12 months) received standard HSCT for SCID at the Federal Research and Clinical Centre of Pediatric Hematology, Oncology and Immunology. In 7 patients we found genetic mutations, and confirmed X1-SCID (n=5), ADA-deficient-SCID (n=1), and Omenn's syndrome (n=1). In other cases we did not discover any genetic mutations, but patients showed clinical signs and immunological phenotypes that match SCID. One patient was transplanted from an HLA-compatible sibling donor, other cases were treated with haploidentical HSCT from their parents. At present, the median follow-up is 76 months (range 3–164 months); 7 children are alive and have full donor chimerism, and five of them demonstrate full immunological reconstitution. 

Currently, gene therapy is not available for most patients, but HSCT is an effective method of treatment for SCID patients.

Keywords

SCID, transplantation, conditioning, gene therapy, children

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HSCT is the standard, and an effective method of therapy of SCID patients. Unfortunately, the poor somatic status of children and/or infectious complications are often grounds for the modification of the existing standard approach to HSCT in SCID. In some cases, decreasing the intensity of conditioning regimens seems to be the cause of mixed chimerism, delayed immunological reconstitution, long-term (or life-long) demand for IVIG transfusions, and an increase in morbidity and mortality after HSCT. Currently there are many publications about gene therapy. It’s a new and promising approach to the treatment of SCID patients. Perhaps it will be a good alternative for the standard HSCT method in the future.

Between 1997 and 2009, twelve patients (1 female and 11 males) with a median age of 6 months (range 2–12 months) received standard HSCT for SCID at the Federal Research and Clinical Centre of Pediatric Hematology, Oncology and Immunology. In 7 patients we found genetic mutations, and confirmed X1-SCID (n=5), ADA-deficient-SCID (n=1), and Omenn's syndrome (n=1). In other cases we did not discover any genetic mutations, but patients showed clinical signs and immunological phenotypes that match SCID. One patient was transplanted from an HLA-compatible sibling donor, other cases were treated with haploidentical HSCT from their parents. At present, the median follow-up is 76 months (range 3–164 months); 7 children are alive and have full donor chimerism, and five of them demonstrate full immunological reconstitution. 

Currently, gene therapy is not available for most patients, but HSCT is an effective method of treatment for SCID patients.

Keywords

SCID, transplantation, conditioning, gene therapy, children

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Federal Research and Clinical Centre of Pediatric Hematology, Oncology and Immunology, Moscow, Russia

Correspondence
Dmitry N. Balashov, Federal Research and Clinical Centre of Pediatric Hematology, Oncology and Immunology, 117/2, Leninsky prosp, Moscow, Russia, 105062
Phone: +7(495) 9369023, Fax +7(495)9369120
E-mail: bala8@yandex.ru

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Federal Research and Clinical Centre of Pediatric Hematology, Oncology and Immunology, Moscow, Russia

Correspondence
Dmitry N. Balashov, Federal Research and Clinical Centre of Pediatric Hematology, Oncology and Immunology, 117/2, Leninsky prosp, Moscow, Russia, 105062
Phone: +7(495) 9369023, Fax +7(495)9369120
E-mail: bala8@yandex.ru

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K. Inherited diseases

Hematopoietic stem cell transplantation (HSCT) in patients with severe combined immunodeficiency (SCID): experiences, possibilities, and prospects

Dmitry N. Balashov, Pavel E. Trakhtman, Elena V. Skorobogatova, Yulia V. Skvortsova, Zarema M. Dyshlevaja, Irina P. Shipitsina, Alexey A. Maschan, Alexander G. Rumyantsev

K. Inherited diseases

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Dmitry N. Balashov, Pavel E. Trakhtman, Elena V. Skorobogatova, Yulia V. Skvortsova, Zarema M. Dyshlevaja, Irina P. Shipitsina, Alexey A. Maschan, Alexander G. Rumyantsev

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Federal Research and Clinical Centre of Pediatric Hematology, Oncology and Immunology, Moscow, Russia

