Skip to main content
. Author manuscript; available in PMC: 2014 Dec 9.
Published in final edited form as: Future Oncol. 2012 Oct;8(10):1273–1299. doi: 10.2217/fon.12.125

Table 1.

Recent clinical trials using different sources of dendritic cells and varying maturation strategies.

Maturation regimen DC phenotype Description: cancer type, stage, sample size and antigen used Important findings Ref.
Immature DCs
GM-CSF and IL-4 Immature

  • Normal, healthy volunteers being vaccinated against influenza

  • n = 2

  • DCs pulsed with influenza antigens and KLH

  • Antigen-specific immune suppression

  • Inhibition of pre-existing antigen-specific T-cell function

 [87]
GM-CSF and IL-4 Immature

  • Recurrence of a variety of pediatric tumors including neuroblastoma, Ewing’s sarcoma, other sarcomas and renal malignancies

  • n = 15

  • DCs pulsed with tumor lysate and KLH

  • Antigen-specific T-cell sensitization

  • Inconclusive, although overall favorable clinical results

  • Significant regression of multiple metastatic sites was seen in one patient

 [271]
Mature versus immature DCs
GM-CSF and IL-4 IL-1β, TNF-α, IL-6, PGE2 Immature Mature

  • Stage IV cutaneous melanoma and progressive disease

  • n = 11

  • DCs pulsed with HLA-specific melanoma class I peptide

  • Mature DCs demonstrated increased CD4+ T-cell recall

  • Mature DCs induced increased antigen-specific CTLs

  • No definitive clinical conclusions

 [272]
pDCs
No human clinical trials
MoDCs
IL-1β, TNF-α, IL-6, PGE2 Mature

  • Metastatic melanoma

  • n = 28

  • DCs pulsed with MHC class I and class II peptides

  • Immune-specific T-cell sensitization

  • Th1-polarized immune response detectable in all patients

  • Mixed, although encouraging clinical results with one patient experiencing full tumor regression

 [273]
IL-1β, TNF-α, IL-6, PGE2 Mature

  • Surgically resected pancreatic or biliary tree (gallbladder, ampullary or bile duct) cancer

  • n = 12

  • DCs pulsed with MLJC1 peptide

  • No direct measure of antigen-specific T-cell sensitization

  • No measurable antibody response

  • Overall increase of Foxp3 expressing regulatory CD4+ cells

  • Mixed clinical outcomes, some evidence of improved survival

 [274]
IL-1β, TNF-α, IL-6, PGE2 Mature

  • Metastatic renal-cell carcinoma

  • n = 14

  • DCs pulsed with autologous tumor lysate and KLH or DCs pulsed with peptide antigen

  • Immune-specific T-cell sensitization

  • No objective clinical response

 [275]
TNF-α,IL-6, IL-1β, PGE2 Mature

  • Stage I multiple myeloma patients

  • n = 9

  • DCs were pulsed with autologous Id protein tumor antigen

  • Antigen-specific T-cell sensitization

  • Unable to clearly assess clinical response

 [276]
TNF-α, IL-1β, PGE2 Mature

  • Patients with newly diagnosed GBM

  • n = 8

  • DCs pulsed with autologous tumor lysate and combination radiation and chemotherapy

  • Mixed immunogenicity, overall increased antigen-specific response

  • Inconclusive clinical outcomes

 [277]
TNF-α, IL-6, IL-1β, PGE2 Mature

  • Patients with progressive malignant melanoma without brain metastases

  • n = 28

  • DCs pulsed with peptides and/or autologous and allogeneic tumor lysates depending on HLA-A2 status administered in conjunction with IL-2 and metronomic cyclophosphamide

  • Antigen-specific T-cell sensitization

  • No decrease in Treg cells

  • No objective clinical response, but evidence of improved disease stabilization

 [278]
IFN-α, TNF-α, polyinosinic:polycytidylic acid DC1

  • Metastatic patients with a variety cancers

  • n = 24

  • DCs pulsed with autologous tumor lysates combined with cyclophosphamide, Peg-IFN and GM-CSF

  • Four of 11 patients demonstrated antigen-specific T-cell activation

  • Circulating tumor cells decreased in six of 19 patients

  • 21% disease stabilization but overall equivocal clinical outcomes

 [279]
IL-1, TNF, IFN and poly-l:C DC1

  • Glioblastoma patients

  • n = 22

  • DC pulsed with previously identified HLA-A2-restricted peptide epitopes

  • Induced increased systemic production of Th1 cytokines

  • Mixed results for antigen-specific sensitization

  • 9% clinical response

 [280]
LPS and IFN-γ DC1

  • Her2-positive DCIS patients

  • n = 27

  • DCs pulsed with HLA-A2-restricted peptide epitopes

  • Antigen-specific T-cell sensitization

  • Reduced or eliminated Her2 expression

  • 90% clinical response

 [157,213]
MoDCs and LCs
CD40L or inflammatory cytokines: IL-1 b, IL-6, TNF-α, andPGE2 DC1

  • Stage III/IV melanoma patients

  • n = 36

  • Compared LC pulsed with melanoma antigen with MoDCs pulsed with melanoma peptide antigen

    (tyrosinase, gp100)

  • LCs demonstrated increased antigen-specific sensitization and were less dependent on exogenous IL-15

  • No significant difference in overall efficacy

 [79]
CD34+ hematopoietic-derived DCs (includes LCs and interstitial DCs)
GM-CSF, FLT3-L, TNF Not specified

  • Metastatic melanoma

  • n = 18

  • DC pulsed with epitopes to melanoma peptide antigens (tyrosinase, gp 100 and Mart-1)

  • Antigen-specific T-cell sensitization

  • Overall enhanced immune response

  • Unable to determine clinical benefit

 [281]
Interstitial DCs
No human clinical trials

These trials demonstrate a bias towards use of monocyte-derived DCs, matured with inflammatory cytokines in an attempt to elicit a DC1-driven immune response.

CTL: Cytotoxic T lymphocyte; DC: Dendritic cell; DCIS: Ductal carcinoma in situ; GBM: Glioblastoma multiforme; GM-CSF: Granulocyte-macrophage colony stimulating factor; KLH: Keyhole limpet hemocyanine;

LC: Langerhans cell; LPS: Lipopolysaccharide; MoDC: Monocyte-derived dendritic cell; pDC: Plasmacytoid DC; Peg-IFN: Pegylated interferon.