Multimodal Therapy with Consolidating Haploidentical Stem Cell Transplantation and Dinutuximab Beta for Patients with High-Risk Neuroblastoma and Central Nervous System Relapse
Abstract
:1. Introduction
2. Materials and Methods
2.1. Study Design and Patients
2.2. Treatment
2.3. Study Assessments
2.4. Statistical Analysis
3. Results
3.1. Patient Characteristics
3.2. Treatment Outcomes
3.3. Safety
3.4. Therapy Recommendations
4. Discussion
Author Contributions
Funding
Institutional Review Board Statement
Informed Consent Statement
Data Availability Statement
Acknowledgments
Conflicts of Interest
References
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Pt | Sex | Age at Diagnosis | INSS Stage | Details of Primary Tumor (And Metastases) | MYCN Status | mIBG Status | Initial Treatment for Primary Tumor |
---|---|---|---|---|---|---|---|
1 | M | 3 yrs 4 m | 4 |
| Amplified | + |
|
2 | M | 3 yrs 4 m | 4 |
| Not amplified | + |
|
3 | M | 2 yrs 3 m | 3 |
| Amplified | + |
|
4 | F | 3 yrs 7 m | 4 |
| Not amplified | + |
|
5 | M | 2 yrs 3 m | 4 |
| Not amplified | + |
|
6 | M | 1 yr 5 m | 4 |
| Amplified | + |
|
7 | M | 7 yrs 2 m | 4 |
| Unknown | + |
|
8 a | M | 5 m | 4S |
| Not amplified | + |
|
9 | M | 3 yrs 9 m | 4 |
| Amplified | + |
|
10 | F | 4 yrs 11 m | 4 |
| Not amplified | + |
|
11 | M | 4 yrs | 4 |
| Not amplified | + |
|
12 | F | 3 yrs 1 m | 4 |
| Not amplified | + |
|
13 | F | 3 yrs 7 m | 4 |
| Amplified | + |
|
Pt | TTFR, m | Details of Relapse | Treatment (Prior to Haplo-SCT and DB) | Status Before Haplo-SCT | Donor | Status after Haplo-SCT | DB Cycles (n) a | Status of Disease after DB Cycle: | Last Known Status | ||
---|---|---|---|---|---|---|---|---|---|---|---|
3 | 5/6 | 9 | |||||||||
1 | 17 | Distant metastases (CNS only) Temporopolar dural metastasis (right cranial fossa) with local hemorrhage |
| PR | Mother | CR | 6 | CR | CR | – |
|
2 | 14 | Distant recurrence (bone/BM, CNS)
Systemic (proximal femur right, trochanter major left, ilium right, right humeral head) |
| MR | Father | PR | 7 | PR | PR | – |
|
3 | 19 | Distant metastases (CNS only) First relapse: isolated cerebellar metastasis left Second relapse: intraspinal metastasis Th5/6 with cross-sectional symptoms and spinal S1; cerebellar metastasis right; blastomatous meningiosis | First relapse:
| PR | Father | PR | 9 | CR | CR | CR |
|
4 | 27 | Distant metastases (CNS only) Intracranial right frontal, left temporal, left frontobasal, involvement of the brain parenchyma, large liquid/hemorrhagic formations, |
| CR | Mother | CR | 7 | CR | CR | – |
|
5 | 25 | Distant recurrence only (bone, CNS)
Bone metastases: right femur, right humerus |
| CR | Mother | CR | 9 | CR | CR | CR |
|
6 | 16 | Distant recurrence only (bone, CNS) Right temporal |
| PR | Mother | CR | 6 | CR | CR | – |
|
7 | 31 | Local and distant recurrences (bone, BM, CNS) First relapse: parameningeal skull base, liver, BM Second relapse: skull base left, left humerus, right femur, right tibia, pelvis Third relapse: left temporopolar, os ilium Fourth relapse: diffuse osteomedullary (filiae scapula right, Th8, distal femur left, proximal tibia right, Th9), skull base with CNS involvement | Relapses 1–3:
| PR | Mother | SD | 9 | PR | PR | CR |
|
