in humans, a combination of XX chromosomes results in a female zygote and that of XY result in a male zygotes. From whom does the a male zygotes inherit an X chromosome

Answer:

Lesson 2: Energy Roles of Organisms

Explanation:

1. B. They both produce carbohydrates

2. B. They both obtain energy by consuming other organisms.

3. C. Carnivore, Consumer

4. A. A decomposer  breaks down organic compounds in dead organic matter, and a detritivote eats dead and decaying mater.

A the cell wall controls division of the cell

mRNA processing and Gene regulation

Explanation:

• A particular gene does NOT constantly churn out the same protein at all times in every cell. This is true for two reasons. First, mRNA processing can allow one gene to produce several different proteins. Second, genes are constantly being turned on and off through the process of gene regulation.

The process by which a pre-mRNA undergo various  modification so that it can become a mature RNA is called RNA processing . During RNA processing, splicing is an important step. During splicing, the introns are precisely excised and exons are ligated together. A process of alternative splicing is excised by which more than one mRNA species can be produced from a single pre-mRNA. Thus mRNA processing is the method that allows  a gene to produce different proteins. secondly, the regulation of genes initiate the control of gene products.

Answer:

The age of 35 years was established to offer invasive techniques, because at this age the risk of secondary abortion was balanced by the technique and the risk of chromosomal alteration.

Explanation:

The possibility of early diagnosis of fetal anomalies of various kinds (neural defects, chromosomopathies, etc.) has been one of the top concerns of gynecologists and geneticists, for obvious reasons.

Throughout these years, prenatal diagnostic techniques have been developed that allow therapeutic decisions by doctors or viability of pregnancy by parents. These techniques are initially performed with non-invasive methods (biochemical determinations, ultrasound), and if the suspicion is increasing, it is passed to more invasive techniques such as amniocentesis or chorionic villus biopsy.

Given that in the latter there is a risk of loss of pregnancy, it is previously attempted to ensure that the indication is correct, and for this, new biochemical tests and risk calculation systems have been added.

Until recently the criterion for establishing the risk of fetal chromosomal abnormality was the mother's age, since there was a clear relationship between maternal age and chromosomal abnormalities, especially Down. The age of 35 years was established to offer invasive techniques, because at this age the risk of secondary abortion was balanced by the technique and the risk of chromosomal alteration. The problem was that a small number of cases were detected. Therefore, other parameters have been sought that estimate more precisely those subsidiary chaos of early detection.

The estimation of the risk in a given pregnant woman is done by multiplying the risk associated with her age for the specific gestational age.

Currently, most prenatal tests consist of AFP, estriol and human chorionic gonadotropin (hCG), which is the triple test, which is a blood test that assesses the risk in a pregnancy of having a Down syndrome or spina bifida It is not a test that tells us whether or not the fetus has any of these defects. It is a test that tells us the probability of risk of having them. Studies have shown that about 70% of fetuses with Down syndrome can be identified early combining the analysis of the mother's age and the results of the triple test.