Your search keyword '"Jain, Chandni"' showing total 11 results

1. A systematic review on the imaging findings in auditory neuropathy spectrum disorder

Author

Mathew, Supriya and Jain, Chandni

Abstract

The present systematic review examined imaging findings in the Auditory Neuropathy Spectrum Disorder (ANSD) population.

Published

2024

2. Central Auditory Processing Abilities in Children with Non-Syndromic Cleft Lip and Palate: An Electrophysiological Study

Author

Kujur, Deepshikha and Jain, Chandni

Abstract

Background The present study compared the central auditory processing abilities using electrophysiological tests in children with non-syndromic cleft lip and palate (NSCLP) and their age-matched control group.Method Thirty children aged 7 to 15 years were recruited for the study. Participants were divided into 2 groups. The clinical group (children with NSCLP) comprised 15 children, while the control group (craniofacially typical peers) comprised 15 children with normal hearing sensitivity and auditory processing skills. Electrophysiological tests, including auditory brainstem responses (ABR), binaural interaction component (BIC) of ABR, auditory late latency responses (ALLR), and P300 were assessed.Results The results showed deviant responses in ABR, BIC, and ALLR in children with NSCLP compared to craniofacially typical counterparts. However, no significant difference was observed in P300 between the two groups.Conclusion Children with NSCLP may be at a higher risk of central auditory processing disorder due to their abnormal neural transmission in the auditory nervous system. Also, assessing auditory processing abilities in children with NSCLP should include electrophysiological tests in the test battery for additional information regarding neural transmission.

Published

2024

3. Central auditory processing abilities in individuals with tinnitus and normal hearing sensitivity: a systematic review

Author

S., Sanjay, Vinod, Vibha, and Jain, Chandni

Abstract

Background: Tinnitus is the perception of sound when there is no external sound stimulus. Individuals with tinnitus may have altered neurological system corresponding to the auditory pathway. Therefore, central auditory processing abilities, which rely on the central auditory pathway, may be affected. This study reviewed the published studies regarding the impact of tinnitus on central auditory processing abilities. Main text: A total of 3087 studies were identified, of which 18 fulfilled the eligibility criteria and were included in the review. The included studies scored good or fair in the quality assessment checklist. The review showed that individuals who had tinnitus with normal hearing sensitivity performed poorly on temporal resolution tests, speech perception in noise, localization, and auditory memory. However, temporal patterning and dichotic tests were not shown to be affected by tinnitus. Conclusion: The audiologists involved in tinnitus assessment are recommended to include central auditory processing tests in routine evaluation for the early diagnosis and intervention for subjects with tinnitus.

Published

2023

4. Trophoblast survival signaling during human placentation requires HSP70 activation of MMP2-mediated HBEGF shedding

Author

Jain, Chandni V, Jessmon, Philip, Barrak, Charbel T, Bolnick, Alan D, Kilburn, Brian A, Hertz, Michael, and Armant, D Randall

Abstract

Survival of trophoblast cells in the low oxygen environment of human placentation requires metalloproteinase-mediated shedding of HBEGF and downstream signaling. A matrix metalloproteinase (MMP) antibody array and quantitative RT-PCR revealed upregulation of MMP2 post-transcriptionally in human first trimester HTR-8/SVneo trophoblast cells and placental villous explants exposed to 2% O2. Specific MMP inhibitors established the requirement for MMP2 in HBEGF shedding and upregulation. Because α-amanitin inhibited the upregulation of HBEGF, differentially expressed genes were identified by next-generation sequencing of RNA from trophoblast cells cultured at 2% O2for 0, 1, 2 and 4 h. Nine genes, all containing HIF-response elements, were upregulated at 1 h, but only HSPA6 (HSP70B’) remained elevated at 2–4 h. The HSP70 chaperone inhibitor VER 155008 blocked upregulation of both MMP2 and HBEGF at 2% O2, and increased apoptosis. However, both HBEGF upregulation and apoptosis were rescued by exogenous MMP2. Proximity ligation assays demonstrated interactions between HSP70 and MMP2, and between MMP2 and HBEGF, supporting the concept that MMP2-mediated shedding of HBEGF, initiated by HSP70, contributes to trophoblast survival at the low O2concentrations encountered during the first trimester, and is essential for successful pregnancy outcomes. Trophoblast survival during human placentation, when oxygenation is minimal, required HSP70 activity, which mediated MMP2 accumulation and the transactivation of anti-apoptotic ERBB signaling by HBEGF shedding.

