Compounds > hydroxyindoleacetic acid
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hydroxyindoleacetic acid and Cells, Neoplasm Circulating

hydroxyindoleacetic acid has been researched along with Cells, Neoplasm Circulating in 1 studies

(5-hydroxyindol-3-yl)acetic acid : A member of the class of indole-3-acetic acids that is indole-3-acetic acid substituted by a hydroxy group at C-5.

Research

Studies (1)

TimeframeStudies, this research(%)All Research%
pre-19900 (0.00)18.7374
1990's0 (0.00)18.2507
2000's0 (0.00)29.6817
2010's0 (0.00)24.3611
2020's1 (100.00)2.80

Authors

AuthorsStudies
Meyer, T1
Caplin, M1
Khan, MS1
Toumpanakis, C1
Shetty, S1
Ramage, JK1
Houchard, A1
Higgs, K1
Shah, T1

Clinical Trials (1)

Trial Overview

TrialPhaseEnrollmentStudy TypeStart DateStatus
A Phase IV, Multicentre, Open Label, Single Group Exploratory Study to Assess the Clinical Value of Enumeration of Circulating Tumour Cells (CTCs) to Predict Clinical Symptomatic Response and Progression Free Survival in Patients Receiving Deep Subcutaneo[NCT02075606]Phase 450 participants (Actual)Interventional2014-05-31Completed
[information is prepared from clinicaltrials.gov, extracted Sep-2024]

Trial Outcomes

Percentage of Subjects Alive and Progression Free at One Year

"Subjects underwent CT or MRI scans at baseline and Week 53. Progression was assessed by investigators using RECIST v1.1. The best overall response to study treatment is the highest time point response achieved by the subject and was assessed as a complete response, partial response, stable disease, progressive disease or non evaluable. For analysis of PFS, event dates were assigned to the first time that progressive disease was noted or the date of death. In case of progressive disease followed by death, the first event was considered in the analysis. Censoring dates were defined in subjects with no progressive disease or death before end of study.~At one year (end of study), the mean percentage of subjects who were alive and progression free, as calculated using the Kaplan-Meier method, is reported by CTC presence and overall." (NCT02075606)
Timeframe: From baseline up to Week 53.

Interventionpercentage of subjects (Mean)
CTC Presence at Baseline69.00
No CTC Presence at Baseline67.75
Lanreotide Autogel66.43

Assessment of Clinical Symptomatic Response

"This endpoint was assessed using 2 efficacy variables:~CTCs, enumerated at baseline and Weeks 5, 17, 25, 53~Clinical symptomatic response, assessed by the use of symptom reporting~Subjects recorded 24-hour symptom frequency and severity for 7 days prior to first treatment (baseline), throughout the study, and up to 28 days following final drug administration. Symptoms were recorded by answering predetermined questions on the interactive voice response system (IVRS).~Subjects were considered to have a clinical symptomatic response between baseline and last study visit if any 1 of the following criteria were fulfilled: the average number of episodes of diarrhoea decreased by at least 50%, the average number of episodes of flushing decreased by at least 50%, the mode severity of flushing decreased by at least 1 level. Clinical symptomatic response was assessed as a qualitative variable (Yes/No) and reported according to CTC presence at baseline and overall." (NCT02075606)
Timeframe: From baseline up to Week 53.

,,
InterventionPercentage of Subjects (Number)
Clinical Symptomatic Response = Yes(2)Clinical Symptomatic Response = No(3)
CTC Presence at Baseline77.822.2
Lanreotide Autogel87.512.5
No CTC Presence at Baseline95.54.5

Mean Change From Baseline in Number of Episodes of Diarrhoea and Flushing

"The effect of lanreotide Autogel on the symptoms of diarrhoea and flushing in subjects was assessed through subject reporting of symptoms every 24-hours for the 7 days prior to treatment (baseline), for the first 16 weeks and on days 11 to 17 after each subsequent injection interval. After the final study drug injection at Week 49, subjects provided 24-hour symptom frequency on days 11 to 28 (up to Week 53). Symptom frequency was recorded by answering predetermined questions on the IVRS.~Mean change from baseline in frequency (number of episodes) of diarrhoea and flushing are described at Visit 2 (average number of episodes in Week 1) and at Visit 14 (average number of episodes over days 11 to 17 after Week 49 injection and over days 11 to 28 after Week 49 injection) by CTC presence at baseline and overall. A negative change indicates an improvement in symptoms from baseline." (NCT02075606)
Timeframe: From baseline up to Week 53.

