Published May 15, 2023 | Version v1
Publication Open

Metastatic clear-cell renal cell carcinoma: a frequent NOTCH1 mutation predictive of response to anti-NOTCH1 CB-103 treatment

Creators

  • 1. National Hospital of Pediatrics
  • 2. Sorbonne Paris Cité
  • 3. Université Paris Cité
  • 4. Inserm
  • 5. Hôpital Necker-Enfants Malades
  • 6. Assistance Publique – Hôpitaux de Paris
  • 7. Sorbonne Université
  • 8. Université Sorbonne Paris Nord
  • 9. Université Paris-Seine
  • 10. Hanoi Medical University
  • 11. Université de franche-comté

Description

Abstract Background Clear-cell renal cell carcinomas (ccRCCs) are malignant tumors with high metastatic potential and resistance to treatments occurs almost constantly. Compared to primary tumors, there are still limited genomic data that has been obtained from metastatic samples. Methods We aimed to characterize metastatic ccRCC by way of whole-genome analyses of metastatic formalin-fixed samples, using OncoScan ® technology. We identified a frequent, unexpected pL1575P NOTCH1 mutation which we set out to characterize for translational purposes. We thus implemented patient-derived xenografts from metastatic samples of human ccRCC to explore its clinical significance. Results We showed that pL1575P NOTCH1 mutation was an activating mutation, leading to the expression of NOTCH1-intracellular domain-active fragments in both cancer cells and tumor endothelial cells, suggesting a trans-differentiation of cancer cells into tumor micro-vessels. We demonstrated that this mutation could be used as a predictive biomarker of response to CB-103, a specific NOTCH1-intracellular domain inhibitor. One striking result was the considerable anti-angiogenic effect, coherent with the presence of NOTCH1 mutation in tumor micro-vessels. Conclusions We identified a frequent, unexpected pL1575P_c4724T_C NOTCH1 mutation as a new biomarker for ccRCC metastases, predictive of response to the CB103 NOTCH1-intracellular domain inhibitor.

⚠️ This is an automatic machine translation with an accuracy of 90-95%

Translated Description (Arabic)

ملخص الخلفية سرطانات الخلايا الكلوية الشفافة (ccRCCs) هي أورام خبيثة ذات إمكانات نقيلية عالية ومقاومة للعلاجات تحدث باستمرار تقريبًا. مقارنة بالأورام الأولية، لا تزال هناك بيانات جينية محدودة تم الحصول عليها من العينات النقيلية. الأساليب كنا نهدف إلى توصيف ccRCC النقيلي عن طريق تحليلات الجينوم الكامل للعينات الثابتة بالفورمالين النقيلي، باستخدام تقنية OncoScan ®. حددنا طفرة pL1575P NOTCH1 متكررة وغير متوقعة والتي شرعنا في توصيفها لأغراض الترجمة. وبالتالي قمنا بتنفيذ طعوم خارجية مشتقة من المريض من عينات منتشرة من ccRCC البشرية لاستكشاف أهميتها السريرية. النتائج أظهرنا أن طفرة pL1575P NOTCH1 كانت طفرة نشطة، مما أدى إلى التعبير عن شظايا NOTCH1 النشطة في المجال داخل الخلايا في كل من الخلايا السرطانية والخلايا البطانية للورم، مما يشير إلى تمايز الخلايا السرطانية إلى الأوعية الدقيقة للورم. أظهرنا أن هذه الطفرة يمكن استخدامها كعلامة حيوية تنبؤية للاستجابة لـ CB -103، وهو مثبط محدد لنطاق NOTCH1 داخل الخلايا. كانت إحدى النتائج اللافتة للنظر هي التأثير الكبير المضاد لتولد الأوعية الدموية، بما يتفق مع وجود طفرة NOTCH1 في الأوعية الدقيقة للورم. الاستنتاجات حددنا طفرة pL1575P_c4724T_C NOTCH1 متكررة وغير متوقعة كمؤشر حيوي جديد لنقائل ccRCC، للتنبؤ بالاستجابة لمثبط المجال داخل الخلايا CB103 NOTCH1.

Translated Description (English)

Abstract Background Clear-cell renal cell carcinomas (ccRCCs) are malignant tumors with high metastatic potential and resistance to treatments occurs almost constantly. Compared to primary tumors, there are still limited genomic data that has been obtained from metastatic samples. Methods We aimed to characterize metastatic ccRCC by way of whole-genome analyses of metastatic formalin-fixed samples, using OncoScan ® technology. We identified a frequent, unexpected pL1575P NOTCH1 mutation which we set out to characterize for translational purposes. We thus implemented patient-derived xenografts from metastatic samples of human ccRCC to explore its clinical significance. Results We showed that pL1575P NOTCH1 mutation was an activating mutation, leading to the expression of NOTCH1-intracellular domain-active fragments in both cancer cells and tumor endothelial cells, suggesting a trans-differentiation of cancer cells into tumor micro-vessels. We demonstrated that this mutation could be used as a predictive biomarker of response to CB-103, a specific NOTCH1-intracellular domain inhibitor. One striking result was the considerable anti-angiogenic effect, consistent with the presence of NOTCH1 mutation in tumor microvessels. Conclusions We identified a frequent, unexpected pL1575P_c4724T_C NOTCH1 mutation as a new biomarker for ccRCC metastases, predictive of response to the CB103 NOTCH1-intracellular domain inhibitor.

