We present the results of a pilot study using pentamer (PM) and streptamer (ST) multimer complexes for monitoring CMV-specific CD8+ T-cells (CTLs). We analysed 15 patients that underwent allogeneic Stem Cell Transplantation (HSCT). Patient characteristics are summarized in Table 1. All patients and donors were positive for the HLA-A*02:01 allele. PM and ST were directed against the epitope NLVPMVATV (495-503) of the CMV phosphoprotein 65 (pp65). Samples were obtained at 15-day intervals until day +90 and monthly thereafter.
| Patient | CMV status (D/R) | Gender | Age | Diagnosis | Donor | Conditioning | Engraftment (day) | Follow up (months) | GVHD (day) |
|---|---|---|---|---|---|---|---|---|---|
| 1 | +/+ | F | 43 | NHL | SIB | RIC | 24 | 15 | - |
| 2 | -/+ | F | 33 | MDS | URD | RIC | 19 | 12 | - |
| 3 | +/+ | M | 55 | AML | SIB | MAC | 17 | 14 | 47 |
| 4 | -/+ | F | 41 | AML | URD | MAC | 21 | 21 | - |
| 5 | +/+ | F | 32 | AML | SIB | MAC | 20 | 13 | 25 |
| 6 | +/+ | F | 64 | MDS | SIB | RIC | 27 | 14 | 89 |
| 7 | -/+ | M | 58 | CLL | URD | RIC | 23 | 13 | 92 |
| 8 | +/+ | M | 57 | ALL | URD | MAC | 15 | 5 | - |
| 9 | +/+ | F | 39 | AML | URD | MAC | 20 | 12 | - |
| 10 | -/+ | M | 42 | ALL | URD | MAC | 21 | 25 | - |
| 11 | -/+ | M | 44 | AML | URD | MAC | 12 | 8 | 153 |
| 12 | +/+ | F | 65 | AML | SIB | RIC | 25 | 8 | - |
| 13 | -/+ | M | 27 | AML | SIB | MAC | 30 | 3 | 18 |
| 14 | +/+ | M | 65 | AML | SIB | RIC | 19 | 6 | 62 |
| 15 | +/- | F | 30 | SAA | SIB | RIC | 13 | 3 | - |
| Patient | CMV status (D/R) | Gender | Age | Diagnosis | Donor | Conditioning | Engraftment (day) | Follow up (months) | GVHD (day) |
|---|---|---|---|---|---|---|---|---|---|
| 1 | +/+ | F | 43 | NHL | SIB | RIC | 24 | 15 | - |
| 2 | -/+ | F | 33 | MDS | URD | RIC | 19 | 12 | - |
| 3 | +/+ | M | 55 | AML | SIB | MAC | 17 | 14 | 47 |
| 4 | -/+ | F | 41 | AML | URD | MAC | 21 | 21 | - |
| 5 | +/+ | F | 32 | AML | SIB | MAC | 20 | 13 | 25 |
| 6 | +/+ | F | 64 | MDS | SIB | RIC | 27 | 14 | 89 |
| 7 | -/+ | M | 58 | CLL | URD | RIC | 23 | 13 | 92 |
| 8 | +/+ | M | 57 | ALL | URD | MAC | 15 | 5 | - |
| 9 | +/+ | F | 39 | AML | URD | MAC | 20 | 12 | - |
| 10 | -/+ | M | 42 | ALL | URD | MAC | 21 | 25 | - |
| 11 | -/+ | M | 44 | AML | URD | MAC | 12 | 8 | 153 |
| 12 | +/+ | F | 65 | AML | SIB | RIC | 25 | 8 | - |
| 13 | -/+ | M | 27 | AML | SIB | MAC | 30 | 3 | 18 |
| 14 | +/+ | M | 65 | AML | SIB | RIC | 19 | 6 | 62 |
| 15 | +/- | F | 30 | SAA | SIB | RIC | 13 | 3 | - |
Three patterns were observed. In 3 patients (20%) no CMV-specific-CTLs could be detected despite several CMV reactivations, requiring prolonged cumulative antiviral therapy (median 68 days; range 67-136).
In 7 patients (47%) CMV reactivation occurred at a mean of 41 days (10-94) and triggered a rapid increase of CMV-specific-CTLs with a median of 22.7 x 105/L (range 1.3-279.7). The CMV-PCR became immediately negative and antiviral therapy was stopped promptly after a median of 15.5 days (6-23).
Finally, 5 patients (33%) showed an early immune reconstitution with CMV-specific-CTLs detected with a median of 0.7 x 105/L (range 0.2-2.8) in the absence of CMV-PCR reactivation at a median of 21 days (10-34) post-SCT. No CMV-PCR reactivation was observed in this group with a median follow-up of 12 months (5-14).
Monitoring CMV-specific-T-cells might be able to distinguish patients at higher risk of recurrent virus reactivation and in need of prolonged antiviral therapy. Patients with increasing CMV-specific-CTLs detectable at the time of CMV-PCR reactivation may only need a short course of antiviral therapy, while those with early CMV-specific-CTLs may be protected from CMV reactivation.
Using Multimer-based (Pentamer and Streptamer) monitoring of CMV-specific T-cell immune reconstitution after allogeneic HSCT may contribute to the clinical decision regarding when and for how long to commence anti-CMV therapy.
No relevant conflicts of interest to declare.
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