Cytosine arabinoside as a major risk factor for Streptococcus viridans septicemia following bone marrow transplantation: A 5-year prospective study

D. Engelhard; H. Elishoov; R. Or; E. Naparstek; A. Nagler; N. Strauss; G. Cividalli; M. Aker; N. Ramu; A. Simhon; G. Rahav; M. Shapiro; T. Sacks; Z. Gimon; K. Abu-Dalu; C. Brautbar; S. Slavin

Cytosine arabinoside as a major risk factor for Streptococcus viridans septicemia following bone marrow transplantation: A 5-year prospective study

D. Engelhard, H. Elishoov, R. Or, E. Naparstek, A. Nagler, N. Strauss, G. Cividalli, M. Aker, N. Ramu, A. Simhon, G. Rahav, M. Shapiro, T. Sacks, Z. Gimon, K. Abu-Dalu, C. Brautbar, S. Slavin

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48 Scopus citations

Abstract

The incidence and clinical course of nosocomial septicemia with Streptococcus viridans was evaluated prospectively in 242 consecutive bone marrow transplant (BMT) recipients throughout their 15-213 days' (median 47) hospitalization, including 4-58 days (median 18) of neutropenia. Initial empiric therapy for febrile neutropenia consisted of mezlocillin, gentamicin and cefazolin; glycopeptide was excluded, S. viridans septicemia occurred in 23/209 (11%) subjects with underlying malignant disease, and only during neutropenia with concomitant mucositis: in 20 subjects (four with ampicillin-resistant strains), S. viridans septicemia occurred at onset of febrile neutropenia, 1-5 days (median 4.5) post-BMT. All survived with an uncomplicated clinical course. Thus, glycopeptide seems unnecessary in the initial empiric antibiotic regimen. The other three subjects demonstrated S. viridans septicemia (two with ampicillin-resistant strains) on day 11 post-BMT; two died. The major risk identified was cytosine arabinoside administration in the conditioning regimen (P < 0.01).

Original language	English
Pages (from-to)	565-570
Number of pages	6
Journal	Bone Marrow Transplantation
Volume	16
Issue number	4
State	Published - 1995
Externally published	Yes

Keywords

Ara-C
Bone marrow transplantation
Neutropenia
Septicemia
Streptococcus viridans

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Engelhard, D., Elishoov, H., Or, R., Naparstek, E., Nagler, A., Strauss, N., Cividalli, G., Aker, M., Ramu, N., Simhon, A., Rahav, G., Shapiro, M., Sacks, T., Gimon, Z., Abu-Dalu, K., Brautbar, C., & Slavin, S. (1995). Cytosine arabinoside as a major risk factor for Streptococcus viridans septicemia following bone marrow transplantation: A 5-year prospective study. Bone Marrow Transplantation, 16(4), 565-570.

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title = "Cytosine arabinoside as a major risk factor for Streptococcus viridans septicemia following bone marrow transplantation: A 5-year prospective study",

abstract = "The incidence and clinical course of nosocomial septicemia with Streptococcus viridans was evaluated prospectively in 242 consecutive bone marrow transplant (BMT) recipients throughout their 15-213 days' (median 47) hospitalization, including 4-58 days (median 18) of neutropenia. Initial empiric therapy for febrile neutropenia consisted of mezlocillin, gentamicin and cefazolin; glycopeptide was excluded, S. viridans septicemia occurred in 23/209 (11%) subjects with underlying malignant disease, and only during neutropenia with concomitant mucositis: in 20 subjects (four with ampicillin-resistant strains), S. viridans septicemia occurred at onset of febrile neutropenia, 1-5 days (median 4.5) post-BMT. All survived with an uncomplicated clinical course. Thus, glycopeptide seems unnecessary in the initial empiric antibiotic regimen. The other three subjects demonstrated S. viridans septicemia (two with ampicillin-resistant strains) on day 11 post-BMT; two died. The major risk identified was cytosine arabinoside administration in the conditioning regimen (P < 0.01).",

keywords = "Ara-C, Bone marrow transplantation, Neutropenia, Septicemia, Streptococcus viridans",

author = "D. Engelhard and H. Elishoov and R. Or and E. Naparstek and A. Nagler and N. Strauss and G. Cividalli and M. Aker and N. Ramu and A. Simhon and G. Rahav and M. Shapiro and T. Sacks and Z. Gimon and K. Abu-Dalu and C. Brautbar and S. Slavin",

year = "1995",

language = "אנגלית",

volume = "16",

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journal = "Bone Marrow Transplantation",

