SNPMiner Trials by Shray Alag

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Report for Mutation G681A

Developed by Shray Alag, 2020.
SNP Clinical Trial Gene

There are 2 clinical trials

Clinical Trials

1 A Phase 1 Study of Hypofractionated Stereotactic Radiotherapy and Concurrent HIV Protease Inhibitor Nelfinavir as Part of a Neoadjuvant Regimen in Patients With Locally Advanced Pancreatic Cancer

This phase I trial is studying the side effects and best dose of stereotactic radiation therapy and nelfinavir mesylate when given together with gemcitabine hydrochloride, leucovorin calcium, and fluorouracil in treating patients with locally advanced pancreatic cancer. Stereotactic radiation therapy may be able to send x-rays directly to the tumor and cause less damage to normal tissue. Drugs, such as nelfinavir mesylate, may make tumor cells more sensitive to radiation therapy. Drugs used in chemotherapy, such as gemcitabine hydrochloride, leucovorin calcium, and fluorouracil, work in different ways to stop the growth of tumor cells, either by killing the cells or by stopping them from dividing. Giving stereotactic radiation therapy and nelfinavir mesylate together with combination chemotherapy may kill more tumor cells.

NCT01068327 Adenocarcinoma of the Pancreas Stage III Pancreatic Cancer Drug: gemcitabine hydrochloride Drug: leucovorin calcium Drug: fluorouracil Drug: nelfinavir mesylate Radiation: stereotactic body radiation therapy Radiation: hypofractionated radiation therapy Procedure: therapeutic conventional surgery
MeSH:Pancreatic Neoplasms
HPO:Neoplasm of the pancreas

The pharmacokinetic parameters will be presented as the mean and standard deviation.. Pharmacogenomic status of CYP2C19*2 (G681A) (correlative). --- G681A ---

To measure the pharmacogenomic status of CYP2C19*2 (G681A) in the study population. --- G681A ---

Primary Outcomes

Description: Due to delayed toxicities attributable to radiotherapy, all toxicities observed within 1 month of surgery will be scored. Toxicity will be graded and tabled by dose levels.

Measure: Dose-limiting toxicity as assessed by National Cancer Institute Common Terminology Criteria for Adverse Events (NCI CTCAE) v3.0

Time: Within 1 month of surgery

Description: The MTD of SRT/nelfinavir mesylate is defined as the highest dose level at which no greater than one dose-limiting toxicity is observed in 6 patients.

Measure: Maximally tolerated dose (MTD) of stereotactic radiotherapy and concurrent nelfinavir mesylate

Time: 3 patients will initially be treated at each dose level (4 levels); a minimum of 1 month of observation after surgery is required in all 3 patients before escalation

Secondary Outcomes

Description: At the MTD, the rate of surgical complete resection with 90% exact binomial confidence intervals will be calculated.

Measure: Rate of complete surgical resection

Time: At the time of surgery (2-3 weeks after completion of SRT)

Description: At the MTD, the rate of pathologic response with 90% exact binomial confidence intervals will be calculated.

Measure: Pathological response

Time: Pre- to post-treatment

Description: Pre- to post-treatment changes in tumor size on CT or MRI scan (if CT is not sufficient).

Measure: Tumor response on CT/MRI

Time: Change from pre- to post-treatment

Measure: Correlation between the radiologic response and pathologic response

Time: Pre- to post-treatment

Description: Exploratory analyses will compare pre- to post-nelfinavir mesylate treatment changes in Akt levels between patients who achieve or do not achieve R0 resection by the nonparametric Wilcoxon rank sum test.

Measure: Phospho-AKT expression in pancreatic tumor tissue (correlative)

Time: Pre- to post-nelfinavir mesylate

Description: The data will be modeled using WinNonLin Pro version 4.1. The pharmacokinetic parameters will be presented as the mean and standard deviation.

Measure: Pharmacokinetics of nelfinavir mesylate (correlative)

Time: After at least 1 week of NFV: *0 h (trough); *After NFV dosing: 1, 2, 3, 4, 5, 6, 8, and 12 h

Description: There is currently insufficient clinical data to indicate whether any of the specific polymorphisms proposed to be studied, particularly those subjects with a heterozygous state, will correlate with meaningful differences in the pharmacokinetic parameters of nelfinavir mesylate. These analyses must therefore be exploratory in nature.

Measure: Pharmacogenomic status of CYP2C19*2 (G681A) (correlative)

Time: Enrollment, at the time of planned tumor tissue procurement, and at the time that re-staging studies are done

2 Creation and Evaluation of the Effectiveness of the Remote Monitoring System for Patients, Who Had Myocardial Infarction

one-centered, open, prospective, non-randomized, controlled clinical study will be aimed at creating remote monitoring system for patients' condition and the development of methodological approaches and its usage for conducting patients, who had myocardial infraction and who has a very high risk of developing an unfavorable outcome.