Interventionnumber of episodes (Mean)
Diarrhoea: Visit 2 (daily)Flushing: Visit 2 (daily)
Missing CTC Status at Baseline0.380.00

Mean Change From Baseline in Number of Episodes of Diarrhoea and Flushing

"The effect of lanreotide Autogel on the symptoms of diarrhoea and flushing in subjects was assessed through subject reporting of symptoms every 24-hours for the 7 days prior to treatment (baseline), for the first 16 weeks and on days 11 to 17 after each subsequent injection interval. After the final study drug injection at Week 49, subjects provided 24-hour symptom frequency on days 11 to 28 (up to Week 53). Symptom frequency was recorded by answering predetermined questions on the IVRS.~Mean change from baseline in frequency (number of episodes) of diarrhoea and flushing are described at Visit 2 (average number of episodes in Week 1) and at Visit 14 (average number of episodes over days 11 to 17 after Week 49 injection and over days 11 to 28 after Week 49 injection) by CTC presence at baseline and overall. A negative change indicates an improvement in symptoms from baseline." (NCT02075606)
Timeframe: From baseline up to Week 53.

,,
Interventionnumber of episodes (Mean)
Diarrhoea: Visit 2 (daily)Diarrhoea: Visit 14 (days 11-17)Diarrhoea: Visit 14 (days 11-28)Flushing: Visit 2 (daily)Flushing: Visit 14 (days 11-17)Flushing: Visit 14 (days 11-28)
CTC Presence at Baseline-0.66-1.91-2.15-1.76-3.37-3.49
Lanreotide Autogel-0.42-1.18-1.30-1.43-2.88-2.79
No CTC Presence at Baseline-0.27-0.64-0.63-1.25-2.51-2.23

Mode Symptom Severity of Episodes of Flushing

The effect of lanreotide Autogel on the mode severity of flushing was assessed through subject reporting of symptoms every 24-hours for the 7 days prior to treatment (baseline), for the first 16 weeks and on days 11 to 17 after each subsequent injection interval until Week 49. After the final study drug injection at Week 49, subjects provided 24-hour symptom severity on days 11 to 28 (up to Week 53). Symptom severity was recorded by answering predetermined questions on the IVRS using a three-point system (mild, moderate or severe). The mode (most frequent) intensity of flushing are reported at baseline and at Visit 14 (average number of episodes over days 11 to 17 after Week 49 injection and over days 11 to 28 after Week 49 injection). Percentages of subjects in each severity category are based on the number of subjects in the analysis set with available responses. Data is presented according to CTC presence at baseline and overall. (NCT02075606)
Timeframe: From baseline up to Week 53.

,,
Interventionpercentage of subjects (Number)
No flushing: BaselineMild: BaselineModerate: BaselineSevere: BaselineNo flushing: Visit 14 (days 11-17)Mild: Visit 14 (days 11-17)Moderate: Visit 14 (days 11-17)Severe: Visit 14 (days 11-17)No flushing: Visit 14 (days 11-28)Mild: Visit 14 (days 11-28)Moderate: Visit 14 (days 11-28)Severe: Visit 14 (days 11-28)
CTC Presence at Baseline22.727.345.54.537.543.818.80.013.360.026.70.0
Lanreotide Autogel14.038.046.02.032.445.921.60.023.555.917.62.9
No CTC Presence at Baseline0.050.050.00.028.647.623.80.031.652.610.55.3