Published

2017

5. Potential role of epigenetic mechanisms in regulation of trophoblast differentiation, migration, and invasion in the human placenta

Author

Kohan-Ghadr, Hamid-Reza, Kadam, Leena, Jain, Chandni, Armant, D. Randall, and Drewlo, Sascha

Abstract

ABSTRACTThe proper establishment and organogenesis of the placenta is crucial for intrauterine fetal growth and development. Endometrial invasion by the extravillous trophoblast cells, as well as formation of the syncytiotrophoblast (STB), are of vital importance for placental function. Trophoblast migration and invasion is often compared to tumor metastasis, which uses many of the same molecular mechanisms. However, unlike cancer cells, both initiation and the extent of trophoblast invasion are tightly regulated by feto-maternal cross-talk, which when perturbed, results in a wide range of abnormalities. Multiple factors control the trophoblast, including cytokines and hormones, which are subject to transcriptional regulatory networks. The relevance of epigenetics in transcriptional regulation of trophoblast differentiation and invasion, as well as in the onset of placenta-related pregnancy disorders, became recognized decades ago. Although, there has been tremendous progress in uncovering the molecular foundation of placental development, there is still much to be learned about the epigenetic machinery, and its role in trophoblast differentiation and invasion.This review will provide an overview of the epigenetic control of trophoblast differentiation and invasion. It will also highlight the major epigenetic mechanisms involved in pregnancy complications related to placental deficiencies.

Published

2016

6. The Secreted Protein Rv1860 of Mycobacterium tuberculosisStimulates Human Polyfunctional CD8+T Cells

Author

Satchidanandam, Vijaya, Kumar, Naveen, Biswas, Sunetra, Jumani, Rajiv S., Jain, Chandni, Rani, Rajni, Aggarwal, Bharti, Singh, Jaya, Kotnur, Mohan Rao, and Sridharan, Anand

Abstract

ABSTRACTWe previously reported that Rv1860 protein from Mycobacterium tuberculosisstimulated CD4+and CD8+T cells secreting gamma interferon (IFN-?) in healthy purified protein derivative (PPD)-positive individuals and protected guinea pigs immunized with a DNA vaccine and a recombinant poxvirus expressing Rv1860 from a challenge with virulent M. tuberculosis. We now show Rv1860-specific polyfunctional T (PFT) cell responses in the blood of healthy latently M. tuberculosis-infected individuals dominated by CD8+T cells, using a panel of 32 overlapping peptides spanning the length of Rv1860. Multiple subsets of CD8+PFT cells were significantly more numerous in healthy latently infected volunteers (HV) than in tuberculosis (TB) patients (PAT). The responses of peripheral blood mononuclear cells (PBMC) from PAT to the peptides of Rv1860 were dominated by tumor necrosis factor alpha (TNF-a) and interleukin-10 (IL-10) secretions, the former coming predominantly from non-T cell sources. Notably, the pattern of the T cell response to Rv1860 was distinctly different from those of the widely studied M. tuberculosisantigens ESAT-6, CFP-10, Ag85A, and Ag85B, which elicited CD4+T cell-dominated responses as previously reported in other cohorts. We further identified a peptide spanning amino acids 21 to 39 of the Rv1860 protein with the potential to distinguish latent TB infection from disease due to its ability to stimulate differential cytokine signatures in HV and PAT. We suggest that a TB vaccine carrying these and other CD8+T-cell-stimulating antigens has the potential to prevent progression of latent M. tuberculosisinfection to TB disease.

Published

2016

7. Cell signaling in trophoblast-uterine communication.

Author

FRITZ, RANI, JAIN, CHANDNI, and ARMANT, D. RANDALL

Subjects

EMBRYO implantation, CELLULAR signal transduction, TROPHOBLAST, UTERUS, BLASTOCYST, PREGNANCY

Abstract

Intricate and precise communication between the blastocyst and the uterus orchestrates embryo implantation. However, many questions remain unanswered regarding the molecular complexities of implantation. On-time implantation requires a receptive uterus and a mature blastocyst with trophoblast cells capable of adhering to and invading the endometrium. Defects in uterine receptivity or embryo/uterine signaling can cause implantation failure or early pregnancy loss, whereas deficient trophoblast differentiation can generate placental abnormalities that produce adverse pregnancy outcomes. This review will discuss several examples of signaling pathways that regulate trophoblast and uterine development during this period. Leukemia inhibitory factor is involved in uterine priming for implantation. The epidermal growth factor signaling system contributes to trophoblast-uterine communication, as well as trophoblast adhesion and invasion. Indian hedgehog signaling synchronizes tissue compartments within the uterus, and WNT signaling mediates numerous interactions within the implantation site and developing placenta. The autocrine, paracrine and juxtacrine interactions mediated by these signaling pathways contribute significantly to the establishment of pregnancy, although there are many other known and yet to be discovered factors that synchronize the maternal and embryonic developmental programs. [ABSTRACT FROM AUTHOR]

