In vitro T cell proliferation from kidney allograft biopsies with unremarkable pathology: New strategies for an old problem

Craig R. Smith; Andrés Jaramillo; Nancy J. Poindexter; Nancy S. Steward; Kim C. Lu; Daniel C. Brennan; Gary G. Singer; Brent W. Miller; Martin D. Jendrisak; Surendra Shenoy; Jeffrey A. Lowell; Todd K. Howard; T. Mohanakumar

doi:10.1097/00007890-200201150-00026

In vitro T cell proliferation from kidney allograft biopsies with unremarkable pathology: New strategies for an old problem

Craig R. Smith, Andrés Jaramillo, Nancy J. Poindexter, Nancy S. Steward, Kim C. Lu, Daniel C. Brennan, Gary G. Singer, Brent W. Miller, Martin D. Jendrisak, Surendra Shenoy, Jeffrey A. Lowell, Todd K. Howard, T. Mohanakumar

Research output: Contribution to journal › Article › peer-review

5 Scopus citations

Abstract

Acute rejection of renal allografts is mediated by infiltrating alloreactive T cells. The goals of this study were to correlate T cell proliferation with rejection and to determine whether T cell proliferation in the absence of rejection would predict future rejection episodes. Toward this, kidney biopsies (n=100) were cultured in the presence of interleukin-2. Cultures were examined at 4, 24, and 48 hr for T cell proliferation. A strong correlation was observed between T cell proliferation at any time point and rejection. There was not a significant correlation between T cell proliferation in biopsies with no rejection and the occurrence of a rejection episode within 2 months. However, T cell proliferation after 4 hr was a better predictor of the occurrence of rejection within 2 months compared with observations after 24 and 48 hr. Therefore, a subgroup of patients with unremarkable biopsies but T cell proliferation may be at risk for rejection and warrant closer observation and possible tailoring of immunosuppression.

Original language	English (US)
Pages (from-to)	142-145
Number of pages	4
Journal	Transplantation
Volume	73
Issue number	1
DOIs	https://doi.org/10.1097/00007890-200201150-00026
State	Published - Jan 15 2002
Externally published	Yes

ASJC Scopus subject areas

Transplantation

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Smith, C. R., Jaramillo, A., Poindexter, N. J., Steward, N. S., Lu, K. C., Brennan, D. C., Singer, G. G., Miller, B. W., Jendrisak, M. D., Shenoy, S., Lowell, J. A., Howard, T. K., & Mohanakumar, T. (2002). In vitro T cell proliferation from kidney allograft biopsies with unremarkable pathology: New strategies for an old problem. Transplantation, 73(1), 142-145. https://doi.org/10.1097/00007890-200201150-00026

Smith, CR, Jaramillo, A, Poindexter, NJ, Steward, NS, Lu, KC, Brennan, DC, Singer, GG, Miller, BW, Jendrisak, MD, Shenoy, S, Lowell, JA, Howard, TK & Mohanakumar, T 2002, 'In vitro T cell proliferation from kidney allograft biopsies with unremarkable pathology: New strategies for an old problem', Transplantation, vol. 73, no. 1, pp. 142-145. https://doi.org/10.1097/00007890-200201150-00026

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title = "In vitro T cell proliferation from kidney allograft biopsies with unremarkable pathology: New strategies for an old problem",

abstract = "Acute rejection of renal allografts is mediated by infiltrating alloreactive T cells. The goals of this study were to correlate T cell proliferation with rejection and to determine whether T cell proliferation in the absence of rejection would predict future rejection episodes. Toward this, kidney biopsies (n=100) were cultured in the presence of interleukin-2. Cultures were examined at 4, 24, and 48 hr for T cell proliferation. A strong correlation was observed between T cell proliferation at any time point and rejection. There was not a significant correlation between T cell proliferation in biopsies with no rejection and the occurrence of a rejection episode within 2 months. However, T cell proliferation after 4 hr was a better predictor of the occurrence of rejection within 2 months compared with observations after 24 and 48 hr. Therefore, a subgroup of patients with unremarkable biopsies but T cell proliferation may be at risk for rejection and warrant closer observation and possible tailoring of immunosuppression.",

author = "Smith, {Craig R.} and Andr{\'e}s Jaramillo and Poindexter, {Nancy J.} and Steward, {Nancy S.} and Lu, {Kim C.} and Brennan, {Daniel C.} and Singer, {Gary G.} and Miller, {Brent W.} and Jendrisak, {Martin D.} and Surendra Shenoy and Lowell, {Jeffrey A.} and Howard, {Todd K.} and T. Mohanakumar",

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AU - Poindexter, Nancy J.

AU - Steward, Nancy S.

AU - Lu, Kim C.

AU - Brennan, Daniel C.

AU - Singer, Gary G.

AU - Miller, Brent W.

AU - Jendrisak, Martin D.

AU - Shenoy, Surendra

AU - Lowell, Jeffrey A.

AU - Howard, Todd K.

AU - Mohanakumar, T.

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N2 - Acute rejection of renal allografts is mediated by infiltrating alloreactive T cells. The goals of this study were to correlate T cell proliferation with rejection and to determine whether T cell proliferation in the absence of rejection would predict future rejection episodes. Toward this, kidney biopsies (n=100) were cultured in the presence of interleukin-2. Cultures were examined at 4, 24, and 48 hr for T cell proliferation. A strong correlation was observed between T cell proliferation at any time point and rejection. There was not a significant correlation between T cell proliferation in biopsies with no rejection and the occurrence of a rejection episode within 2 months. However, T cell proliferation after 4 hr was a better predictor of the occurrence of rejection within 2 months compared with observations after 24 and 48 hr. Therefore, a subgroup of patients with unremarkable biopsies but T cell proliferation may be at risk for rejection and warrant closer observation and possible tailoring of immunosuppression.

AB - Acute rejection of renal allografts is mediated by infiltrating alloreactive T cells. The goals of this study were to correlate T cell proliferation with rejection and to determine whether T cell proliferation in the absence of rejection would predict future rejection episodes. Toward this, kidney biopsies (n=100) were cultured in the presence of interleukin-2. Cultures were examined at 4, 24, and 48 hr for T cell proliferation. A strong correlation was observed between T cell proliferation at any time point and rejection. There was not a significant correlation between T cell proliferation in biopsies with no rejection and the occurrence of a rejection episode within 2 months. However, T cell proliferation after 4 hr was a better predictor of the occurrence of rejection within 2 months compared with observations after 24 and 48 hr. Therefore, a subgroup of patients with unremarkable biopsies but T cell proliferation may be at risk for rejection and warrant closer observation and possible tailoring of immunosuppression.

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In vitro T cell proliferation from kidney allograft biopsies with unremarkable pathology: New strategies for an old problem

Abstract

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