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Engelhard, D, Elishoov, H, Or, R, Naparstek, E, Nagler, A, Strauss, N, Cividalli, G, Aker, M, Ramu, N, Simhon, A, Rahav, G, Shapiro, M, Sacks, T, Gimon, Z, Abu-Dalu, K, Brautbar, C & Slavin, S 1995, 'Cytosine arabinoside as a major risk factor for Streptococcus viridans septicemia following bone marrow transplantation: A 5-year prospective study', Bone Marrow Transplantation, vol. 16, no. 4, pp. 565-570.

TY - JOUR

T1 - Cytosine arabinoside as a major risk factor for Streptococcus viridans septicemia following bone marrow transplantation

T2 - A 5-year prospective study

AU - Engelhard, D.

AU - Elishoov, H.

AU - Or, R.

AU - Naparstek, E.

AU - Nagler, A.

AU - Strauss, N.

AU - Cividalli, G.

AU - Aker, M.

AU - Ramu, N.

AU - Simhon, A.

AU - Rahav, G.

AU - Shapiro, M.

AU - Sacks, T.

AU - Gimon, Z.

AU - Abu-Dalu, K.

AU - Brautbar, C.

AU - Slavin, S.

PY - 1995

Y1 - 1995

N2 - The incidence and clinical course of nosocomial septicemia with Streptococcus viridans was evaluated prospectively in 242 consecutive bone marrow transplant (BMT) recipients throughout their 15-213 days' (median 47) hospitalization, including 4-58 days (median 18) of neutropenia. Initial empiric therapy for febrile neutropenia consisted of mezlocillin, gentamicin and cefazolin; glycopeptide was excluded, S. viridans septicemia occurred in 23/209 (11%) subjects with underlying malignant disease, and only during neutropenia with concomitant mucositis: in 20 subjects (four with ampicillin-resistant strains), S. viridans septicemia occurred at onset of febrile neutropenia, 1-5 days (median 4.5) post-BMT. All survived with an uncomplicated clinical course. Thus, glycopeptide seems unnecessary in the initial empiric antibiotic regimen. The other three subjects demonstrated S. viridans septicemia (two with ampicillin-resistant strains) on day 11 post-BMT; two died. The major risk identified was cytosine arabinoside administration in the conditioning regimen (P < 0.01).

AB - The incidence and clinical course of nosocomial septicemia with Streptococcus viridans was evaluated prospectively in 242 consecutive bone marrow transplant (BMT) recipients throughout their 15-213 days' (median 47) hospitalization, including 4-58 days (median 18) of neutropenia. Initial empiric therapy for febrile neutropenia consisted of mezlocillin, gentamicin and cefazolin; glycopeptide was excluded, S. viridans septicemia occurred in 23/209 (11%) subjects with underlying malignant disease, and only during neutropenia with concomitant mucositis: in 20 subjects (four with ampicillin-resistant strains), S. viridans septicemia occurred at onset of febrile neutropenia, 1-5 days (median 4.5) post-BMT. All survived with an uncomplicated clinical course. Thus, glycopeptide seems unnecessary in the initial empiric antibiotic regimen. The other three subjects demonstrated S. viridans septicemia (two with ampicillin-resistant strains) on day 11 post-BMT; two died. The major risk identified was cytosine arabinoside administration in the conditioning regimen (P < 0.01).

KW - Ara-C

KW - Bone marrow transplantation

KW - Neutropenia

KW - Septicemia

KW - Streptococcus viridans

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C2 - 8528173

AN - SCOPUS:0028842574

SN - 0268-3369

VL - 16

SP - 565

EP - 570

JO - Bone Marrow Transplantation

JF - Bone Marrow Transplantation

IS - 4

ER -

Cytosine arabinoside as a major risk factor for Streptococcus viridans septicemia following bone marrow transplantation: A 5-year prospective study

Abstract

Keywords

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