| Literature DB >> 31275380 |
Shahla Bari1, Jameel Muzaffar2, Austin Chan3, Sanjay R Jain3, Ahmad M Haider4, Marjorie Adams Curry5, Christopher J Hostler6.
Abstract
Due to HAART and consequent decline in mortality from infectious complications, HIV patients have an increasing burden of non-AIDS defining cancers. Data on their safety and efficacy is unknown as these patients were excluded from clinical trials due to concern of unforeseen side effects. Objectives. The main objective of our study was to evaluate the efficacy and safety profile of PD-1 and PD-L1 inhibitors in HIV patients being treated for advanced cancers and to assess the impact of these drugs on HIV status of the patients specifically CD4 count and HIV viral load. Materials and Methods. This was a retrospective analysis of data of 17 patients HIV treated with one of the PD-1/PD-L1 inhibitors (Nivolumab, Pembrolizumab, Atezolizumab, Durvalumab, or Avelumab) for advanced cancer. Results. 10 out of 17 patients responded to therapy. 7 patients, all of whom had shown response to therapy, were alive and 4 were still on checkpoint inhibitor. 10 patients including all 7 nonresponders had died. Responders had minimum of 15 weeks of response while one had ongoing continued response at 34 weeks. Side effects were seen in 7 patients and only one patient needed cessation of therapy. CD4 counts were stable on treatment while HIV RNA remained undetectable. Conclusion. PD-1 and PD-L1 inhibitors appear to have comparable efficacy and tolerable side effect profile and have no effect on HIV markers when used in HIV patients with advanced cancers.Entities:
Year: 2019 PMID: 31275380 PMCID: PMC6582789 DOI: 10.1155/2019/2989048
Source DB: PubMed Journal: J Oncol ISSN: 1687-8450 Impact factor: 4.375
Clinical characteristics, response, and toxicity profile of patients.
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| 57/F | Lung SCC IV | <1% | Carbo Tax 2 | NA | NA | D (PD) | |
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| 40/M | Lung ADC IV | NA | Carbo Tax 3 then Nivo 1 | NA | NA | D(sepsis) | |
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| 62/M | Lung SCC II | NA | Lobectomy then Cis Docetaxel 1 then Carbo Tax 1 then Nivo 10 | SD | 28 weeks. stopped due to pneumonitis | Pneumonitis (3) | Alive |
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| 45/M | Lung ADC IV | NA | Carbo Alimta 4 then Alimta 4 then Nivo 10 | PR | 24 and ongoing | Colitis (2) | Alive |
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| 45/F | Lung ADC IV | <1% | Carbo Alimta 4 then Alimta 13 then Nivo 17 then Docetaxel | PR | 34 weeks | Alive | |
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| 56/M | Lung SCC IV | NA | Pembro 6 then Carbo Tax 2 | SD | 16 weeks | D(PD) | |
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| 55/M | Lung ADC IV | 20% | Carbo Alimta 4 then Alimta 3 then Pembro 7 then Trastu + Pertuzumab | SD | 22 weeks | Fatigue (1) | alive |
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| 60/M | Lung ADC IV | NA | Carbo Alimta 4 then Alimta 10 then Nivo 8 | PR | 16 and ongoing | Elevated TSH | alive |
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| 58/M | Lung mixed IV | NA | Cis Etopo x5 then Nivo 5 | PD | NA | D(PD) | |
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| 48/M | Lung ADC IV | 90% | Erlotinib 5 months then Pembro 2 | PD | NA | D(PD) | |
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| 40/F | Anal SCC IV | NA | Chemo RT hen CarboTax 5 then Nivo 1 | NA | NA | D (PD) | |
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| 54/M | Anal SCC IV | NA | Mitomycin Xeloda then Nivo 13 | PD | 26 weeks | Hypothyroidism | D(PD) |
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| 43/M | HCC III | NA | Regorafinib 24 then Nivo 12 | SD | 25 weeks | Fatigue (1) | D(PD) |
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| 44/M | HCC IV | NA | RFA, TACE hen Soafenib 3 months then Nivo 12 | PR | 25 and ongoing | Hyperglycemia, Hypothyroidism | Alive |
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| 59/M | RCC III | NA | Sorafenib then Sunitinib then Everolimus the Nivo 11 then Axitinib | SD | 22 weeks | Elevated TSH | D(sepsis) |
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| 42/M | DLBCL IV | NA | RCHOP then RICE PBSCT then Nivo 10 then Rev Rtux 1 | PD | 22 weeks | D(PD) | |
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| 56/M | Invasive basal | NA | Vsmodegib 6 then Nivo 10 | PR | 24 weeks and ongoing | Elevated TSH | alive |
Abbreviations: SCC: squamous cell cancer. ADC: adenocarcinoma. RCC: renal cell cancer. HCC: hepatocellular cancer. DLBCL: diffuse large B cell lymphoma. Nivo: Nivolumab. Pembro: Pembrolizumab. AT: Atezolizumab. NA: not available. SD: stable disease. PR: partial response. PD: progressive disease. Carbo Tax: Carboplatin and Paclitaxel. Cis: Cisplatin. Trastu: Trastuzumab. Cis Etopo: Cisplatin Etoposide. RT: Radiation therapy. RFA: radiofrequency ablation. RCHOP: Rituximab, Cyclophosphamide, Adriamycin, Oncovin, Prednisone. RICE: Rituximab, Ifosfamide, Carboplatin, Etoposide. SCT: stem cell transplant. RR: Rituximab, Revlimid. D: Dead.
HIV-related markers while on immune checkpoint inhibitor therapy.
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| FTC/TDF + DTG | 573 | NA | 0 | NA |
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| EVG/c/FTC/TDF | 242 | NA | <400 | NA |
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| DTG, DRV/r | 795 | 552 | <400 | 0 |
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| ABC/DTG/3TC | 424 | 460 | 0 | 0 |
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| FTC/TDF + DTG | 427 | 402 | 0 | <400 |
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| FTC/TDF + DRV | 626 | 517 | 0 | 0 |
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| ETR, DTG, DRV/r | 607 | 597 | <20 | <20 |
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| EFV/FTC/TDF | 305 | NA | <20 | NA |
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| FTC/TAF + DTG | NA | NA | NA | NA |
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| RPV/FTC/TDF | 469 | NA | <20 | NA |
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| FTC/TDF + DTG | 624 | NA | 500 | NA |
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| ABC/3TC/DTG | 250 | 262 | <20 | <20 |
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| FTC/TDF + DTG | 326 | 431 | 0 | 0 |
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| FTC/TDF + DTG | 150 | 120 | <20 | <20 |
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| TDF/RAL | 461 | 376 | <400 | <400 |
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| DRV/c + DTG | 163 | 285 | 89 | <20 |
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| FTC/TDF + DTG | 264 | 370 | 0 | <400 |
Abbreviations: NA: data not available. ∗: died before response could be assessed. VL: viral load.
HAART regimen: FTC/TDF: emtricitabine/tenofovir disoproxil fumarate. DTG: dolutegravir. EVG/c: elvitegravir/cobicistat. DRV/r: darunavir/ritonavir. ABC: abacavir. 3TC: lamivudine. TDF: tenofovir disoproxil fumarate. RAL: raltegravir. DRV/c: darunavir. ETR: etravirine. EFV: efavirenz. TAF: tenofovir alafenamide. RPV: rilpivirine.