NCT04424368 Myocardial Infarction Adherence, Patient Device: The remote monitoring system
MeSH:Myocardial Infarction Infarction
HPO:Myocardial infarction

At the end of a 12 month observation with the registration of unfavorable cardiovascular occasions (death from cardiovascular reasons, nonfatal myocardial infraction, cerebral stroke, necessity for repeated revascularization of the coronary arteries) based on the analysis of non-genetic and genetic factors (polymorphism of genes Thr174Met and Met235Thr in gene angiotensinogen, Arg389Gly and Ser49Gly in gene adrenoceptor beta 1, Ser447Ter in gene lipoprotein lipase and Leu28Pro in gene apolipoprotein E, Trp212Ter and G681A in gene cytochrome P450 family 2 subfamily C member 19) factors of unfavorable prognosis will be identified and considering which group of patients requires the use of remote monitoring system will be formed. --- Thr174Met --- --- Met235Thr --- --- Arg389Gly --- --- Ser49Gly --- --- Leu28Pro --- --- G681A ---

Primary Outcomes

Description: the number of deaths from cardiovascular causes

Measure: cardiovascular mortality

Time: 12 months

Description: incidence of acute myocardial infarction

Measure: acute myocardial infarction

Time: 12 months

Description: incidence of cerebral stroke

Measure: cerebral stroke

Time: 12 months

Description: frequency of repeated revascularization of coronary arteries

Measure: revascularization

Time: 12 months

Description: frequency of hospitalization about the progression of coronary heart disease

Measure: hospitalization

Time: 12 months

HPO Nodes

HP:0002894: Neoplasm of the pancreas
Genes 103
CHEK2 STK11 CDC73 BAP1 CDKN2A APC TERT RAD50 SPINK1 NOP10 STK11 PMS2 RAD51C BMPR1A FLI1 EPCAM ACD CLCNKB CDC73 NUTM1 CDK4 NTHL1 NPM1 VHL MRE11 WRAP53 CDKN1B TP53 TP53 PDGFRB BRIP1 NOTCH3 MLH3 MSH2 WT1 BRCA1 TP53 CDKN2A BARD1 MSH6 KRAS PMS1 PALLD CDKN2A STK11 NBN MITF TERC MEN1 BRCA2 RAD51 MLH1 AAGAB TP53 RNF43 TERT COL14A1 CCND1 KRAS MC1R BRCA2 PALB2 MGMT TP53 RAD51D PARN TGFBR2 KRAS BRD4 SMAD4 MAFA SMAD4 PRKAR1A CDKN1B RPS20 BRCA2 SEMA4A CDKN2B CHEK2 NHP2 RTEL1 EWSR1 MEN1 TERF2IP POT1 CDC73 MDM2 APC USB1 CDKN2A GCGR TINF2 CTC1 CDKN1A BRCA1 CDKN2B PIK3CA DKC1 SLC12A3 CDKN2C FAN1 PTEN PALB2
Protein Mutations 17
A636P G12C G12D G12R G12V G135C G13D G20210A G681A I1307K P13K Q61L Q61R R72P S428F V222A V600E
SNP 0
HP:0001658: Myocardial infarction
Genes 79
MYH9 JAK2 IL12A CYP27A1 HLA-B BSCL2 LIMK1 RFC2 LDLR LPL RAF1 MEFV SH2B3 ABCA1 WRN GTF2I SCNN1A TBL2 CYP27A1 HLA-B MEFV ABCG8 ELN BRAF C4A IL12A-AS1 CEP19 CAV1 IKZF1 UBAC2 MLX THOC2 CTNNB1 PTPN11 SCNN1G MEF2A IL10 CLIP2 IL12B ABCC6 MYH9 ABCA1 LDLRAP1 GLA STAT4 SH2B3 CFTR SLC2A10 IL23R CBS ERAP1 BAZ1B LMNA PCSK9 CCR1 BRAF FOS APOB KLRC4 JAK2 AGPAT2 TET2 LRP6 BCHE ABCG5 TLR4 HLA-B DYRK1B SCNN1B GTF2IRD1 TP53 PPARG CAVIN1 MPL ENPP1 PIGA FAS CALR HGD
Protein Mutations 13
A1166C C344T C807T G1051A G20210A G3514C G98T I843S L33P M235T Q192R Q222R V34L
SNP 11
rs10153820 rs16969968 rs1761667 rs4244285 rs4986893 rs6434222 rs6971 rs7586970 rs7903146 rs8069645 rs8176528