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BIOC 201 FINAL EXAM QUESTIONS 2025. Exam Questions and Correct Answers With 100% Correct Answers | Latest 2025 Update.

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BIOC 201 FINAL EXAM QUESTIONS 2025. Exam Questions and Correct Answers With 100% Correct Answers | Latest 2025 Update.

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Institution
BIOC 201
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BIOC 201 FINAL REVIEW QUESTIONS AND ACCURATE ANSWERS 2024/2025 |
VERIFIED
covalent and hydrogen bonds - -covalent bonds form between atoms in a molecule

-hydrogen bonds form between polar water molecules

-electrons spend more time near oxygen, more electronegative

-arrangement constantly changes, multiple hydrogen bonds at a time



hydrophobic interaction - -hydrophobic substances are nonpolar and repel water

-lipids in a water environment will attract each other, decreasing entropy

-molecules are more ordered near surfaces, when surface area decreases (lipids group together),
entropy decreases



polysaccharide structure-function - -carbohydrate chains, polymers of sugars, helix shape

-monosaccharides are joined by glycosidic linkage (covalent bond formed by dehydration reaction

-glucose polymers include starch (plant storage, alpha linkages), glycogen (animal storage), cellulose
(plant structure, beta linkages), and chitin (animal structure)

-hydrolysis breaks down polysaccharides for energy



lipid structure-function - -fats consist of glycerol and fatty acids (hydrophobic carbon skeleton)

-triacylglycerol has 3 fatty acids join to glycerol by an ester linkage

-saturated fats have maximum number of hydrogens, no double bonds, solid at room temp

-unsaturated fats have double bonds, bends in the carbon chain, liquid at room temp

-fats are great for energy storage, adipose tissue

-phospholipids have a hydrophilic head, hydrophobic tail

-form phospholipid bilayer together, cell membrane

-steroid are soluble, have cyclical carbon structures, include cholesterol (in animal cell membranes) and
hormones



protein structure - -amino acids have an amino, carboxyl, and variable group

-polypeptides are polymers of amino acids, joined by peptide bonds (dehydration reaction)

,-amino acids are always added to the C-terminus

-primary structure is the sequence of amino acids, determined by genetic information

-secondary structure is the coils and folds resulting from hydrogen bonds, alpha helix or beta sheet

-tertiary structure is overall shape resulting from side chain interactions, held together by hydrogen
bonds, disulfide bridges (covalent), and ionic bonds, hydrophobic collapse pushes nonpolar parts of the
protein inward and decreases surface area

-quaternary structure is the combination of tertiary proteins, hemoglobin is made of 4 parts



nucleic acid structure - -nucleotides have a nitrogenous base (AGCTU), pentose sugar (deoxyribose,
ribose), phosphate group

-pyrimidines are CTU, purines are AG

-double hydrogen bond between A and T/U, triple hydrogen bond between G and C

-nucleotides are joined by phosphodiester linkage, covalent bond between sugar of one and phosphate
of the other



protein folding - -chaperones are proteins that assist in proper protein folding

-hydrophobic collapse is delayed by HSP60, HSP70, powered by ATP, keeping proteins away from external
influences

-HSP70 holds on and lets go

-HSP60 changes shape at same time, cooperativity



protein turnover - -ubiquitin-proteasome system breaks down misfolded proteins (30% of all proteins)

-ubiquitin ligase (enzyme) attaches ubiquitin to the protein, signalling a proteasome to come break it
down with hydrolysis



ATP function - -ATP hydrolysis (exergonic reaction, favored) is coupled with protein synthesis (endergonic
reaction, unfavored)

-ATPase (ex. HSP70) puts strain on ATP, Mg2+ holds other bonds in place, water hydrolyzes, and a
phosphate is released

-the phosphate is used to phosphorylate something



enzyme structure-function - -proteins that catalyze metabolic chemical reactions

, -bind to specific substrates and lower the activation energy for a certain reaction to occur

-active site, lock and key, induced fit



enzyme regulation - -allosteric regulation involves some ligand binding to the allosteric site, causing a
conformation change of the enzyme

-covalent modification involves phosphorylation of the enzyme, phosphate came from ATP



organelle functions - -nucleus, nuclear envelope, nuclear lamina, chromosomes/chromatin, nucleolus

-mitochondria, chloroplasts, etc.

-ribosomes are suspended in cytosol or attached to ER (make proteins that need to be shipped
somewhere)

-endomembrane system includes nuclear envelope, endoplasmic reticulum, golgi apparatus, lysosomes,
vacuoles, plasma membrane

-smooth ER does synthesis of lipids, metabolism of carbohydrates, detox of drugs

-rough ER has ribosomes on it that feed their polypeptides into the ER lumen

-golgi apparatus modifies, sorts, and targets products to various pars of cell, identification tags

-lysosomes are membranous sacs of hydrolytic enzymes that animal cells use to digest molecules

-acidic environment inside

-phagocytosis is where a vacuole fuses with lysosome

-autophagy is where damaged organelles are surround by a membrane and brought to lysosome



proteins and endomembrane system - -proteins have targeting signals, the first directs them to the
endomembrane system, the second directs them to a specific part of the cell

-a signal recognition particle (SRP) stops translation and brings the ribosome to the rough ER

-everything must go through the Golgi apparatus



cell wall and extracellular matrix - -cell wall protects plant cells and prevents excessive uptake of water

-made of cellulose

-primary cell wall (flexible),middle lamella (glue), secondary cell wall (durable)

-perforated by plasmodesmata between cells

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