Overcoming resistance to BRAFV600E inhibition in melanoma by deciphering and targeting personalized protein network alterations

Vasudevan, Swetha; Flashner-Abramson, Efrat; Alkhatib, Heba; Chowdhury, Sangita Roy; Adejumobi, Ibukun Adesoji; Vilenski, D; Stefansky, Shira; Rubinstein, Ariel M.; Kravchenko‐Balasha, Nataly

doi:10.1038/s41698-021-00190-3

Cited by 15 publications

(42 citation statements)

References 46 publications

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“…The TCGA dataset comprising of 747 breast tumors was a part of a large dataset consisting of 3467 human tumors, which were profiled on a reverse-phase protein array (RPPA) for 181 cancer associated proteins, and analyzed using surprisal analysis as described in [ 18 , 19 , 22 ]. The input data was obtained from TCPA (The Cancer Proteome Atlas) portal.…”

Section: Methodsmentioning

confidence: 99%

“…It is important to note that each protein can participate in many unbalanced processes. In this study, we analyze changes in the proteomic processes as described previously [ 18 , 19 , 22 ].…”

Section: Methodsmentioning

confidence: 99%

“…Not all tumors are influenced by all unbalanced processes. So for each tumor, a set of unbalanced processes is generated, which is converted into a patient-specific barcode as described in [ 18 , 19 , 22 ]. Briefly, for each patient, λ α (k) ( α = 1, 2, 3, …, n ) values are normalized as follows: If λ α (k) > 2 (and is therefore significant according to calculation of threshold values [ 22 ]) then it was normalized to 1; if λ α (k) < −2 (significant according to threshold values as well) then it was normalized to −1; and if −2 < λ α (k) < 2 then it was normalized to 0.…”

Section: Methodsmentioning

confidence: 99%

“…Each patient is assigned then a barcode using −1, 1 and 0 values—which represents a patient-specific combination of the active processes ( Table S1 ). This combination is a patient-specific signaling signature that can be used further to devise patient-specific drug therapies [ 18 , 19 ] as shown in Figure 2. For more details see Figure S1 describing the flow of the analysis and references [ 18 , 19 ].…”

Section: Methodsmentioning

confidence: 99%

“…We suggest that a key for promising therapies lies in an accurate resolution of the PaSSS in each TNBC. All patient-specific processes should be inhibited, through targeting one or two central protein hubs in each process, in order to reduce the tumor-specific biochemical flux [ 19 ]. PaSSS analysis suggested that only a small part of TNBC tumors (~30%) would benefit from anti-EGFR therapies and only when they are combined with anti-ER therapies.…”

Section: Introductionmentioning

confidence: 99%

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Drug-Induced Resistance and Phenotypic Switch in Triple-Negative Breast Cancer Can Be Controlled via Resolution and Targeting of Individualized Signaling Signatures

Vasudevan

Adejumobi

Alkhatib

et al. 2021

Cancers

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Triple-negative breast cancer (TNBC) is an aggressive subgroup of breast cancers which is treated mainly with chemotherapy and radiotherapy. Epidermal growth factor receptor (EGFR) was considered to be frequently expressed in TNBC, and therefore was suggested as a therapeutic target. However, clinical trials of EGFR inhibitors have failed. In this study, we examine the relationship between the patient-specific TNBC network structures and possible mechanisms of resistance to anti-EGFR therapy. Using an information-theoretical analysis of 747 breast tumors from the TCGA dataset, we resolved individualized protein network structures, namely patient-specific signaling signatures (PaSSS) for each tumor. Each PaSSS was characterized by a set of 1–4 altered protein–protein subnetworks. Thirty-one percent of TNBC PaSSSs were found to harbor EGFR as a part of the network and were predicted to benefit from anti-EGFR therapy as long as it is combined with anti-estrogen receptor (ER) therapy. Using a series of single-cell experiments, followed by in vivo support, we show that drug combinations which are not tailored accurately to each PaSSS may generate evolutionary pressure in malignancies leading to an expansion of the previously undetected or untargeted subpopulations, such as ER+ populations. This corresponds to the PaSSS-based predictions suggesting to incorporate anti-ER drugs in certain anti-TNBC treatments. These findings highlight the need to tailor anti-TNBC targeted therapy to each PaSSS to prevent diverse evolutions of TNBC tumors and drug resistance development.

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Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Drug-Induced Resistance and Phenotypic Switch in Triple-Negative Breast Cancer Can Be Controlled via Resolution and Targeting of Individualized Signaling Signatures

Vasudevan

Adejumobi

Alkhatib

et al. 2021

Cancers

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In vitro cancer models as an approach to identify targetable developmental phenotypes in cancer stem cells

Biddle

2023

In vitro models

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Cancer therapeutics are often highly toxic to the patient, and they often elicit rapid resistance in the tumour. Recent advances have suggested a potential new way in which we may improve on this, through two important concepts: (1) that multitudinous pathway alterations converge on a limited number of cancer cellular phenotypes, and (2) that these cancer cellular phenotypes depend on reactivation of developmental processes that are only minimally active in adult tissues. This provides a rationale for pursuing an approach of ‘drugging the phenotype’ focussed on targeting reactivated cellular processes from embryonic development. In this concepts paper, we cover these recent developments and their implications for the development of new cancer therapeutics that can avoid patient toxicity and acquired resistance. We then propose that in vitro tumour and developmental models can provide an experimental approach to identify and target the specific developmental processes at play, with a focus on the reactivation of developmental processes in the cancer stem cells that drive tumour progression and spread. Ultimately, the aim is to identify cellular processes that are specific to developmental phenotypes, are reactivated in cancer stem cells, and are essential to tumour progression. Therapeutically targeting these cellular processes could represent a new approach of ‘drugging the phenotype’ that treats the tumour whilst avoiding patient toxicity or the acquisition of therapeutic resistance.

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Targeting EGFR in melanoma – The sea of possibilities to overcome drug resistance

Pastwińska

Karaś

Karwaciak

et al. 2022

Biochimica et Biophysica Acta (BBA) - Reviews on Cancer

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Overcoming resistance to BRAFV600E inhibition in melanoma by deciphering and targeting personalized protein network alterations

Cited by 15 publications

References 46 publications

Drug-Induced Resistance and Phenotypic Switch in Triple-Negative Breast Cancer Can Be Controlled via Resolution and Targeting of Individualized Signaling Signatures

Drug-Induced Resistance and Phenotypic Switch in Triple-Negative Breast Cancer Can Be Controlled via Resolution and Targeting of Individualized Signaling Signatures

In vitro cancer models as an approach to identify targetable developmental phenotypes in cancer stem cells

Targeting EGFR in melanoma – The sea of possibilities to overcome drug resistance

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