Correspondence
Dmitry N. Balashov, Federal Research and Clinical Centre of Pediatric Hematology, Oncology and Immunology, 117/2, Leninsky prosp, Moscow, Russia, 105062
Phone: +7(495) 9369023, Fax +7(495)9369120
E-mail: bala8@yandex.ru

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HSCT is the standard, and an effective method of therapy of SCID patients. Unfortunately, the poor somatic status of children and/or infectious complications are often grounds for the modification of the existing standard approach to HSCT in SCID. In some cases, decreasing the intensity of conditioning regimens seems to be the cause of mixed chimerism, delayed immunological reconstitution, long-term (or life-long) demand for IVIG transfusions, and an increase in morbidity and mortality after HSCT. Currently there are many publications about gene therapy. It’s a new and promising approach to the treatment of SCID patients. Perhaps it will be a good alternative for the standard HSCT method in the future.

Between 1997 and 2009, twelve patients (1 female and 11 males) with a median age of 6 months (range 2–12 months) received standard HSCT for SCID at the Federal Research and Clinical Centre of Pediatric Hematology, Oncology and Immunology. In 7 patients we found genetic mutations, and confirmed X1-SCID (n=5), ADA-deficient-SCID (n=1), and Omenn's syndrome (n=1). In other cases we did not discover any genetic mutations, but patients showed clinical signs and immunological phenotypes that match SCID. One patient was transplanted from an HLA-compatible sibling donor, other cases were treated with haploidentical HSCT from their parents. At present, the median follow-up is 76 months (range 3–164 months); 7 children are alive and have full donor chimerism, and five of them demonstrate full immunological reconstitution. 

Currently, gene therapy is not available for most patients, but HSCT is an effective method of treatment for SCID patients.

Keywords

SCID, transplantation, conditioning, gene therapy, children

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Hematopoietic stem cell transplantation (HSCT) in patients with severe combined immunodeficiency (SCID): experiences, possibilities, and prospects

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Dmitry N. Balashov, Pavel E. Trakhtman, Elena V. Skorobogatova, Yulia V. Skvortsova, Zarema M. Dyshlevaja, Irina P. Shipitsina, Alexey A. Maschan, Alexander G. Rumyantsev

Federal Research and Clinical Centre of Pediatric Hematology, Oncology and Immunology, Moscow, Russia

Correspondence
Dmitry N. Balashov, Federal Research and Clinical Centre of Pediatric Hematology, Oncology and Immunology, 117/2, Leninsky prosp, Moscow, Russia, 105062
Phone: +7(495) 9369023, Fax +7(495)9369120
E-mail: bala8@yandex.ru

HSCT is the standard, and an effective method of therapy of SCID patients. Unfortunately, the poor somatic status of children and/or infectious complications are often grounds for the modification of the existing standard approach to HSCT in SCID. In some cases, decreasing the intensity of conditioning regimens seems to be the cause of mixed chimerism, delayed immunological reconstitution, long-term (or life-long) demand for IVIG transfusions, and an increase in morbidity and mortality after HSCT. Currently there are many publications about gene therapy. It’s a new and promising approach to the treatment of SCID patients. Perhaps it will be a good alternative for the standard HSCT method in the future.

Between 1997 and 2009, twelve patients (1 female and 11 males) with a median age of 6 months (range 2–12 months) received standard HSCT for SCID at the Federal Research and Clinical Centre of Pediatric Hematology, Oncology and Immunology. In 7 patients we found genetic mutations, and confirmed X1-SCID (n=5), ADA-deficient-SCID (n=1), and Omenn's syndrome (n=1). In other cases we did not discover any genetic mutations, but patients showed clinical signs and immunological phenotypes that match SCID. One patient was transplanted from an HLA-compatible sibling donor, other cases were treated with haploidentical HSCT from their parents. At present, the median follow-up is 76 months (range 3–164 months); 7 children are alive and have full donor chimerism, and five of them demonstrate full immunological reconstitution. 

Currently, gene therapy is not available for most patients, but HSCT is an effective method of treatment for SCID patients.

Keywords

SCID, transplantation, conditioning, gene therapy, children