# Analyzing Real-World Infection Risk in Multiple Myeloma Patients Receiving Teclistamab

**Authors:** Paddy Ssentongo, Emma G. Guare, Chen Song, Yoshitaka Inoue, Manpreet Sandhu, Charyguly Annageldiyev, Jeffrey Sivik, Kevin Rakszawski, Seema Naik, Kentaro Minagawa, Shin Mineishi, Catharine I. Paules

PMC · DOI: 10.3390/curroncol33030154 · 2026-03-08

## TL;DR

This study shows that teclistamab, a treatment for multiple myeloma, is linked to a high risk of severe infections early in therapy, often leading to hospitalization and treatment discontinuation.

## Contribution

The study provides real-world evidence of infection risks with teclistamab, emphasizing the need for improved infection management strategies in clinical practice.

## Key findings

- Over half of patients receiving teclistamab developed at least one infection, often severe and occurring early in treatment.
- Infections led to frequent hospitalizations and were a major reason for permanently stopping teclistamab therapy.
- Most documented infections were Grade ≥ 3, with a median time to first infection of 20 days.

## Abstract

Teclistamab is an immune-based treatment for relapsed or refractory multiple myeloma that can improve disease control but also increases the risk of infection. We reviewed real-world outcomes of patients treated with teclistamab at our institution to better understand the frequency, timing, and severity of infections. More than half of patients developed at least one infection, many of which were severe and occurred early during therapy. Infections frequently led to hospitalization and were a common reason for permanent discontinuation of teclistamab. These findings highlight the substantial infection burden associated with teclistamab in routine clinical practice and underscore the need for improved strategies to prevent, monitor, and manage infections in patients receiving this therapy.

Background: Teclistamab is an anti-B-cell maturation antigen bispecific antibody used in relapsed, refractory multiple myeloma that induces durable responses but is associated with infectious complications. Real-world data characterizing infection risk remain limited. Methods: We conducted a single-center retrospective cohort study of relapsed/re fractory multiple myeloma patients treated with teclistamab from 1 January 2023 to 20 November 2023. The primary objective was to establish the incidence of infections after initiation of teclistamab. Secondary objectives included infection-related outcomes and identifying potential risk factors for infection. Results: 19 patients received teclistamab with a median age of 72 [IQR: 62–74] years and 73.7% had Karnofsky performance score < 80. A total of 11 (57.9%) patients developed 19 infections, with seven patients having multiple infections. There were five bacteremias, five other bacterial infections, seven respiratory viral infections, and 2 CMV reactivation events. Median time to first infection was 20 days (IQR: 9–87) and median grade of all infections was three (range: 1–5). Of the 19 documented infections, 15 (78.9%) were Grade ≥ 3. A total of 10 patients in the infection group and three in the non-infection group discontinued therapy permanently (p = 0.013). Conclusion: In this real-world cohort, infectious complications emerged early and frequently during teclistamab therapy and were a major driver of treatment interruption and permanent discontinuation. The clinical impact of infection extended beyond acute morbidity, often limiting continued access to an otherwise effective therapy in a heavily pretreated population. These findings highlight the need for proactive, individualized infection risk assessment and for standardized, evidence-informed approaches to infection monitoring, prophylaxis, and treatment modification during teclistamab therapy. Larger, multicenter studies will be essential to define strategies that balance infection risk with treatment durability in patients with limited therapeutic alternatives.

## Linked entities

- **Diseases:** multiple myeloma (MONDO:0009693)

## Full-text entities

- **Genes:** CEP70 (centrosomal protein 70) [NCBI Gene 80321] {aka BITE}
- **Diseases:** antibody deficiency (MESH:D007153), hypogammaglobulinemia (MESH:D000361), CMV (MESH:D003586), inflammatory (MESH:D007249), CRS (MESH:D000080424), B-cell malignancies (MESH:D016393), PCP (MESH:D011020), toxicity (MESH:D064420), ANC (MESH:C564275), infectious complications (MESH:D003141), neurotoxicity (MESH:D020258), neutropenia (MESH:D009503), pancytopenia (MESH:D010198), fungal infections (MESH:D009181), ALC (MESH:D009845), meningitis (MESH:D008580), bacteremia (MESH:D016470), cholangitis (MESH:D002761), encephalopathy (MESH:D001927), bacterial infection (MESH:D001424), death (MESH:D003643), Cancer (MESH:D009369), ICANS (MESH:C000722498), osteomyelitis (MESH:D010019), Multiple Myeloma (MESH:D009101), viral infection (MESH:D014777), sinopulmonary infections (MESH:C536718), VZV (MESH:D000073618), opportunistic infections (MESH:D009894), urinary tract infection (MESH:D014552), impairment of humoral immunity (MESH:C562390), injury to (MESH:D014947), septic shock (MESH:D012772), Infection (MESH:D007239), encephalitis (MESH:D004660)
- **Chemicals:** valtrex (MESH:D000077483), Dexamethasone (MESH:D003907), steroid (MESH:D013256), acyclovir (MESH:D000212), Teclistamab (-), tocilizumab (MESH:C502936)
- **Species:** Pneumocystis (genus) [taxon 4753], Homo sapiens (human, species) [taxon 9606]

## Figures

1 figure with captions in the complete paper: https://tomesphere.com/paper/PMC13025476/full.md

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Source: https://tomesphere.com/paper/PMC13025476