Mode Symptom Severity of Episodes of Flushing

The effect of lanreotide Autogel on the mode severity of flushing was assessed through subject reporting of symptoms every 24-hours for the 7 days prior to treatment (baseline), for the first 16 weeks and on days 11 to 17 after each subsequent injection interval until Week 49. After the final study drug injection at Week 49, subjects provided 24-hour symptom severity on days 11 to 28 (up to Week 53). Symptom severity was recorded by answering predetermined questions on the IVRS using a three-point system (mild, moderate or severe). The mode (most frequent) intensity of flushing are reported at baseline and at Visit 14 (average number of episodes over days 11 to 17 after Week 49 injection and over days 11 to 28 after Week 49 injection). Percentages of subjects in each severity category are based on the number of subjects in the analysis set with available responses. Data is presented according to CTC presence at baseline and overall. (NCT02075606)
Timeframe: From baseline up to Week 53.

Interventionpercentage of subjects (Number)
No flushing: BaselineMild: BaselineModerate: BaselineSevere: Baseline
Missing CTC Status at Baseline1000.00.00.0

Percentage of Subjects With Time Point Responses According to Response Evaluation Criteria in Solid Tumours (RECIST) Assessments at Weeks 25 and 53

"Subjects underwent Computed Tomography (CT) or Magnetic Resonance Imaging (MRI) scans at baseline, Visit 8 (Week 25) and Visit 15 (Week 53). Progression was assessed by investigators using RECIST v1.1, and classified as a complete response, partial response, stable disease, progressive disease or non evaluable.~The time point responses at Week 25 and Week 53 were analysed by CTC presence at baseline and overall. The percentage of subjects within each response category are presented. Percentages are based on the number of subjects in the concerned population with available responses." (NCT02075606)
Timeframe: Week 25 and Week 53.

,,
Interventionpercentage of subjects (Number)
Week 25: Complete ResponseWeek 25: Partial ResponseWeek 25: Stable DiseaseWeek 25: Progressive DiseaseWeek 25: Non evaluableWeek 53: Complete ResponseWeek 53: Partial ResponseWeek 53: Stable DiseaseWeek 53: Progressive DiseaseWeek 53: Non evaluable
CTC Presence at Baseline0.018.272.79.10.00.06.766.726.70.0
Lanreotide Autogel0.013.073.913.00.00.05.464.929.70.0
No CTC Presence at Baseline0.08.375.016.70.00.04.563.631.80.0

QoL Questionnaire: EORTC QLQ-G.I.NET21

The effect of lanreotide Autogel treatment on QoL was assessed using the EORTC QLQ-G.I.NET21 at baseline, Weeks 13 (Visit 5), 25 (Visit 8) and 53 (Visit 15/end of study). The QLQ-G.I.NET21 questionnaire contained 21 questions that used a 4-point scale (1 = Not at all, 2 = A little, 3 = Quite a bit, 4 = Very much) to evaluate 3 defined multi-item symptom scales (endocrine, gastrointestinal and treatment related side effects), 2 single item symptoms (bone/muscle pain and concern about weight loss), 2 psychosocial scales (social function and disease-related worries) and 2 other single items (sexuality and communication). Each individual subscore was transformed to range from 0 to 100. Higher scores indicate worse symptoms or more problems. The mean change from baseline at each time point is reported for each of the category subscores. (NCT02075606)
Timeframe: From baseline up to Week 53.

