Early predictors of transplant-related mortality (TRM) after allogeneic bone marrow transplants (BMT): blood urea nitrogen (BUN) and bilirubin

Summary:We monitored levels of C-reactive protein (CRP) in 96 consecutive adult allogeneic BMT patients (age 15-50 years) transplanted in our unit. Major transplantrelated complications (MTC) occurred in 32% of cases and included: hepatic veno-occlusive disease, pneumonitis, severe endothelial leakage syndrome and >II acute GVHD. Transplant-related mortality (TRM) before day 100 post-BMT was 13.5%. Variables included in a stepwise logistic regression model were: gender, age, disease category, donor type, T cell depletion, TBI, use of growth factors, bacteremia, mean CRP-levels >50 mg/l between days 0 and 5 (CRP day 0-5) and >100 mg/l between days 6 and 10 (CRP day 6-10) post-BMT. Only high CRP-levels (for MTC and TRM) (P < 0.001) and donor-type (for TRM) (P ‫؍‬ 0.02) were independent risk factors. The estimated probability for MTC was 73% (CRP day 6-10 >100 mg/l) vs 17% (CRP day 6-10 <100 mg/l). Using the same cut-off levels, the probabilities for TRM were 36.5% vs 1% in the identical sibling donor situation and 88% vs 12.5% in other donor-type transplants. We conclude that the degree of systemic inflammation, as reflected by CRP-levels, during the first 5-10 days after BMT identifies patients at risk of MTC and TRM. Our data may be useful in selecting patients for clinical trials involving pre-emptive antiinflammatory treatment. Bone Marrow Transplantation (2002) 30, 441-446. doi:10.1038/sj.bmt.1703672 Keywords: C-reactive protein; severe complications; transplant-related mortality; allogeneic BMT Despite improvements in supportive care, the practice of allogeneic BMT remains limited by its toxicity. Overall

Section: Discussionmentioning

confidence: 99%

“…5 Also, an early increase in serum bilirubin and/or blood urea nitrogen (BUN) after BMT has been associated with TRM. 6 Tissue damage can lead to a systemic inflammatory response. C-reactive protein (CRP) is an acute phase protein produced by hepatocytes and is a reliable marker of systemic inflammation.…”

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confidence: 99%

An early increase in serum levels of C-reactive protein is an independent risk factor for the occurrence of major complications and 100-day transplant-related mortality after allogeneic bone marrow transplantation

Schots

Riet

Othman³

et al. 2002

“…Developing a strategy for pre-emptive intervention against acute GVHD is more difficult to achieve, given the inherent treatment of some patients who would not have developed disease. In 1999, Bacigalupo et al 48 used a clinical scoring system, measured at day þ 7 after HCT, to predict risk of both acute GVHD and TRM. A pilot study in 18 patients followed, which treated highrisk patients with pre-emptive anti-thymocyte globulin, 49 and this clinical scoring system was then refined to include day þ 7 serum levels of BUN, cholinesterase, total proteins, gamma glutamyl transferase, along with donor type and cell dose.…”

Section: Biomarkers For Acute Gvhd Y-b Chen and Cs Cutlermentioning

confidence: 99%

Biomarkers for acute GVHD: can we predict the unpredictable?

2012

Acute GVHD remains an important complication after allogeneic hematopoietic cell transplantation (HCT). Many efforts have been devoted to identifying potential noninvasive peripheral blood biomarkers to help improve the diagnosis or management of acute GVHD while avoiding invasive tissue biopsies. Early attempts to identify biomarkers focused on inflammatory cytokines, especially IL-2 or TNF-a, however, both of these and others were not specific for GVHD, often being elevated in the setting of generalized inflammation, accompanying other major complications of HCT as well. More recent efforts have focused on additional cytokines and other cell-surface molecules, which function in leukocyte trafficking and activation with the hope that these can also serve as targets for novel therapeutic approaches. Modern proteomic methods have allowed the screening of large numbers of patient samples and yielded several novel candidate biomarkers, including elafin and reg3a, which may not be directly involved in the immunological pathogenesis of GVHD, but may be unique biomarkers for end-organ injury. Combining these new molecules with traditionally identified cytokines to form an acute GVHD biomarker panel has recently shown the ability to predict outcomes in patients who develop acute GVHD. The ultimate goals of identifying a specific biomarker are to refine diagnosis, guide therapy and develop risk-adapted approaches in order to better treat patients and improve outcomes after allogeneic HCT. These approaches include differential treatment for patients who develop acute GVHD with a high-risk biomarker profile as well as pre-emptive therapy in patients after HCT prior to the development of symptoms. With the recent progress summarized below, these goals may soon be realized.