Translated Description (French)

Abstract Background Clear-cell rénale cell carcinomes (ccRCCs) are malignant tumors with high métastatic potential and resistance to treatments occurs almost constantly. Compared to primary tumors, there are still limited genomic data that has been obtained from meastatic samples. Methods We aimed to characterize metastatic ccRCC by way of whole-genome analyses of metastatic formalin-fixed samples, using OncoScan ® technology. We identified a frequent, unexpected pL1575P NOTCH1 mutation which we set out to characterize for translational purposes. We thus implemented patient-derived xenografts from metastatic samples of human ccRCC to explore its clinical significance. Résultats We showed that pL1575P NOTCH1 mutation was an activating mutation, leading to the expression of NOTCH1-intracellular domain-active fragments in both cancer cells and tumor endothelial cells, suggesting a trans-differentiation of cancer cells into tumor micro-vessels. We demonstrated that this mutation could be used as a predictive biomarker of response to CB-103, a specific NOTCH1-intracellular domain inhibitor. One striking result was the considérable anti-angiogenic effect, cohesent with the presence of NOTCH1 mutation in tumor micro-vessels. Conclusions We identified a frequent, unexpected pL1575P_c4724T_C NOTCH1 mutation as a new biomarker for ccRCC metatases, predictive of response to the CB103 NOTCH1-intracellular domain inhibitor.

Translated Description (Spanish)

Resumen Antecedentes Clear-cell renal cell carcinomas (ccRCCs) are malignant tumors with high metastatic potential and resistance to treatments occurs almost constantly. Compared to primary tumors, there are still limited genomic data that has been obtained from metastatic samples. Methods We aimed to characterize metastatic ccRCC by way of whole-genome analyses of metastatic formalin-fixed samples, using OncoScan ® technology. We identified a frequent, unexpected pL1575P NOTCH1 mutation which we set out to characterize for translational purposes. We thus implementad patient-derived xenografts from metastatic samples of human ccRCC to explore its clinical significance. Results We showed that pL1575P NOTCH1 mutation was an activating mutation, leading to the expression of NOTCH1-intracellular domain-active fragments in both cancer cells and tumor endothelial cells, suggesting a trans-differentiation of cancer cells into tumor micro-vessels. We demonstrated that this mutation could be used as a predictive biomarker of response to CB-103, a specific NOTCH1-intracellular domain inhibitor. One striking result was the considerable anti-angiogenic effect, coherent with the presence of NOTCH1 mutation in tumor micro-vessels. Conclusions We identified a frequent, unexpected pL1575P_c4724T_C NOTCH1 mutation as a new biomarker for ccRCC metastases, predictive of response to the CB103 NOTCH1-intracellular domain inhibitor.

Files

s40164-023-00408-z.pdf

Files (1.4 MB)

⚠️ Please wait a few minutes before your translated files are ready ⚠️ Note: Some files might be protected thus translations might not work.
Name Size Download all
md5:6657dbef3aa13bb251f58d7c122e7c76
1.4 MB
Preview Download

Additional details

Additional titles

Translated title (Arabic)
سرطان الخلايا الكلوية النقيلي النقيلي: طفرة NOTCH1 متكررة تنبئ بالاستجابة للعلاج المضاد لـ NOTCH1 CB -103
Translated title (English)
Metastatic clear-cell renal cell carcinoma: a frequent NOTCH1 mutation predictive of response to anti-NOTCH1 CB-103 treatment
Translated title (French)
Metastatic clear-cell rénale cell carcinome : a frequent NOTCH1 mutation predictive of response to anti-NOTCH1 CB-103 treatment
Translated title (Spanish)
Metastatic clear-cell renal cell carcinoma: a frequent NOTCH1 mutation predictive of response to anti-NOTCH1 CB-103 treatment

Identifiers

Other
https://openalex.org/W4376641787
DOI
10.1186/s40164-023-00408-z

Is supplement to
https://openalex.org/W4302307493 (Other)
https://openalex.org/W2533581028 (Other)
https://openalex.org/W2405318000 (Other)
https://openalex.org/W2394514550 (Other)
https://openalex.org/W2103599065 (Other)
https://openalex.org/W2097812111 (Other)
https://openalex.org/W2078925029 (Other)
https://openalex.org/W2051583827 (Other)
https://openalex.org/W2045819279 (Other)
https://openalex.org/W2008548563 (Other)

GreSIS Basics Section

Is Global South Knowledge
Yes
Country
Vietnam

References

  • https://openalex.org/W1968657935
  • https://openalex.org/W2033372592
  • https://openalex.org/W2064800483
  • https://openalex.org/W2147810480
  • https://openalex.org/W2408504246
  • https://openalex.org/W2557303080
  • https://openalex.org/W2595956919
  • https://openalex.org/W2797282777
  • https://openalex.org/W2913745075
  • https://openalex.org/W3038448785
  • https://openalex.org/W3089976119
  • https://openalex.org/W4205308968
  • https://openalex.org/W4220889808