Peptide Receptor Radionuclide Therapy in Patients with Inoperable Meningiomas: Our Experience and Review of the Literature

MinutoliFabio,; Amato, Ernesto; Sindoni, Alessandro; CardileDavide,; Conti, Alfredo; HerbergAstrid,; BaldariSergio,

doi:10.1089/cbr.2013.1599

Cited by 28 publications

(20 citation statements)

References 57 publications

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“…Our study as well as other recent work (3,4) suggests that somatostatin receptor-targeted radiopeptides represent a promising therapeutic option for patients with progressive meningiomas. Herein lies an opportunity for the field of nuclear medicine, in collaboration with neurooncology, radiation oncology, and neurosurgery, to translate this tool from a promising option into a validated therapy.…”

Section: Replysupporting

confidence: 74%

Reply: Somatostatin Receptor–Targeted Radiopeptide Therapy in Patients with Progressive Unresectable Meningioma

Radojewski¹,

Dumont²,

Marincek³

et al. 2016

J Nucl Med

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Section: Replysupporting

confidence: 74%

Reply: Somatostatin Receptor–Targeted Radiopeptide Therapy in Patients with Progressive Unresectable Meningioma

Radojewski¹,

Dumont²,

Marincek³

et al. 2016

J Nucl Med

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“…Moreover, the results of a phase II prospective clinical trial, in which 67.6% of patients achieved SD and the mean survival of all enrolled patients was 8.6 years, lent further support to the use of SSTR2-directed PRRT in patients with progressive unresectable meningioma (102). Many more clinical studies have confirmed the efficacy and safety of SSTR2-targeted PRRT in the treatment of meningiomas (103)(104)(105). Indeed, the recent European Association of Neuro-Oncology guidelines on meningioma have declared PRRT a promising approach to treat refractory meningiomas across all WHO grades in the future (1).…”

Section: Ptsmentioning

confidence: 84%

Clinical Significance of Somatostatin Receptor (SSTR) 2 in Meningioma

Zhou

Wang

et al. 2020

Front. Oncol.

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Somatostatin receptor (SSTR) 2, widely expressed in meningioma, is a G-proteincoupled receptor and can be activated by somatostatin or its synthetic analogs. SSTR2 is therefore extensively studied as a marker and target for the diagnosis and treatment of meningioma. Accumulating studies have revealed the crucial clinical significance of SSTR2 in meningioma. Summarizing the progress of these studies is urgently needed as it may not only provide novel and better management for patients with meningioma but also indicate the direction of future research. Pertinent literature is reviewed to summarize the recent collective knowledge and understanding of SSTR2's clinical significance in meningioma in this review. SSTR2 offers novel ideas and approaches in the diagnosis, treatment, and prognostic prediction for meningioma, but more and further studies are required.

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“…However, patients with impaired renal function have to be evaluated thoroughly before considering therapy with radiolabeled somatostatin analogs. Alternatively, according to the results of Minutoli et al (22), 111 In-labeled somatostatin analogs might be used instead of b-emitting radionuclides in cases with a higher risk of renal toxicity.…”

Section: Discussionmentioning

confidence: 99%

⁹⁰Y-DOTATOC as a Therapeutic Option for Complex Recurrent or Progressive Meningiomas

et al. 2015

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The standard treatment of meningiomas is surgery or radiotherapy. Complex, especially recurrent or progressive cases, may exhibit tumor growth involving critical neurovascular structures or diffuse growth, resulting in limited efficacy and higher risk of standard treatment. We evaluated whether somatostatin receptor-targeted radionuclide therapy with 90 Y-DOTATOC may be a therapeutic option. Methods: Fifteen patients with recurrent or progressive meningiomas after multimodal pretreatment or unfavorable medical risk profile were treated with systemic 90 Y-DOTATOC. Endpoints were progression-free survival and toxicity. Results: Usually applied doses were 7,400 MBq/m 2 of 90 Y-DOTATOC in 2 fractions. Mean observation time was 49.7 mo (range, 12-137 mo). Overall median progression-free survival was at least 24 mo. Toxicity was moderate, mostly hematologic (n 5 8) and transient. Conclusion: 90 Y-DOTATOC therapy is feasible and may represent a promising second-or third-line option for complex meningiomas, which are progressive or otherwise not treatable with a reasonable risk-benefit ratio.

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Peptide Receptor Radionuclide Therapy in Patients with Inoperable Meningiomas: Our Experience and Review of the Literature

Abstract: In consideration of its efficacy and the lack of significant toxicity, PRRT of meningiomas using (111)In-Pentetreotide could be proposed even nowadays when the use of (177)Lu- or (90)Y-labeled peptides seems unsafe, namely in patients with renal impairment/toxicity.

Cited by 28 publications

References 57 publications

Reply: Somatostatin Receptor–Targeted Radiopeptide Therapy in Patients with Progressive Unresectable Meningioma

Reply: Somatostatin Receptor–Targeted Radiopeptide Therapy in Patients with Progressive Unresectable Meningioma

Clinical Significance of Somatostatin Receptor (SSTR) 2 in Meningioma

⁹⁰Y-DOTATOC as a Therapeutic Option for Complex Recurrent or Progressive Meningiomas

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Peptide Receptor Radionuclide Therapy in Patients with Inoperable Meningiomas: Our Experience and Review of the Literature

Abstract: In consideration of its efficacy and the lack of significant toxicity, PRRT of meningiomas using (111)In-Pentetreotide could be proposed even nowadays when the use of (177)Lu- or (90)Y-labeled peptides seems unsafe, namely in patients with renal impairment/toxicity.

Cited by 28 publications

References 57 publications

Reply: Somatostatin Receptor–Targeted Radiopeptide Therapy in Patients with Progressive Unresectable Meningioma

Reply: Somatostatin Receptor–Targeted Radiopeptide Therapy in Patients with Progressive Unresectable Meningioma

Clinical Significance of Somatostatin Receptor (SSTR) 2 in Meningioma

90Y-DOTATOC as a Therapeutic Option for Complex Recurrent or Progressive Meningiomas

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Product

Resources

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⁹⁰Y-DOTATOC as a Therapeutic Option for Complex Recurrent or Progressive Meningiomas