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Dive into the research topics where Nora Naumann is active.

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Featured researches published by Nora Naumann.


Journal of Clinical Investigation | 2009

In vivo selection of hematopoietic progenitor cells and temozolomide dose intensification in rhesus macaques through lentiviral transduction with a drug resistance gene

André Larochelle; Uimook Choi; Yan Shou; Nora Naumann; Natalia A. Loktionova; Joshua R. Clevenger; Allen Krouse; Mark E. Metzger; Robert E. Donahue; Elizabeth M. Kang; Clinton F. Stewart; Derek A. Persons; Harry L. Malech; Cynthia E. Dunbar; Brian P. Sorrentino

Major limitations to gene therapy using HSCs are low gene transfer efficiency and the inability of most therapeutic genes to confer a selective advantage on the gene-corrected cells. One approach to enrich for gene-modified cells in vivo is to include in the retroviral vector a drug resistance gene, such as the P140K mutant of the DNA repair enzyme O6-methylguanine-DNA methyltransferase (MGMT*). We transplanted 5 rhesus macaques with CD34+ cells transduced with lentiviral vectors encoding MGMT* and a fluorescent marker, with or without homeobox B4 (HOXB4), a potent stem cell self-renewal gene. Transgene expression and common integration sites in lymphoid and myeloid lineages several months after transplantation confirmed transduction of long-term repopulating HSCs. However, all animals showed only a transient increase in gene-marked lymphoid and myeloid cells after O6-benzylguanine (BG) and temozolomide (TMZ) administration. In 1 animal, cells transduced with MGMT* lentiviral vectors were protected and expanded after multiple courses of BG/TMZ, providing a substantial increase in the maximum tolerated dose of TMZ. Additional cycles of chemotherapy using 1,3-bis-(2-chloroethyl)-1-nitrosourea (BCNU) resulted in similar increases in gene marking levels, but caused high levels of nonhematopoietic toxicity. Inclusion of HOXB4 in the MGMT* vectors resulted in no substantial increase in gene marking or HSC amplification after chemotherapy treatment. Our data therefore suggest that lentivirally mediated gene transfer in transplanted HSCs can provide in vivo chemoprotection of progenitor cells, although selection of long-term repopulating HSCs was not seen.


Pediatrics | 2006

Sarcoidosis in Chronic Granulomatous Disease

Suk See De Ravin; Nora Naumann; Michael R. Robinson; Karyl S. Barron; David E. Kleiner; Jean Ulrick; Julia Friend; Victoria L. Anderson; Dirk N. Darnell; Elizabeth M. Kang; Harry L. Malech

In addition to increased susceptibility to infections in patients with chronic granulomatous disease (CGD), a higher incidence of sterile inflammatory disorders in these patients has been noted. However, sarcoidosis has not been reported previously in CGD. In this report, we describe two patients who have CGD and a disorder consistent with sarcoidosis on the basis of unequivocal clinical-radiographic presentations, their responses to treatment, and serum angiotensin-converting enzyme levels. Serum angiotensin-converting enzyme levels were measured in 26 other patients with CGD to establish an appropriate reference range. A possible relationship between CGD and sarcoidosis is discussed.


Blood | 2007

Gene therapy improves immune function in preadolescents with X-linked severe combined immunodeficiency

Javier Chinen; Joie Davis; Suk See De Ravin; Beverly N. Hay; Amy P. Hsu; Gilda F. Linton; Nora Naumann; Effie Nomicos; Christopher Silvin; Jean Ulrick; Narda L. Whiting-Theobald; Harry L. Malech; Jennifer M. Puck


Blood | 2006

Correction of canine X-linked severe combined immunodeficiency by in vivo retroviral gene therapy

Suk See De Ravin; Douglas R. Kennedy; Nora Naumann; Jeffrey S. Kennedy; Uimook Choi; Brian J. Hartnett; Gilda F. Linton; Narda L. Whiting-Theobald; Peter F. Moore; William Vernau; Harry L. Malech; Peter J. Felsburg


Archive | 2013

vivo retroviral gene therapy Correction of canine x-linked severe combined immunodeficiency by in

Peter J. Felsburg; Gilda F. Linton; Narda L. Whiting-Theobald; Peter F Moore; William Vernau; Harry L. Malech; Douglas R. Kennedy; Nora Naumann; Jeffrey S. Kennedy; Brian J


Archive | 2007

Gene Therapy Improves Immune Function in Pre-adolescents with X-linked Severe Combined Immunodeficiency Short Title for Running Head: Gene Therapy for XSCID pre-adolescents

Javier Chinen; Joie Davis; Suk See De Ravin; Beverly N. Hay; Amy P. Hsu; Gilda F. Linton; Nora Naumann; Effie Nomicos; Christopher Silvin; Jean Ulrick; Narda L. Whiting-Theobald; Harry L. Malech; Jennifer M. Puck


Molecular Therapy | 2006

671. SIV-Derived Lentiviral Vectors Pseudotyped with Modified RD114 Envelope and Containing Mutant MGMT Efficiently Transduce Human CD34+ PBSCs and Allow Selection

Nora Naumann; Uimook Choi; Suk See De Ravin; Morvarid Moayeri; Larry Lantz; Lanise Cardwell-Miller; Harry L. Malech


Blood | 2006

Correction of canine X-linked severe combined immunodeficiency by in vivo retroviral gene therapy. Commentary

Katherine P. Ponder; Suk See Ting-De Ravin; Douglas R. Kennedy; Nora Naumann; Jeffrey S. Kennedy; Uimook Choi; Brian J. Hartnett; Gilda F. Linton; Narda L. Whiting-Theobald; Peter F. Moore; William Vernau; Harry L. Malech; Peter J. Felsburg


Blood | 2006

Correction of Human X-Linked Chronic Granulomatous Disease (X-CGD) Following Transduction of X-CGD CD34+ Cells with a Modified RD114-Pseudotyped Simian Immunodeficiency Virus Lentiviral Vector in a NOD/SCID Mouse Xenograft Model.

Nora Naumann; Suk See De Ravin; Uimook Choi; Morvarid Moayeri; Yasuhiro Ikeda; Harry L. Malech


Blood | 2006

Improvement of Canine XSCID by In Vivo Gene Therapy Using RD114/TR-Pseudotyped SIV Lentiviral Vectors.

Morvarid Moayeri; Suk See De Ravin; Douglas R. Kennedy; Nora Naumann; Yasuhiro Ikeda; Peter J. Felsburg; Harry L. Malech

Collaboration


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Harry L. Malech

National Institutes of Health

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Suk See De Ravin

National Institutes of Health

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Gilda F. Linton

National Institutes of Health

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Uimook Choi

National Institutes of Health

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Peter J. Felsburg

University of Pennsylvania

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William Vernau

University of California

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Brian J. Hartnett

University of Pennsylvania

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