8 | 82 | Local and distant recurrences (bone, BM, CNS) First relapse: osseous, pulmonary, orbital metastases, infiltration of the skull base, epidural spread, BM infiltration Second relapse: disseminated; progression of existing lesions, new metastases on the lateral right orbital wall, right mediastinal, abdominal retroperitoneal | First relapse:
| PR | Mother | PR | 6 a | PR | PD | – |
|
9 | 12 | First relapse Distant recurrence only (bone, CNS) Multiple leptomeningeal and intraspinal Second relapse Intracranial, multiple intraspinal | First relapse:
| PR | Mother | CR | 6 | CR | PD | – |
|
10 | Unknown b | Distant recurrence only (other, CNS) Cerebral relapse, paraventricular right mass of the caudate nucleus |
| PR | Mother | CR | 3 | PD | – | – |
|
11 | 14 | Distant recurrence only (bone, BM, CNS)
|
| CR | Father | CR | 5 | CR | CRc | – |
|
12 | 19 | Local and distant recurrences (bone, BM, lymph nodes, CNS)
|
| PR | Mother | PR | 5 | CR | CR c | – |
|
13 | 14 | CNS only: parenchymatous cerebral relapse (frontal) |
| CR | Father | CR | 5 | CR | CR |
|
Adverse Events, n (%) | Grade 1/2 a | Grade 3/4 a |
General condition | 8 (10.5) | 4 (5.3) |
Diarrhea | 9 (11.8) | 2 (2.6) |
Constipation | 12 (15.8) | 0 (0) |
Stomatitis | 9 (11.8) | 0 (0) |
Skin toxicity | 8 (10.5) | 0 (0) |
Allergy | 4 (5.3) | 4 (5.3) |
Nausea/vomitting | 6 (7.9) | 1 (1.3) |
Central neurotoxicity | 2 (2.6) | 3 (3.9) |
Hypotension | 4 (5.3) | 1 (1.3) |
Pulmonary toxicity | 3 (3.9) | 0 (0) |
Veno-occlusive disease | 0 (0) | 0 (0) |
Cardiac function | 0 (0) | 0 (0) |
QT interval | 0 (0) | 0 (0) |
ECHO: LV-SF | 0 (0) | 0 (0) |
Laboratory abnormalities | ||
SGOT/SGPT elevation | 10 (13.2) | 2 (2.6) |
Hemoglobin level reduced | 8 (10.5) | 4 (5.3) |
White blood count reduced | 5 (6.6) | 7 (9.2) |
Absolute neutrophil count reduced | 2 (2.6) | 10 (13.2) |
Platelets reduced | 5 (6.6) | 3 (3.9) |
Proteinuria | 7 (9.2) | 0 (0) |
Bilirubin elevation | 5 (6.6) | 1 (1.3) |
Creatinine elevation | 5 (6.6) | 0 (0) |
Decreased GFR (mL/min/1.73 m2) b | 3 (3.9) | 0 (0) |
Hemolytic anemia | 0 | 1 (1.3) |
Hematuria | 1 (1.3) | 0 (0) |
Surgery | If possible, a resection of the CNS metastasis should be performed initially in order to obtain tissue to evaluate suitability for targeted therapy. Resection after neoadjuvant chemotherapy can be considered in asymptomatic cases in order to reduce the risk of tumor spillage. In our experience, improvement without resection is also possible in case of surgically unfavorably located metastases. |
Systemic therapy | CNS-directed chemotherapy should be administered. We had a good experience with irinotecan and temozolomide. Concomitant therapy with dinutuximab beta can be considered, especially in patients with combined relapses. However, the risk for serious neurotoxicity is increased at the start of dinutuximab beta treatment and after surgery in patients with CNS metastases. |
Targeted therapy | Targeted therapy, such as ALK inhibitors, should be given if indicated. We recommend interrupting therapy during haplo-SCT until stable engraftment is achieved. There are currently no data on concomitant ALK inhibitor therapy and radiotherapy in patients with neuroblastoma. Based on reports of adult patients with lung cancer, concomitant use can be considered [25]. |