Published

2014

8. The effect of tinnitus on some psychoacoustical abilities in individuals with normal hearing sensitivity.

Author

Jain, Chandni and Sahoo, Jitesh Prasad

Abstract

Introduction: Tinnitus is the perception of a sound without an external source. It can affect auditory perception abilities in individuals with normal hearing sensitivity. Purpose: The aim of the study was to determine the effect of tinnitus on psychoacoustic abilities in individuals with normal hearing sensitivity. Materials and Methods: The study was conducted on twenty subjects with tinnitus and twenty subjects without tinnitus. Tinnitus group was again divided into mild and moderate tinnitus based on the tinnitus handicap inventory. Data Collection and Analysis: Differential limen of intensity, differential limen of frequency, gap detection test, modulation detection thresholds were done through the mlp toolbox in Matlab and speech in noise test was done with the help of Quick SIN in Kannada. Results: Results of the study showed that the clinical group performed poorly in all the tests except for differential limen of intensity. Conclusions: Tinnitus affects aspects of auditory perception like temporal resolution, speech perception in noise and frequency discrimination in individuals with normal hearing. This could be due to subtle changes in the central auditory system which is not reflected in the pure tone audiogram. [ABSTRACT FROM AUTHOR]

Published

2014

9. Spectrophotometric evaluation of the color changes of different feldspathic porcelains after exposure to commonly consumed beverages

Author

Jain, Chandni, Bhargava, Akshay, Gupta, Sharad, Rath, Rishi, Nagpal, Abhishek, and Kumar, Prince

Published

2013

10. Fetal genome profiling at 5 weeks of gestation after noninvasive isolation of trophoblast cells from the endocervical canal

Author

Jain, Chandni V., Kadam, Leena, van Dijk, Marie, Kohan-Ghadr, Hamid-Reza, Kilburn, Brian A., Hartman, Craig, Mazzorana, Vicki, Visser, Allerdien, Hertz, Michael, Bolnick, Alan D., Fritz, Rani, Armant, D. Randall, and Drewlo, Sascha

Abstract

Fetal trophoblast cells obtained noninvasively early in gestation provided fetal DNA for comprehensive targeted sequencing across the genome.

Published

2016

11. Regulation of HBEGF Biosynthesis by MicroRNA in Human Trophoblast Cells.

Author

Jain, Chandni, Jessmon, Philip, Kilburn, Brian A., and Armant, D. Randall

Abstract

The epidermal growth factor (EGF) family member, heparin binding EGF-like growth factor (HBEGF), is present in the uterus at the time of embryo implantation and is expressed in invading trophoblast cells of the placenta indicating its central role in implantation and subsequent placentation. Previous work has demonstrated that HBEGF protein levels are dramatically upregulated in trophoblast cells cultured at low (2%) O2without a change in HBEGF mRNA. Therefore, it can be hypothesized that HBEGF is translationally regulated by O2in trophoblast cells where it prevents apoptosis during the first trimester when O2levels are ~2%. MicroRNAs (miRNAs) are small non-coding RNA species that primarily target the 3' untranslated region (3'UTR) of mRNA and regulate translation. They are transcribed as pri-miRNAs by RNA Polymerase II and are subsequently processed by nuclear proteins Drosha and DGCR8 into shorter pre-miRNA precursors. After export into the cytoplasm, pre-miRNAs are processed into their mature form. MicroRNAs specifically bind to target transcripts and, due to imperfect base pairing, can alter translation of mRNA. A miRNA-mediated mechanism could be responsible for the translational regulation of HBEGF by O2concentration. In this study the role of miRNA in regulating translation of HBEGF mRNA through its 3'UTR was investigated. The potential role of miRNA in the targeted regulation of HBEGF biosynthesis was examined by RNAi knockdown of the miRNA-processing protein, DGCR8, in HTR-8/SVneo human first trimester trophoblast cells by transfection of siRNA using siPORT NeoFX transfection agent. Western blots with antibody against DGCR8 and toxicity assays were used to optimize conditions. HBEGF quantified by ELISA did not increase when DGCR8 was knocked down at 20% O2, indicating that HBEGF expression was not repressed by miRNA. However, the upregulation of HBEGF at 2% O2was inhibited. A dual luciferase reporter construct (psiCHECK-2) containing the intact HBEGF 3'UTR or specific subregions was implemented to examine its translational regulatory potential. The intact 3'UTR reduced luciferase activity (p=0.008). However, the isolated 5' and 3' regions of the 3'UTR increased reporter activity by 4- to 5-fold (p<0.05) when the central domain was removed. These findings suggest that miRNAs alter interaction between inhibitory elements in the central domain of the 3'UTR and flanking elements to increase HBEGF translation. It is concluded that HBEGF is not transcriptionally regulated by O2in human trophoblast cells, but is translationally regulated through the interaction of miRNA with the HBEGF 3'UTR. Supported by the intramural research program of NICHD/NIH.

Published

2012