Clinical and immunological responses after CD30-specific chimeric antigen receptor–redirected lymphocytes

Carlos A. Ramos; Brandon Ballard; Huimin Zhang; Olga Dakhova; Adrian P. Gee; Zhuyong Mei; Mrinalini Bilgi; Meng-Fen Wu; Hao Liu; Bambi Grilley; Catherine M. Bollard; Bill H. Chang; Cliona M. Rooney; Malcolm K. Brenner; Helen E. Heslop; Gianpietro Dotti; Barbara Savoldo

doi:10.1172/jci94306

Clinical and immunological responses after CD30-specific chimeric antigen receptor–redirected lymphocytes

Carlos A. Ramos(Houston Methodist), Brandon Ballard(Houston Methodist), Huimin Zhang(Houston Methodist), Olga Dakhova(Houston Methodist), Adrian P. Gee(Houston Methodist), Zhuyong Mei(Houston Methodist), Mrinalini Bilgi(Houston Methodist), Meng-Fen Wu(Dan L Duncan Comprehensive Cancer Center), Hao Liu(Dan L Duncan Comprehensive Cancer Center), Bambi Grilley(Houston Methodist), Catherine M. Bollard(Houston Methodist), Bill H. Chang(Oregon Health & Science University), Cliona M. Rooney(Houston Methodist), Malcolm K. Brenner(Houston Methodist), Helen E. Heslop(Houston Methodist), Gianpietro Dotti(Houston Methodist), Barbara Savoldo(Houston Methodist)

Journal of Clinical Investigation

August 13, 2017

10.1172/jci94306

Cited by 368Open Access

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Abstract

BACKGROUND: Targeting CD30 with monoclonal antibodies in Hodgkin lymphoma (HL) and anaplastic large cell lymphoma (ALCL) has had profound clinical success. However, adverse events, mainly mediated by the toxin component of the conjugated antibodies, cause treatment discontinuation in many patients. Targeting CD30 with T cells expressing a CD30-specific chimeric antigen receptor (CAR) may reduce the side effects and augment antitumor activity. METHODS: We conducted a phase I dose escalation study in which 9 patients with relapsed/refractory HL or ALCL were infused with autologous T cells that were gene-modified with a retroviral vector to express the CD30-specific CAR (CD30.CAR-Ts) encoding the CD28 costimulatory endodomain. Three dose levels, from 0.2 × 108 to 2 × 108 CD30.CAR-Ts/m2, were infused without a conditioning regimen. All other therapy for malignancy was discontinued at least 4 weeks before CD30.CAR-T infusion. Seven patients had previously experienced disease progression while being treated with brentuximab. RESULTS: No toxicities attributable to CD30.CAR-Ts were observed. Of 7 patients with relapsed HL, 1 entered complete response (CR) lasting more than 2.5 years after the second infusion of CD30.CAR-Ts, 1 remained in continued CR for almost 2 years, and 3 had transient stable disease. Of 2 patients with ALCL, 1 had a CR that persisted 9 months after the fourth infusion of CD30.CAR-Ts. CD30.CAR-T expansion in peripheral blood peaked 1 week after infusion, and CD30.CAR-Ts remained detectable for over 6 weeks. Although CD30 may also be expressed by normal activated T cells, no patients developed impaired virus-specific immunity. CONCLUSION: CD30.CAR-Ts are safe and can lead to clinical responses in patients with HL and ALCL, indicating that further assessment of this therapy is warranted. TRIAL REGISTRATION: ClinicalTrials.gov NCT01316146. FUNDING: National Cancer Institute (3P50CA126752, R01CA131027 and P30CA125123), National Heart, Lung, and Blood Institute (R01HL114564), and Leukemia and Lymphoma Society (LLSTR 6227-08).

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