Compartmental chemotherapy | Intrathecal chemotherapy, such as etoposide or topotecan, can be considered, especially in patients with leptomeningeal involvement or cancerous meningiosis, or if radiotherapy is not possible. |
Radiotherapy | Current recommendations favor craniospinal irradiation with a local boost over the whole brain or local irradiation for neuroblastoma with CNS relapse. In the case of craniospinal irradiation with a local boost, we recommend proton therapy. In case of isolated CNS relapses, early radiotherapy should be administered. If tolerable, concomitant therapy with temozolomide can be considered, especially for patients with combined relapses. |
Haploidentical stem cell transplantation | Haplo-SCT should follow previously reported guidance, with myeloablative conditioning with fludarabine, thiotepa, melphalan, and ATG. Transplantation should only be performed if remission status ≥PR is achieved. T- and B-cell-depleted grafts should be used. |
Post-transplant-immunotherapy | Dinutuximab beta should be initiated 40–180 days post-transplant if the patient has no signs of GvHD and does not require immunosuppressant medication. According to the Summary of Product Characteristics, five cycles of dinutuximab beta should be given. We do not recommend concomitant therapy with cytokines, like IL-2. |
Maintenance therapy | Maintenance therapy with targeted therapy, like ALK inhibitors, can be considered. |
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Flaadt, T.; Ebinger, M.; Schreiber, M.; Ladenstein, R.L.; Simon, T.; Lode, H.N.; Hero, B.; Schuhmann, M.U.; Schäfer, J.; Paulsen, F.; et al. Multimodal Therapy with Consolidating Haploidentical Stem Cell Transplantation and Dinutuximab Beta for Patients with High-Risk Neuroblastoma and Central Nervous System Relapse. J. Clin. Med. 2023, 12, 6196. https://doi.org/10.3390/jcm12196196
Flaadt T, Ebinger M, Schreiber M, Ladenstein RL, Simon T, Lode HN, Hero B, Schuhmann MU, Schäfer J, Paulsen F, et al. Multimodal Therapy with Consolidating Haploidentical Stem Cell Transplantation and Dinutuximab Beta for Patients with High-Risk Neuroblastoma and Central Nervous System Relapse. Journal of Clinical Medicine. 2023; 12(19):6196. https://doi.org/10.3390/jcm12196196
Chicago/Turabian StyleFlaadt, Tim, Martin Ebinger, Malin Schreiber, Ruth L. Ladenstein, Thorsten Simon, Holger N. Lode, Barbara Hero, Martin U. Schuhmann, Jürgen Schäfer, Frank Paulsen, and et al. 2023. "Multimodal Therapy with Consolidating Haploidentical Stem Cell Transplantation and Dinutuximab Beta for Patients with High-Risk Neuroblastoma and Central Nervous System Relapse" Journal of Clinical Medicine 12, no. 19: 6196. https://doi.org/10.3390/jcm12196196
APA StyleFlaadt, T., Ebinger, M., Schreiber, M., Ladenstein, R. L., Simon, T., Lode, H. N., Hero, B., Schuhmann, M. U., Schäfer, J., Paulsen, F., Timmermann, B., Eggert, A., & Lang, P. (2023). Multimodal Therapy with Consolidating Haploidentical Stem Cell Transplantation and Dinutuximab Beta for Patients with High-Risk Neuroblastoma and Central Nervous System Relapse. Journal of Clinical Medicine, 12(19), 6196. https://doi.org/10.3390/jcm12196196