“…However, one first needs to identify patients at risk of GVHD soon after transplant, and with this aim, we worked on a scoring system on day þ 7 after HSCT, first based on day þ 7 bilirubin and blood urea nitrogen. 12 These two laboratory tests identify patients with a significantly different risk of GVHD and transplantrelated mortality (TRM), as shown in our Unit of adult transplants and validated in a separate pediatric Unit using a different central lab. 12 The next step was to test whether an early intervention with immunosuppression was feasible and whether it would reduce severe acute GVHD: we ran a small pilot study with ATG 1.25 mg/kg 3 Â starting on day þ 7, in 18 high-risk patients, and compared the results with a historic group of 20 untreated high-risk patients (controls), and showed reduced acute GVHD in patients receiving the additional dose of ATG on day þ 7.…”

Section: Introductionmentioning

confidence: 96%

“…12 These two laboratory tests identify patients with a significantly different risk of GVHD and transplantrelated mortality (TRM), as shown in our Unit of adult transplants and validated in a separate pediatric Unit using a different central lab. 12 The next step was to test whether an early intervention with immunosuppression was feasible and whether it would reduce severe acute GVHD: we ran a small pilot study with ATG 1.25 mg/kg 3 Â starting on day þ 7, in 18 high-risk patients, and compared the results with a historic group of 20 untreated high-risk patients (controls), and showed reduced acute GVHD in patients receiving the additional dose of ATG on day þ 7. 13 We were in the meantime refining the scoring system on day þ 7, and found other significant laboratory tests such as serum cholinesterase, total serum proteins and gamma glutamyl transferase: 14 the revised day þ 7 score identifies patients with a low risk (15%), an intermediate risk (40%) and a high risk of TRM (60%).…”

Section: Introductionmentioning

confidence: 96%

Pre-emptive treatment of acute GVHD: a randomized multicenter trial of rabbit anti-thymocyte globulin, given on day+7 after alternative donor transplants

Bacigalupo

Lamparelli

Milone

et al. 2009

Self Cite

We have previously shown that hemopoietic stem cell transplant (HSCT) recipients can be stratified on day þ 7 as having low, intermediate or a high risk of transplantrelated mortality (TRM). With the aim of reducing TRM and GVHD, intermediate and high-risk patients (n ¼ 170) were randomized to receive anti-thymocyte globulin (ATG, thymoglobuline) on day þ 7 (n ¼ 84) or no treatment (n ¼ 86) (controls). There was a reduction of TRM from 35% in controls to 29% in ATG patients (P ¼ 0.3), of acute GVHD III-IV from 15 to 5% (P ¼ 0.02) and of chronic GVHD from 26 to 11% (P ¼ 0.03); survival was comparable. The predictive value of the day þ 7 score on TRM was confirmed for controls (19 vs 42% for intermediate vs high risk, respectively, P ¼ 0.03), whereas ATG abrogated this predictive effect (29 vs 29%). ATG reduced GVHD (P ¼ 0.006) in high-risk patients, but not in patients with an intermediate risk.In conclusion, we confirm that TRM can be predicted on the basis of day þ 7 laboratory values, after alternative donor HSCT; in high-, but not intermediate-risk patients, the administration of ATG on day þ 7 reduces GVHD. These results may represent a platform for risk-adapted post transplant immune modulation.