By
Liz Highleyman
Despite
effective ART, some people with full viral load suppression do not achieve robust
CD4 cell gains (known as discordant response). Furthermore, the cells that do
return may not have the same function as those lost. Several recent studies indicate
that spending more time with lower CD4 counts increases the risk of not only AIDS-defining
opportunistic illness, but also non-AIDS-related diseases such as cancer, well
before reaching the "danger zone" below 200 cells/mm3.
Yves
Levy and an international team of colleagues aimed to determine whether recombinant
human IL-7 would have a positive effect on T-cell recovery and thymic function
in HIV patients on ART
with undetectable viral load.
IL-7
is among the many cytokines, or chemical messengers, that influence immune system
activity. Two recently completed large trials, ESPRIT
AND SILCAAT, looked at another cytokine, interleukin 2 (IL-2). Other such
messengers are also under study.
Past
research by Levy and others has shown that IL-7 stimulates T-cell maturation and
release from the thymus, as well as inhibiting spontaneous CD4 and CD8 cell death.
The thymus is a gland in the upper chest where T-cells mature; it typically shrinks
and becomes less active as people age.
The
INSPIRE study included 22 participants randomly assigned to receive weekly injections
of 10 or 20 mcg/kg of IL-7 (using a preparation called CYT107) or placebo for
12 weeks. The study also has a 30 mcg/kg dose cohort, but Levy only reported interim
results from the 2 lower-dose groups.
All
study participants were men. Those receiving IL-7 had a median age of about 40
years; placebo recipients were on average about age 50. All had a viral load below
50 copies/mL. At the time of enrollment, CD4 count ranged from 101 to 400 cells/mm3
(median of about 270 cells/mm3), but the median nadir (lowest-ever) level was
100 cells/mm3, indicating advanced immune deficiency. The median CD8 count was
about 750 cells/mm3 and the median CD4/CD8 ratio was 0.35.
Results
 | Overall,
IL-7 appeared generally safe and well tolerated in the 10 and 20 mcg/kg dose cohorts
over 12 weeks. |
| No
serious adverse events or dose-limiting toxicities were reported. |
| Some
patients experienced mild-to-moderate local injection site reactions, but no systemic
reactions. |
| Viral
load generally remained suppressed, although 4 patients in the 20 mcg/kg group
experienced low-level transient "blips" (3 with 500 copies/mL or less,
1 with around 1000 copies/mL). |
|
Participants experienced significant increases in both CD4 and CD8 cell counts: |
| | | CD4
cells: | | | 
10 mcg/kg group: 152% increase from baseline (median 268 cells/mm3) to week 4
(median 643 cells/mm3), falling back to 87% by week 12 (median 419 cells/mm3).
|
| | | |
20 mcg/kg group: 205% increase from baseline (median 240 cells/mm3) to week 4
(median 709 cells/mm3), falling back to 135% by week 12 (median 563 cells/mm3). |
| | CD8
cells: | | | |
10 mcg/kg group: 91% increase from baseline (median 761 cells/mm3) to week 4 (median
1434 cells/mm3), falling back to 42% by week 12 (median 1081 cells/mm3). |
| | | |
20 mcg/kg group: 131% increase from baseline (median 659 cells/mm3) to week 4
(median 1695 cells/mm3), falling back to 65% by week 12 (median 1210 cells/mm3).
|
|
|
| 1
of 7 participants (14%) in the 10 mcg/kg group and 5 of 8 (63%) in the 20 mcg/kg
group reached a CD4 cell level above 500 cells/mm3, which took a median of 14
days. |
| There
were gains in both naive T-cells (not yet committed to fighting specific pathogens)
and central memory cells (which "remember" past invaders), but more
mature effector memory cells did not increase. |
| Patients'
thymus glands appeared to release more cells, leading to increased numbers of
"recent thymic emigrants." |
Based
on these findings, the researchers concluded that "A 3 injection cycle of
[recombinant human] IL-7 induces a dose-dependent and sustained increase of CD4
T-cells. A higher proportion of patients experienced CD4 counts > 500 cells/mm3
and a trend toward higher thymic output at 20 mcg/kg."Larger
and longer studies will be needed to determine whether these promising increases
in CD4 and CD8 cell levels translate into clinical benefits. As
reported earlier this year, ESPRIT AND SILCAAT showed that IL-2 did not lead
to improved long-term clinical outcomes or survival, even though it did produce
CD4 cell increases.
Levy
noted that the types of CD4 T-cells expanded by IL-7 are completely different
from those expanded by IL-2, and rather than looking at progression to AIDS or
death, as done in ESPRIT and SILCAAT, it may be possible to see beneficial clinical
outcomes sooner using different types of endpoints.
Hosp.
H. Mondor, Créteil, France; NIAID/NIH, Bethesda, MD; San Raffaele Scientific
Inst., Milano, Italy; MUHC, Montreal, Canada; Hosp K. Bicêtre, Kremlin Bicêtre,
France; Hosp St Louis, Paris, France; Univ. of Miami Sch. of Medecine, Miami,
FL; Cytheris, Issy-Les-Moulineaux, France; NIML, Montreal, Canada; Case Western
Reserve Univ., Cleveland, OH.
9/18/09
Reference
Y
Levy, I Sereti, G Tambussi, and others. INSPIRE Study: Effects of r-hIL-7 on T
cell recovery and thymic output in HIV-infected patients receiving c-ART - interim
analysis of a phase I/IIa multicenter study. 49th Interscience Conference on Antimicrobial
Agents and Chemotherapy (ICAAC 2009). San Francisco. September 12-15, 2009. Abstract
H-1230a.