InterventionUnits on a scale (Mean)
Endocrine symptoms: Visit 5Endocrine symptoms: Visit 8Endocrine symptoms: End of studyGastrointestinal symptoms: Visit 5Gastrointestinal symptoms: Visit 8Gastrointestinal symptoms: End of studyTreatment symptoms: Visit 5Treatment symptoms: Visit 8Treatment symptoms: End of studySocial function: Visit 5Social function: Visit 8Social function: End of studyDisease related worries: Visit 5Disease related worries: Visit 8Disease related worries: End of studyMuscle/Bone pain: Visit 5Muscle/Bone pain: Visit 8Muscle/Bone pain: End of studySexual function: Visit 5Sexual function: Visit 8Sexual function: End of studyInformation/communication function: Visit 5Information/communication function: Visit 8Information/communication function: End of studyBody image: Visit 5Body image: Visit 8Body image: End of study
Lanreotide Autogel-15.4-17.0-16.02.11.21.01.27.612.0-11.3-6.5-4.5-14.1-15.9-12.2-7.9-6.5-11.8-5.6-8.9-13.3-8.5-3.7-5.60.91.9-1.0

Quality of Life (QoL) Questionnaire: European Organisation for Research and Treatment of Cancer (EORTC) QoL Questionnaire (QLQ)-C30

"The effect of lanreotide Autogel treatment on QoL was assessed using the EORTC QLQ-C30 at baseline, Weeks 13 (Visit 5), 25 (Visit 8) and 53 (Visit 15/end of study). The 30 item scale is divided into 9 multi item scales (including 5 functional scales, 1 global health status/QoL scale and 3 general symptom scales) and 6 single items. Possible answers to the first 28 items (all items except the 2 concerning global quality of life) go from 1 (Not at all) to 4 (Very much). The answers for the 2 last questions (Q29- 30) go from 1 (Very poor) to 7 (Excellent). All of the scales and single-item measures range in score from 0 to 100. For multi-item scales, the raw score will be calculated by the addition of item responses divided by the number of items. Higher scores for global health and functional domains indicate a better QoL, while higher symptom scores indicate worse symptoms.~The mean change from baseline at each time point is reported for each of the category subscores." (NCT02075606)
Timeframe: From baseline up to Week 53.

InterventionUnits on a scale (Mean)
Physical functioning: Visit 5Physical functioning: Visit 8Physical functioning: End of studyRole functioning: Visit 5Role functioning: Visit 8Role functioning: End of studyEmotional functioning: Visit 5Emotional functioning: Visit 8Emotional functioning: End of studyCognitive functioning: Visit 5Cognitive functioning: Visit 8Cognitive functioning: End of studySocial functioning: Visit 5Social functioning: Visit 8Social functioning: End of studyGlobal QoL: Visit 5Global QoL: Visit 8Global QoL: End of studyFatigue: Visit 5Fatigue: Visit 8Fatigue: End of studyNausea and vomiting: Visit 5Nausea and vomiting: Visit 8Nausea and vomiting: End of studyPain: Visit 5Pain: Visit 8Pain: End of studyDyspnoea: Visit 5Dyspnoea: Visit 8Dyspnoea: End of studyInsomnia: Visit 5Insomnia: Visit 8Insomnia: End of studyAppetite loss: Visit 5Appetite loss: Visit 8Appetite loss: End of studyConstipation: Visit 5Constipation: Visit 8Constipation: End of studyDiarrhoea: Visit 5Diarrhoea: Visit 8Diarrhoea: End of studyFinancial difficulties: Visit 5Financial difficulties: Visit 8Financial difficulties: End of study
Lanreotide Autogel1.22.01.91.33.2-1.46.14.31.1-0.91.5-2.410.04.53.912.57.44.3-4.4-6.3-4.2-4.2-1.4-0.9-7.9-2.31.8-3.51.0-4.8-6.3-5.7-2.9-0.9-6.5-0.01.9-1.01.9-18.5-12.7-10.8-6.7-4.0-1.0

Trials

1 trial available for hydroxyindoleacetic acid and Cells, Neoplasm Circulating

ArticleYear
Circulating tumour cells and tumour biomarkers in functional midgut neuroendocrine tumours.
    Journal of neuroendocrinology, 2022, Volume: 34, Issue:4

    Topics: Adult; Biomarkers, Tumor; Disease Progression; Humans; Hydroxyindoleacetic Acid; Neoplastic Cells, C

2022